1. Introduction

Molecular biomarkers are broadly used for diagnosis, treatment selection and disease monitoring in many clinical settings [1,2]. In the past decade, research in Waldenström macroglobulinemia (WM) has exemplified how nucleic acid analysis may lead to biomarker discovery, hereby enabling more accurate diagnosis and therapy selection. WM is a lymphoplasmacytic lymphoma (LPL) characterized by the predominant bone marrow (BM) accumulation of small lymphocytes, plasma cells (PC) and plasmacytoid lymphocytes. In WM, these abnormal cells are responsible for the overproduction of monoclonal immunoglobulin M (IgM) paraprotein. This abnormal proliferation of neoplastic B-cells impairs the BM equilibrium, hereby inducing cytopenias, and leads to an overabundance of monoclonal IgM, resulting in blood hyperviscosity [3,4]. From a pathological perspective, the WM heterogeneous cell population consists of different B-cells across a morphological continuum, suggesting that the disease may originate during B-cell differentiation after somatic hypermutation in the germinal center and prior to isotype class switching [5,6].

WM belongs to the spectrum of IgM gammopathies, encompassing a wide and heterogeneous group of hematological conditions, ranging from asymptomatic IgM monoclonal gammopathies of undetermined significance (IgM-MGUS), through symptomatic IgM related disorders (such as IgM gammopathies of renal or neurological significance), to asymptomatic WM (aWM), and ultimately to symptomatic WM [7,8,9,10,11,12]. Therefore, an appropriate diagnostic classification that can distinguish between these different entities is crucial. The Second International Workshop Criteria (2° IWWM) formulated the following requirements for WM diagnosis: (a) the presence of IgM monoclonal gammopathy of any size, (b) a BM trephine biopsy with lymphoplasmacytic infiltration and (c) an immunophenotype that excludes the possibility of other lymphoproliferative disorders [9] (Figure 1). Of note, the different diagnostic criteria have been updated several times, and caution should be exercised when comparing between studies [11,13,14,15,16,17,18] (Figure 1).

Patients with IgM-MGUS can progress to WM at a rate of 1.5% to 2% per year [22]. Approximately 20–25% of WM patients are asymptomatic at the time of diagnosis, but up to 70% of these patients will eventually develop disease-associated symptoms within 10 years [23].

WM was described for the first time in 1944 and the role of genetic factors in the pathogenesis has been suggested early on, based on prior observations of familial aggregation [24,25]. Since then, a growing number of studies on the genomic and transcriptomic profiles of WM and IgM-MGUS have pointed out the complexity of these hematological diseases [10]. Although clearly associated with del(6q21) and del(13q14), the relatively low frequencies (40% and 10% respectively) of these aberrations and their detectability in other B-cell lymphoproliferative disorders (i.e., chronic lymphocytic leukemia (CLL) or multiple myeloma (MM)) did not allow for their straightforward use in WM diagnosis [11,26]. In 2012, the first whole-genome sequencing (WGS) study by Treon et al. revolutionized genetic insights by demonstrating a somatic mutation in myeloid differentiation primary response 88 gene (MYD88^L265P) in 90% of WM and 10% of IgM-MGUS cases [27]. These findings were soon reproduced in larger patient series, and increasingly sensitive methods confirmed the presence of MYD88^L265P in more than 95% of WM patients. Moreover, WGS identified several other highly prevalent somatic mutations in CXCR4 (CXCR4^WHIM or CXCR4^MUT) and ARID1A genes [27,28]. Of note, genetic factors have not yet been included in the current diagnostic and prognostic (International Prognostic Scoring System (IPSS)) criteria of WM [29,30]. Besides mutational profile, different classes of coding and non-coding RNA have also increasingly been investigated as these molecules may have crucial roles in disease onset and progression by regulating gene expression and cellular function, and may serve as potential biomarkers [31,32,33].

In recent years, liquid biopsy has been proposed as an alternative to invasive tissue biopsy [34,35,36]. Potential advantages include its minimally invasive nature, its ability to reflect spatial inter- and intra-tumor heterogeneity and the possibility to provide longitudinal monitoring through repeated sampling [37]. The development and use of circulating, reliable biomarkers through liquid biopsy sampling for the diagnosis, therapy response prediction and prognostication of WM could significantly impact daily clinical practice. However, critical challenges such as method standardization and sensitivity must be overcome to facilitate its translation from bench to bedside.

This review aims to present current knowledge regarding nucleic acid biomarkers in WM and IgM-MGUS to elucidate their role and highlight their translational potential as precision medicine biomarkers. Moreover, the biological mechanisms thought to be involved in IgM-MGUS to WM progression will be highlighted.

2. DNA Biomarkers

2.1. The Hallmark Genomic Alterations

2.1.1. MYD88^L265P and CXCR4^MUT

The most noteworthy finding in WM has been the discovery of two activating somatic mutations affecting the MYD88 and CXCR4 genes [27]. MYD88^L265P is the most recurrent mutation in the genomic landscape of WM and is found in approximately 90% of the patients (Table 1).

MYD88 is an adaptor protein that acts downstream of the Toll-like and interleukin-1 receptors (TLR/IL1R), which are both implicated in the innate immune response through a similar signaling cascade [68]. A common characteristic of innate immune receptor signaling is the self-clustering of proteins into oligomeric complexes, known as supramolecular organizing centers (SMOCs) [69,70]. TLR/IL1R activation, through the homotypic TIR domain interactions, triggers the oligomerization of MYD88 and the assembly of a multifunctional organizing center, named MYDDosome [71]. The dynamics of protein recruitment and stepwise assembly of the MYDDosome in TLR/IL1R signal still need to be fully elucidated. Although numerous structural conformations are possible, it has been observed that the size of the MYD88 oligomers (>4 MYD88s) is a decisive factor in the IL1R signal transduction and is crucial for recruiting and binding other post-receptor signal transducers, such as interleukin-1 receptor-associated kinases (IRAK4 and IRAK1) or bruton tirosine kinase (BTK), resulting in sustained NF-κB signaling [71,72]. Notably, it has been shown that the MYD88^L265P mutation, seated in the TIR domain, (and not the other no-L265P mutations) has an increased propensity to build extremely stable oligomers, compared to the wild-type protein, leading the MYDDosome formation and thereby constitutive NF-κB activation, contributing to cell proliferation, cytokine secretion (i.e., TNF, IL-6, IL-1) and malignant cell survival [50,73,74].

Another pro-survival signal supported by MYD88^L265P involves the hematopoietic cell kinase (HCK), a member of the SRC tyrosine kinases family that, when activated by IL-6, triggers signaling through BTK, PI3K/AKT, and MAPK/ERK1/2 [75]. Lastly, WM cells can also transship MYD88^L265P via extracellular vesicles (EV), which prompts inflammatory signaling in the absence of receptor activation and might strongly contribute to a growth-supportive proinflammatory microenvironment [76].

In clinical practice, MYD88^L265P aids in supporting the diagnosis of WM and helps differentiate from other IgM-secreting lymphoid malignancies, such as marginal zone lymphoma (MZL) and IgM multiple myeloma (MM), where it is less frequently mutated or absent, respectively. Moreover, MYD88^L265P is detected in more than 50% of IgM-MGUS patients, 10% of whom can evolve to WM and has been observed that those with a higher mutated allele burden (mutant allele relative to wild type) have a greater risk to progress to WM [40,77]. Of interest, MYD88^L265P by itself does not seem to have primary oncogenic effects, as has recently been demonstrated in mouse models [78,79,80].

Despite having a similar histologic and transcriptional profile, MYD88^L265P and MYD88^WT patients exhibit distinct clinical features and an idiosyncratic genomic profile [81,82]. Indeed, copy number alterations (CNA) are common in MYD88^L265P, as well as the prevalence of other somatic mutations, such as CXCR4^MUT [10,82,83]. In MYD88^WT patients, on the contrary, del(6q) is rare; CXCR4 is usually wildtype, and the genomic profile is characterized by somatic mutations that overlap with those detected in DLBCL, such as TBL1XR1, PTPN13, MALT1, BCL10, NFKB2, NFKBIB, NFKBIZ and UDRL1F (downstream of BTK and IRAK) (Figure 2A) [82].

The second most common somatic mutation, observed in up to 40% of WM patients, occurs in the CXCR4 gene (Table 2) [28,51,84,85]. CXCR4 is a chemokine receptor and member of the 7-transmembrane receptors family, that activates intracellular signaling pathways by binding to heterotrimeric G-proteins through its C-terminus segment [86].

More than 40 non-sense (NS) or frameshift (FS) mutations have been observed in the CXCR4 gene (CXCR4^MUT) [28,87]. The most common variant, representing over 50% of CXCR4 mutations, is a non-sense C > A or C > G transversion in a highly conserved region at nucleotide position 1013, responsible for the generation of a stop codon (S338X), resulting in the loss of 15 amino acids at the C-terminal region of the CXCR4 protein [88,89]. These CXCR4^S338X nonsense mutations affect the expression and activity of CXCR4 mainly through the PI3K-AKT-NF-κB and the MEK1/2 and ERK 1/2 pathways, involved in cell proliferation, migration, and survival [90,91].

Practically all CXCR4^MUT patients harbor MYD88^L265P, suggesting the subclonal nature of CXCR4^MUT with respect to MYD88^L265P acquisition, and only rare cases of CXCR4^MUT/MYD88^WT have been reported (Figure 2A) [28,60,87,93,94]. Moreover, CXCR4^MUT shows a highly variable clonal distribution in WM and IgM-MGUS patients and particularly CXCR4^S338X, as opposed to CXCR4^FS mutations, are associated with complex karyotypes [84,87].

In a recent case study in a CXCR4^MUT patient, WGS highlighted alterations in genes associated with DNA damage repair (DDR) (UVRAG gene), tumor suppression (BTG220, DAB2), chromosome instability (MACROD2, CCSER1), cell cycle regulation (SCAPER) and post-translational protein modifications (LNX1 and DCUN1D4). However, further analysis of 46 WM patients did not show a significantly different distribution of these mutations between CXCR4^WT vs. CXCR4^MUT patients [95].

MYD88^L265P and CXCR4^MUT were initially assessed on CD19+ (CD19-selected cells) BM samples using allele-specific quantitative polymerase chain reaction (AS-qPCR) and Sanger sequencing. Subsequently, many studies have used unselected BM samples and distinct assays and methods with different levels of sensitivity (Table 1 and Table 2). Both mutations can be detected not only in BM, PB (of note, B-cell–depleting agents, particularly rituximab, can greatly decrease mutation detection rate in PB) and plasma but also in skin, cerebrospinal fluid (CSF) and pleural effusions [62,96,97,98].

As of today, a gold standard molecular method for MYD88 and CXCR4 mutation detection is lacking. Although CD19+ cell sorting can improve the mutation detection sensitivity, cell selection is not cost-effective and not applicable to all clinical laboratories [10,27,38,40,43,47,49,60,97]. A recent study demonstrated that in unselected BM samples, AS-qPCR was superior in detecting CXCR4^S338X compared to amplicon massively parallel sequencing (MPS) (63% vs. 16%) [92]. Additionally, sensitivity of both methods was higher for MYD88^L265P detection (98% and 69% respectively), confirming the subclonal nature of CXCR4^S338X but also indicating a direct dependence of MPS performance on the level of BM involvement [58,67,92].

Consistently, a strong correlation between the mutational burden and the number of pathological cells has been demonstrated in unsorted material [40,42]. Therefore, the MYD88^L265P/MYD88^WT ratio might also be proposed as a quantitative marker and useful diagnostic tool for MRD analysis. Recently, digital PCR (dPCR) has been described as more sensitive than AS-qPCR across different specimen types (including plasma-cfDNA), for MYD88^L265P screening and MRD analysis, suggesting that the implementation of dPCR assay in routine diagnostic laboratories might avoid the need for CD19+ selection [62,99].

2.1.2. 6q21 Deletion

Small CNAs involving B-cell regulatory genes are highly prevalent in WM [28]. Paiva et al. showed that the frequency of patients displaying CNAs significantly increased with disease stage (IgM-MGUS (36%), aWM (73%) and WM (82%)) [100].

The 6q21 deletion (del(6q)) is the most frequent cytogenetic aberration and is detected by fluorescence in situ hybridization (FISH) in up to 30–50% of WM cases [83,101,102,103,104]. Other less frequent cytogenetics abnormalities include del13q (15%), trisomy 18 (10%), trisomy 4 and del17p (8%) (Figure 2B) [26,105,106]. Chromosome 6q deletion, mostly from q14 to q27, contains negative regulators of the MYD88/NFκB pathway (BLIMP1, TNFAIP3, HIVEP2, TRAF3IP2, IRAK1BP1), BTK inhibitors (IBTK) as well as controllers of apoptosis and differentiation (FOXO3, BCLAF1, PERP) [21,83,107,108,109].

So far, limited and discordant data linking molecular and cytogenetic information are available. Despite the initial observation that del(6q) and CXCR4 mutations are mutually exclusive, conflicting data have been reported [83,84,103]. In a cohort of 219 patients, Krzisch et al. found that 35% of del(6q) cases harbored CXCR4 mutations, as detected by chromosomal banding analysis (CBA), FISH, and targeted MPS. Moreover, a significantly more complex karyotype was shown in patients with del(6q) [110].

Cytogenetic studies may be useful to detect del(6q) as well as other abnormalities that might aid in differential diagnosis and outcome prediction [26]. However, the difficulty to obtain tumor metaphases in vitro due to the low mitotic index of the tumor cells and the need for CD19+ BM cells selection hampers the employment of CAB and FISH analysis for routine diagnostic assessment in WM patients.

2.2. Infrequent DNA Mutations

Albeit at low frequency, other recurring somatic mutations have been reported, including ARID1A (17%), CD79B, KMT2D (or MLL2), MYBBP1A and TP53 (<15% of cases each) (Table 3, Figure 2C) [26,27,28].

Using MPS in a large series of WM and IgM-MGUS patients, Varettoni et al. (2017) demonstrated subclonal mutations in KMT2D (16%), TP53 (8%), NOTCH2 (7%), PRDM1 (4%), ARID1A (3%), CD79B (3%) and TRAF3 (1%), while no mutations were found in MYBBP1A and TNFAIP3 [10]. Of note, the median number of KMT2D mutations was significantly higher in WM compared to IgM-MGUS patients. A subsequent study evaluating the 12 most frequently mutated genes confirmed an increased mutational load in different stages of monoclonal gammopathies: 21% in IgM-MGUS (additional mutations in at least 1/12 genes), 35% in aWM (by 8/12 genes) and 50% in symptomatic WM (by 12/12 genes) [93]. A recent study by Roos-Wiel et al. identified a novel recurring activating somatic mutation (p.Q226E) in the hematopoietic transcription factor SPI1 in 6% of patients, leading to altered gene expression programs responsible for oncogenic proliferative signaling and for blocking B cell differentiation [112]. This finding has been supported in a larger series of WM patients [110].

2.3. Impact of Somatic Mutations on Outcome and Therapy Response

It has been widely demonstrated that MYD88 and CXCR4 mutations have both diagnostic and therapeutic implications in WM. So far, four distinct subsets of WM patients with peculiar clinical features, different outcomes and drug responses have been identified: MYD88^L265P/CXCR4^MUT, MYD88^L265P/CXCR4^WT, MYD88^WT/CXCR4^WT and MYD88^WT/CXCR4^MUT.

MYD88^L265P/CXCR4^S388X patients show a higher BM disease burden, higher serum IgM levels and are more likely to have symptomatic disease compared to MYD88^L265P/CXCR4^FS-MUT, MYD88^L265P/CXCR4^WT or MYD88^WT/CXCR4^WT patients that show respectively a lower and the lowest (WT/WT) BM disease involvement. Discordances between studies in WM have been reported, but the most supported observation is that MYD88^L265P/CXCR4^MUT patients show lower, later and less deep responses to BTK inhibitors (mainly ibrutinib), eventually resulting in shorter PFS compared to MYD88^L265P/CXCR4^WT patients [61,113]. MYD88^WT/CXCR4^WT cases, on the other hand, show resistance to targeted drugs (i.e., BTK-inhibitors, but also PI3K and mTOR inhibitors) and are characterized by an increased risk of disease transformation to high-grade lymphoma or of developing a therapy-related myelodysplastic syndrome (t-MDS), both leading to a poor OS [61,114,115]. Additionally, MYD88^WT patients with DDR mutations represent a subgroup with ultra-high-risk disease [82,114]. Lastly, outcome and therapy response are still a challenge to face in the small subgroup of MYD88^WT/CXCR4^MUT patients [116].

Recently, multicenter phase II and III trials comparing the efficacy and safety of novel BTK inhibitors to ibrutinib, hinted at a higher efficacy of acalabrutinib and zanubrutinib in a small subset of MYD88^WT patients, by showing overall and major response (at least a partial response [PR]) rates comparable to MYD88^L265P cases [117,118,119]. However, both the heterogeneity of the methods adopted for mutation detection (from Sanger to targeted MPS), and the low limit of detection (0.5%), could have led to a misclassification of patients with a mutation level below the sensitivity of the employed methods [119]. Therefore, additional, more standardized studies, as well as longer follow-up cohorts are needed to better clarify the real impact of novel BTK-inhibitors in molecularly-driven subgroups of WM patients.

Within the uncommon mutations, ARID1A mutations are associated with greater tumor involvement [115]. Mutations in CD79B are mainly observed in MYD88^L265P/CXCR4^MUT patients, with the exception of two studies in which the co-expression of CD79B and MYD88^L265P/CXCR4^WT was associated with disease transformation and progression [84,120]. Despite being rare, trisomy 4, SPI1 and TP53 mutations have been associated with aggressive disease course and shorter OS. Data concerning the coexistence of TP53 mutations with both MYD88^L265P and CXCR4^MUT and the activity of ibrutinib in this group of patients are conflicting [110,111,121]. The few available studies regarding the impact of cytogenetic abnormalities in WM reported shorter progression-free survival (PFS) in del17p patients, as well as more symptomatic disease, shorter time to treatment and poorer clinical outcomes (both PFS and OS) in del6q cases [26,83,100,103,105,110].

3. RNA Biomarkers

Approximately 80% of the human genome is transcribed into RNA, of which only 1.5% is protein-coding mRNA, with the rest being termed non-coding RNA (ncRNA). Current classifications differentiate between short ncRNAs (less than 200 nucleotides, including miRNAs) and large ncRNAs (larger than 200 bases, generally termed lncRNAs, but also including circRNAs) [122]. RNA molecules have unique properties that make them attractive potential biomarkers. Since these molecules mediate or influence intercellular communication, they may lead to an improved understanding of differentially expressed key pathways involved in lymphoma initiation and transformation. Moreover, the dynamics of RNA patterns may reflect functional, longitudinal changes in both the tumor and the non-malignant compartment during disease course or treatment.

3.1. Coding mRNA

Gene expression profiling studies showed that lymphoplasmacytic WM cells (CD138+/CD19+) have a homogeneous transcription profile with an mRNA signature that resembles CLL and normal B cells but clearly differs from MM and normal plasma cells (NPC). Both WM and CLL are indolent lymphomas that are likely to be derived from memory B-cells, which might explain the similar B-cell-like signature [123,124]. Among the 73 genes differentially expressed in WM compared to CLL and MM, IL-6 was most significantly upregulated. Increased IL-6 mRNA and protein levels have been reported in other studies and are thought to promote IgM secretion and WM cell growth [125,126,127,128]. Gene ontology analysis based on WM unique genes showed activation of the MAPK pathway, which is also involved in IL-6 signaling [124]. By targeting IL-6 with tocilizumab, a reduction in tumor growth rate and IgM secretion has been demonstrated in vivo [129]. These results support its role in the WM tumor microenvironment (TME) and its potential as a therapeutic target.

As the WM clone is comprised of B lineage cells ranging from B lymphocytes (BL) to plasma cells (PC), several studies have compared separate expression profiles of clonal CD19+ WM B-cells (WM-BL) and CD138+ WM plasma cells (WM-PC) with their respective normal counterparts (NBL and NPC, respectively). Using MPS, Hunter et al. presented the first transcriptional landscape of WM-BL compared to NBL. Upregulated genes included RAG1, RAG2, DNTT and IGLL1, involved in VDJ recombination, BCR signaling and somatic mutation. The class switch recombination gene AICDA was not observed, which is consistent with the lack of immunoglobulin class switching. Furthermore, upregulation of CXCR4 and its ligand CXCL12 have been reported to increase cell adhesion to VCAM1, which might explain the homotypic cell clustering in WM patients [104]. Gutiérrez et al. identified a total of 171 and 498 genes that were differentially expressed between WM-BL and WM-PC compared to NBL and NPC, respectively. Further analysis illustrated the aberrant differentiation of clonal BL into PC by identifying 37 genes, including PAX5, whose expression level in WM-PC was intermediate between WM-BL on the one hand and MM-PC/NPC on the other hand. CD79, BLNK and SYK, all targets of PAX5 and characteristic markers of B lymphoid cell identity, were upregulated in WM-PC, with an expression level more similar to WM-BL. BLIMP1 and IRF4 levels, which play crucial roles in PC differentiation, were decreased in WM-PC compared to MM-PC/NPC. These data suggest that lower PAX5 repression in WM-PC attributes to its phenotypic pattern of intermediate features between clonal BL and PC. This is in line with the finding that most genes that were exclusively dysregulated in WM-PC compared to MM-PC and NPC were also overexpressed in WM-BL, further suggesting that WM-PC results from an incomplete maturation process of clonal BL [128]. Of interest, another study could not identify a higher similarity between WM cells and normal memory B-cells compared to peripheral B-cells [104]. Lastly, Gaudette et al. showed that dysregulation of BCL-2 family members could help in discriminating between B-cell-like phenotype (WM-BL, NBL and CLL) and PC phenotype (WM-PC, NPC and MM), illustrating that its expression may be driven by the state of differentiation. WM-PC cells expressed BCL-2 family proteins at levels more similar to NPC than MM, which is indicative of a higher apoptotic threshold in WM cells [130]. Increased expression of the antiapoptotic gene BCL-2, as well as a decreased level of proapoptotic BAX, have been previously reported [104].

Regarding the impact of recurrent genetic alterations on transcriptional regulation, a study showed that expression profiles in MYD88^WT patients were relatively heterogeneous with downregulation of NF-κB signaling-associated genes and upregulation of PIK3 signaling. Of the 1155 genes that were differentially expressed between MYD88^L265P and MYD88^WT patients, only 603 were identified in the MYD88^L265P/CXCR4^WT vs. MYD88^L265P/CXCR4^WHIM signature. As CXCR4^WHIM mutations are found almost exclusively in MYD88^L265P patients, CXCR4^WHIM mutations appear to counteract tumor suppressor upregulation in response to mutant MYD88^L265P signaling, as evidenced by the normalization for TLR4 signaling associated gene expression and upregulation of IRAK3. In the MYD88^L265P/CXCR4^WT genotype, a marked increase of GPER1, WNT5A, IGF1 and IL17RB expression was shown, in which IL17RB and IGF1 activate NF-κB and AKT1/MAPK signaling, respectively [104,131]. The strongest gene markers for MYD88^L265P/CXCR4^WHIM patients were the upregulation of CXCR7 and TSPAN33, as well as suppression of IL-15 [104]. Concerning 6q deletions, Chng et al. found no differentially expressed genes between deleted and non-deleted cases [124]. This is in contrast with the study of Hunter et al. that included a larger number of WM samples, and demonstrated that 6q deletions were associated with over 131 differentially expressed genes, including suppression of the NF-κB negative regulator HIVEP2, as well as BCLAF1, FOXO3 and ARID1B [104].

Regarding their potential use as biomarkers in WM, a study has shown that the level of mRNA expression was greatly dependent on the extent of BM involvement, with the expression profile of cases with low infiltration, clustering with normal plasmacytes [124]. In the same vein, one study showed that many genes relevant to WM biology, including CXCL13, TP53, CXCR4, MYD88, CDC23 and AKAP1 were significantly associated with BM disease involvement [104] (Table 4).

3.2. Non-Coding RNA

3.2.1. miRNA

MicroRNAs (miRNAs) are short non-coding RNAs of ~22 nucleotides that play essential roles in almost all biological pathways, negatively regulating gene expression by targeting mRNA, typically at the 3′-untranslated region. Since miRNAs can target up to several hundred mRNAs, aberrant expression can influence a multitude of cell signaling pathways, including cancer onset and progression [31]. Several papers have investigated the role of miRNAs in WM/IgM-MGUS and their potential use as biomarkers (Table 5).

3.2.2. Diagnostic Markers

Bouyssou et al. have shown that a 12-miRNA signature from extracellular vesicles was able to discriminate asymptomatic WM patients from healthy controls [138]. Hunter et al. identified 10 miRNAs that were differentially expressed in WM, of which five target the IRS-PI3K signaling pathway that plays a role in the growth and survival of WM cells: miR-29c (PIK3R1); miR-155 (SHIP1); miR-21 (PTEN, PDCD4); miR-145 (IRS1); and miR-126-3p (IRS1, PIK3R2) [132]. The combination of increased miR-320a and miR-320b levels as well as decreased miR-151-5p and let-7a levels has also been shown to distinguish WM from healthy controls, with the latter acting as a tumor suppressor by regulating different oncogenes such as MYC [140,142]. Fulciniti et al. have shown a decreased miR-23b expression in WM and identified an MYC/miR-23b/SP1 feed-forward loop, in which c-MYC acts jointly with SP1 to downregulate miR-23b expression [136]. Gain of function studies showed a decrease in cell proliferation and lower colony formation ability, indicating a tumor suppressor role by reducing SP1-driven NF-κB activity. Treatment with IL-6 or supernatant from BM stromal cells resulted in a further decrease in miR-23b levels, illustrating the role of the human bone marrow TME in its expression [136].

Roccaro et al. identified a WM-specific miRNA signature characterized by increased expression of miR-363-5p/-206/-494/-155/-184/-542-3p, and decreased expression of miR-9-3p [135]. Decreased miR-9-3p and increased miRNA-155 levels have been associated with WM in other studies [132,137,139]. MiR-9-3p acts as a tumor suppressor by targeting protein kinases, oncogenes and transcription factors, thereby enhancing apoptosis as well as inhibiting B-cell differentiation and proliferation. Members of the miR-9 families are known to downregulate PRDM1, a significant regulator of B-cell development [139]. MiR-155 is also involved in essential pathways in different B-cell malignancies, including WM, targeting both AKT and NF-κB signaling pathways [131,143]. In two studies performing miR-155 LNA knockdown in WM cells, the role of miRNA-155 in WM proliferation and growth was confirmed in vitro and in vivo by targeting critical signaling cascades such as MAPK/ERK, PI3/AKT and NF-κB, which are involved in cell-cycle progression, adhesion, and migration [135,144]. Interestingly, stromal cells from miR-155-knockout mice led to significant inhibition of tumor growth, which suggests a role of miR-155 in WM proliferation both in the tumor and in the TME. Gene expression profiling revealed three known miR-155 targets (SMAD5, SOCS1 and CEBPβ) as well as three novel targets (MAFB, SHANK2, and SH3PXD2A) [144]. Gaudette et al. observed a decreased FOXO3 transcription factor and pro-apoptotic BCL2L11 in cells with augmented miR-155-5p expression, hereby blocking apoptosis. Furthermore, mitochondrial priming can be induced by antagonism of miR-155, lowering the apoptosis threshold [130]. Lastly, miR-155 regulates proliferation through the cell-cycle transition. In miR-155 knockdown WM cells, G1 to S phase transition was blocked and associated with elevated transcripts for p53, p63 and p73, potentially providing a crucial alternate mechanism of cell growth arrest in the absence of p53. [135]. Figure 3 shows an illustrative overview of the pathways involved with increased miR-155 expression in WM.

Hodge et al. investigated specific miRNA signatures of different WM cellular subgroups. The miRNA signature of WM-BL consisted of mostly downregulated miRNAs compared to CLL and non-malignant B-cells, including miR-151, miR-335 and miR-342, whereas miR-373 was clearly increased in WM-BL. Most WM-PC clustered with MM-PC, yet retained a distinct miRNA profile of their own, characterized by the increased expression of more than 40 candidate miRNAs. No differentially expressed miRNA was detected between WM-BL and WM-PC, and no clear signature for lymphoplasmacytic (CD19+/CD138+) WM cells could be identified, possibly due to the clone’s morphologic diversity, sharing features of both BL and PC. After combining WM-BL, WM-PC and lymphoplasmacytic cells to mimic the heterogeneity observed in WM tumors, six miRNAs were differentially expressed in WM compared to nonmalignant B lineage cells (decreased expression of miR-152, miR-182, miR-373-5p and miR-575, with the opposite pattern for miR-21 and miR-142-3p) [139].

3.2.3. Therapy Response and Prognostic Marker

Increased expression levels of miR-192-5p, miR-21-5p and miR-320b have been associated with disease progression, while expression of let-7d decreased with disease stage [138]. Increased expression of another 6-miRNA-signature (miR363-5p/206/494/155/184/542-3p) was associated with worse prognosis, predicted by the IPSS [135,145]. Treatment with rituximab, perifosine and bortezomib affected the expressions of the identified miRNAs (except miRNA-206), indicating the role of these miRNAs as therapy response predictors and possible targets for treatment [135]. Caivano et al. showed a trend for a positive association between a high EV miR-155 level and an intermediate-high IPSS score. More data are, however, needed to confirm these results [137].

Roccaro et al. illustrated ex vivo that everolimus targeted mTOR downstream signaling pathways in responders. Furthermore, everolimus induced toxicity, supported by cell-cycle arrest and caspase-dependent and -independent induction of apoptosis, even in the context of BM milieu, affecting migration, adhesion and angiogenesis. Through miR-155 loss-of-function studies, everolimus-dependent anti-WM activity was shown to be partially driven by targeting miR-155 [141]. It has been well documented that miR-155 targets SHIP1, which acts as a negative regulator of the PI3K/AKT and mTOR pathway [146]. Moreover, everolimus synergized with bortezomib and rituximab in targeting WM cells, as shown by synergistic inhibition of NF-κB/p65 activity and p-S6R, respectively—the latter through enhanced antibody-dependent cellular cytotoxicity. These results may support a rationale for combining everolimus with bortezomib or rituximab in certain patients that are refractory to everolimus monotherapy, as well as the use of miR-155 as a biomarker for therapy response prediction [141] (Table 5).

3.2.4. miRNAs and Epigenetic Regulation

Besides genomic losses, epigenetic alternation represents the major mechanism by which gene expression is regulated and includes DNA methylation, histone acetylation and miRNA regulation [147]. A subgroup of miRNAs, called epi-miRNAs, actively modulate epigenetic processes via targeting mRNAs encoding methylating and acetylating enzymes. Histone acetylation is commonly deregulated through alterations in the balance between histone acetyltransferase (HAT) anddeacetylase (HDAC) activity, leading to enhanced gene transcription. Its role has been illustrated in various solid and hematological malignancies [148,149,150].

Roccaro et al. demonstrated that reduced expression of miR-9-3p and increased expression of miR-206-3p resulted in an unbalanced expression of HATs and HDACs at mRNA level in WM-BL, suggesting that histone modification plays a role in the pathogenesis. Specifically, miR-206-3p was found to target HAT KAT6A and miR-9-3p to target HDAC4 and HDAC5. Restoring miR-9-3p levels resulted in induction of toxicity in WM cells, supported by downmodulation of HDAC4 and HDAC5 and upregulation of acetylhistone-H3 and -H4, which led to induction of apoptosis and autophagy [133]. As mentioned, increased expression levels of miR-15a-5p and miR-16-5p have been found in WM patients [138]. In CLL, it has been shown that HDACs overexpression mediates the epigenetic silencing of miR-15a and miR-16. HDAC inhibition-induced expression of miR-15a and miR-16 was associated with decreased Mcl-1 levels, mitochondrial dysfunction and induction of cell death in CLL cells [151]. Furthermore, miR-15a has also been shown to target p53 in a miRNA/p53 feedback circuitry [152]. In MM, microRNA-15a/-16 regulates proliferation and growth of MM cells in vitro and in vivo by inhibiting AKT serine/threonine-protein-kinase (AKT3), ribosomal-protein-S6, MAP-kinases and NF-κB-activator MAP3KIP3 [153]. Del(13q14), which includes the miR-15a-5p/16-5p locus, has been described in 10% of WM patients [3]. Future research could focus on the role of these (epi)miRNAs and their interaction with dysregulated histone acetylation in WM.

In recent years, there has been increased interest in targeting epigenetic modulators by small molecule inhibitors. Different HDAC inhibitors (SAHA, TSA, panobinostat (LBH-589), and sirtinol) demonstrated dose-dependent killing and had at least additive antitumor effects when combined with bortezomib in a WM cell line [134]. In a phase two trial of panobinostat in relapsed/refractory WM patients, partial remission and minimal response were seen in 22% and 25% of cases, respectively. In addition, 50% of patients achieved stable disease and none showed progression while on therapy [154]. BET inhibitors are another class of molecules that inhibit cell proliferation by targeting bromodomain proteins (BRD2, BRD3, BRD4 and BRDT), resulting in decreased MYC expression through transcriptional regulation. A recent study that investigated two BET inhibitors (iBET and JQ1) in WM showed reduced cell proliferation in a dose-dependent manner. There was only a moderate effect on cell viability, which may be explained by increased anti-apoptotic BCL-2 expression, suggesting that targeting BCL-2 may be effective in inducing WM cell death. Indeed, combined treatment of JQ1 and venetoclax enhanced apoptosis. Notably, the efficacy was not compromised in the presence of the TME. Moreover, BET inhibitors were also shown to decrease stromal cell proliferation. This suggests that BET inhibition may influence the epigenetic regulation of both the tumor and the TME. When HDAC and BET inhibitors were combined, synergistic effects on cell death were shown, even with a very low dose of panobinostat (LBH589) [155].

3.2.5. LncRNAs

Long non-coding RNAs (lncRNAs) are a large and heterogeneous class of non-coding transcripts, greater than 200 nucleotides in length. Based on their relative positions to protein-coding genes, lncRNAs are commonly classified as intergenic, intronic, sense overlapping or antisense overlapping [156]. Although their function is still largely unknown, lncRNAs play essential roles in cellular and physiological processes, such as chromatin remodeling, transcriptional regulation, and posttranscriptional modification [32]. Aberrant expression, mutations and SNPs in an increasing number of lncRNAs have been found to be involved in tumorigenesis and metastasis. Their tumor-specificity as well as their stability in circulating body fluids make them attractive potential biomarkers and therapy targets [157].

To date, lncRNA expression in WM has not yet been investigated. In CLL and MM, however, dysregulation of multiple lncRNAs has been shown. In CLL, DLEU2 [158], BM742401 [159] and lincRNA-p21 [160,161] act as tumor suppressors, respectively, by regulating NF-κB signaling and via induction by p53. BIC acts as an oncomiR progenitor by being a host of miR-155 [162] and MIAT by forming a regulatory loop with OCT4 [163]. Other dysregulated lncRNAs with a currently unelucidated mode of action include ZNF667-AS1/lnc-AC004696.1-1, lnc-IRF2-3, and lnc-KIAA1755-4 [164]. In MM, iGAS5 [161,165], DLEU2 [158] and MEG3 [166] have been described as tumor suppressors, respectively, by regulating the mTOR pathway, being host of the miR-15a/16-1 cluster and regulating p53 gene expression. MALAT1 and TUG1 have been reported to act as oncogenes by respectively regulating the bioavailability of TGF-β and affecting the expression of cell cycle regulatory genes by binding PRC2 [161]. Dysregulation of Lnc-SENP5-4/NCBP2-AS2, lnc-CPSF2-2, lnc-LRRC47-1/TP73-AS1, lnc-ANGPTL1-3 and lnc-WHSC2-2 have also been shown in MM, although their function remains unclear [165]. One study reported lower levels of HOTAIR, an epigenetic regulator of chromatin and known oncogene in different solid tumors, in MM patients [161]. Further research, however, is needed to elucidate its role in MM. Lastly, increased lncRNA H19 levels were detected in the serum of (bortezomib resistant) MM patients, which was associated with the disease- and ISS stage. H19 sponges miR-29b-3p, hereby enhancing MCL-1 transcriptional translation and inhibiting apoptosis [167,168]. Since MM and CLL are B-cell neoplasms closely related to WM, the aforementioned lncRNAs could be further investigated. For example, dissecting the role of the DLEU2/miR-15a/16-1 cluster, which is located on chromosome 13q14.3, a region known to be involved in CLL, MM and WM could produce valuable new insights.

3.2.6. CircRNAs

Circular RNAs (circRNAs) are a more recently discovered subclass of large ncRNA, with covalently closed ends and lengths between ~100 to thousands of nucleotides. CircRNAs originate from a host gene and are formed through a backsplicing event, ligating the 3′ end of an exon to the 5′ end of the same or an upstream exon. Being highly evolutionary conserved, circRNAs may function as direct or indirect regulators of host gene expression at the transcriptional level, as sponges or decoys for miRNAs or RNA binding proteins, regulators of protein translation or under certain circumstances even as templates for translation. Altered expression has been shown in different solid and hematological cancers and increasing evidence shows that circRNAs can be used as reliable (cell-free) biomarkers, as they are present in different human body fluids, are highly tissue-specific and are more resistant to exonucleases due to their closed structure [33,169].

To date, differential expression of circRNAs has not been studied in WM. In CLL, circRPL15 has recently been shown to sponge miR-146b-3p, thereby increasing RAF1 levels, activating MAPK signaling and promoting cell growth [170]. Upregulation of circCBFB activates the Wnt/β-catenin pathway by binding miR-607 and thereby derepressing production of FZD3, stimulating proliferation [171]. Moreover, both circRNAs have been associated with worse OS [170,171]. Circ_0132266 acts as a tumor suppressor by sponging miR-337-3p, resulting in increased levels of PML, a known regulator of gene expression and cell viability [172]. In MM, 619 unique circRNAs were identified in a MM cell line through RNA sequencing, including circSMARCA5, circRP11-255H23.2, circIKZF3, circCD11A (ITGAL), and circWHSC1 (MMSET) [173]. CircSMARCA5 has a tumor repressor role by binding to miR-767-5p, thereby inhibiting cell proliferation and promoting apoptosis. Increased expression is associated with a higher complete remission rate, as well as improved PFS and OS [174]. Circ_0000190 also acts as a tumor suppressor by sponging miR-767-5p, which in turn prevents the repression of its target MAPK4, slowing down progression. Upregulation of circ_000190 was associated with longer PFS and improved OS [175]. As the circRNA spectrum in WM is currently uncharted territory, elucidating their expression and function could produce valuable insights into the pathogenesis and identify potential disease-specific biomarkers.

4. IgM-MGUS to WM Progression

Patients with IgM-MGUS have a significantly lower number of mutations than patients with WM. The high prevalence of MYD88^L265P in IgM-MGUS patients (50–80%) suggests that this somatic mutation is most likely an early oncogenic driver (Table 1). Meanwhile, the low prevalence of CXCR4, KMT2D and TP53 mutations (<10%), which usually occur in a later stage, indicates that MYD88^L265P by itself is insufficient to explain the malignant transformation from IgM-MGUS to WM [10]. Multistep genetic and/or microenvironment changes might lead to the progression of IgM-MGUS to WM. Although several clinical studies have identified biomarkers associated with a higher risk of IgM-MGUS to WM progression [176,177,178,179], no reliable molecular markers have been defined and the biological mechanisms driving the progression between these two entities are still unknown. Extensive transcriptome gene expression analysis using microarrays on CD19+ and CD138+ cells of WM and IgM-MGUS samples demonstrated that BLs and PCs harbor distinct molecular signatures [180]. A more recent study identified a common gene set signature that characterizes B-cells of WM and IgM-MGUS subjects, compared to healthy donors. This set of nine genes (HIST1H1B, EZH2, CHECK1, LEF1, ADAM23, RASGRP3, ADRB2, PIK3AP1, CDHR3) might highlight new candidate markers in IgM-MGUS responsible for the risk of progression to WM [181]. Furthermore, several studies have investigated the difference in miRNA expression signatures between IgM-MGUS, aWM and WM. Bouyssou et al. found no differential expression between aWM, WM and relapsed WM patients, suggesting that (exosomal) miRNA changes may occur in an early stage [138]. The assumption that a subset of IgM-MGUS can be regarded as the precursor state of WM is further supported by a study that showed a similar mRNA expression profile between an IgM-MGUS case and WM, suggesting a shared phenotype [124]. The combination of miR-320a and miR-320b was, however, able to distinguish WM from IgM-MGUS and IgM-MM, and decreased levels of miR-320a were significantly associated with MYD88^L265P. As levels of miR-320a negatively correlated with lymphoplasmacytic cells infiltration in the BM, the expression profiles in samples with higher BM involvement were more similar to their malignant counterparts, whereas patients with less involvement had samples that tended to cluster with the respective non-malignant cells [140].

5. Liquid Biopsy

Liquid biopsy is the process of investigating tumor-derived cells, cell-free nucleic acids, metabolites, proteins or extracellular vesicles through biofluid sampling without the need for tissue biopsy. Biological sources for liquid biopsy include PB, urine, cerebrospinal fluid, saliva and pleural effusions, among other body fluids [182].

In the past decade, there have been major advances in the identification of diagnostic, phenotype-defining and prognostic biomarkers in lymphoproliferative diseases, which might complement current classification and prognostic tools, as well as guide therapy choice in a precision medicine approach [183,184]. In blood-derived liquid biopsies, circulating cell-free tumor DNA (ctDNA) and RNA (ctRNA), circulating tumor cells (CTCs), and extracellular vesicles are released into the PB, reflecting the tumor-specific genetic profile of the primary tissue biopsy, as reported by independent studies in hematological malignancies [184,185,186].

Potential advantages of liquid biopsy include its minimally invasive nature, its ability to reflect spatial inter- and intra-tumor heterogeneity and the possibility of longitudinal profiling. To date, however, their analysis has only been implemented as a therapy decision-maker in solid tumors [187,188].

In WM, ctDNA may represent a reliable “echo” of the tumor-specific genomic and epigenomic aberrations of the BM compartment, and even of extramedullary sites, and might be useful in assessing disease status, guiding therapeutic decisions and monitoring minimal residual disease (MRD) (Figure 4).

To this day, only a few studies have investigated the use of cfDNA in the characterization of the mutational landscape of patients with IgM monoclonal gammopathies.

A pioneering study by Bagratuni et al. compared the mutational status of MYD88 and CXCR4 in paired gDNA (from BM CD19+ selected cells) and cfDNA samples of patients with IgM monoclonal gammopathies. Qualitative allele-specific PCR and direct sequencing showed an overall concordance rate, between gDNA and cfDNA, of 94% and 90% for the most common MYD88 and CXCR4 mutations, respectively. These results were consistent among patient subgroups according to disease status (IgM MGUS, aWM, newly diagnosed WM, relapsed/refractory WM and WM in remission) [189]. A subsequent study by Wu et al., comparing BM and cfDNA data from WM patients for MYD88^L265P and CXCR4^S338X mutations by AS-qPCR, revealed only one discordance, related to an aWM patient with a slight BM infiltration [65]. Similarly, Demos et al. validated cfDNA for MYD88^L265P and CXCR4^S338X against CD19-selected and unselected BM and PB tissue fractions, strengthening the evidence that cfDNA can reliably be used to identify these two most common variants in WM patients [190]. Of note, the former studies have reported conflicting data regarding the correlations between BM infiltration, serum IgM levels and the concentrations of cfDNA [65,189,190]. Likewise, Drandi et al. demonstrated the feasibility of cfDNA analysis by dPCR in detecting MYD88^L265P mutation in paired unselected BM and cfDNA samples from 60 WM patients. Their MYD88^L265P dPCR assay showed an overall mutation detection rate on baseline unselected mononuclear cells samples of 95.3% in BM and 71.2% in PB. Interestingly, dPCR detected a log10 higher median MYD88^L265P mutated/WT ratio in ctDNA compared to PB, while no statistically significant difference was observed between ctDNA and BM samples [62]. These data may contribute to the still open debate on whether to use sorted versus unsorted BM mononuclear cells to assess MYD88^L265P mutation (Table 6).

Up to now, there is a lack of consensus regarding the optimal specimen and analytical method for mutational detection in WM, in terms of operating procedures, test sensitivity and result interpretation [99,192]. Researchers must be aware that differences in method sensitivity may lead to both a misclassification of disease status and an overestimation of the efficacy of novel treatments. In a recent publication, different PCR methods (qPCR vs. dPCR) have been compared in BM, PB, CD19+ and cfDNA samples: dPCR appeared to be the most sensitive approach for MYD88 detection. Moreover, an algorithm was provided to suggest the most convenient PCR method based on available specimens and laboratory equipment [99]. Although highly relevant and promising, we are aware that the available data are premature to establish cfDNA as a single approach for disease screening and monitoring. Moreover, standardization of pre-analytical and analytical processes must be performed before integrating cfDNA analysis into the clinical practice. Currently, a multicenter clinical trial for non-invasive diagnostics and monitoring of MRD in WM and IgM-MGUS patients is ongoing (BIO-WM trial: NCT03521516), with the primary endpoint of demonstrating that the MYD88^L265P mutation rate detected in cfDNA by dPCR is equivalent to the rate detected in BM.

Although most studies have focused on cfDNA, there has been an increased interest in different forms of circulating-free RNA biomarkers. Several mechanisms, such as encapsulation within extracellular vesicles (EVs) or ribonucleoprotein RNA-binding proteins complexes, protect circulating-free RNAs (cfRNA) from nuclease activity. Although the source and function of cfRNAs remain largely unknown, RNAs seem to be selectively packaged according to the viability and origin of the cells. Living cells seem to actively release RNA encased in large lipoprotein complexes, such as exosomes or microvesicles, while circulating RNA from dying cells is enclosed within apoptotic bodies or bound in protein complexes [193]. Besides RNA, EVs encapsulate different cellular components such as proteins, lipids, carbohydrates and DNA, thereby protecting them from degradation [194]. In different hematological malignancies, including WM, increased levels of EVs have been demonstrated. EVs have been shown to express malignancy-associated surface markers and to positively correlate with prognostic scores such as IPSS [195]. Furthermore, precursor miRNAs can be processed into mature miRNAs inside tumor-derived exosomes carrying the microRNA biogenesis machinery [196]. Recently, Mancek-Keber et al. highlighted an interesting role of EVs in lymphoma progression. Once EVs are internalized by the recipient cells, the transferred MYD88^L265P recruits MYD88^WT and triggers the activation of the NF-kB and the inflammatory pathway, both important for WM pathogenesis [76].

In WM, three studies have investigated circulating EV-derived miRNA expression and showed an upregulation of miR-192-5p, miR-93-5p, miR-15a-5p, miR-16-5p, miR-20a-5p, miR-378a-3p and miR-155 and a downregulation of miR-199a-5p, miR-145-5p, miR199a-3p, miR-221-3p, miR-335-5p, let-7d-5p, miR-320a-3p, miR-320b-3p, miR-151-5p and let-7a-5p, compared to healthy controls [137,138,140]. Moreover, increasing levels of miR-21-5p, miR-192-5p, miR-320b-3 and decreasing levels of let-7d-5p have been significantly associated with disease progression [138]. In the study of Kubizkova et al., both miR-320a and miR-320b were present in exosomes as well as in exosome-depleted samples. Interestingly, their levels tended to be enriched in exosomal fractions, which may indicate active transportation in EVs [140]. The study of Bouyssou et al. showed a lower correlation between miRNA expression in tumor cells and circulating exosomes derived from patient samples as compared to the correlation between miRNA levels of the cellular and exosomal fractions in WM cell lines. This may be explained by the presence of exosomes derived from various cell types including tumor cells, microenvironment cells and immune cells in the PB. Besides tumor-derived content, EV-derived miRNAs may therefore provide additional insights into changes in the TME and immune response during treatment [138]. The role of the TME is increasingly being recognized as a crucial factor in the pathogenesis of several B-cell malignancies, including WM, and to play a protective role in resistance to therapy [131,197,198]. Future research is needed to further elucidate the underlying mechanisms and ultimately enable translation in clinical practice (Table 7).

6. Conclusions

This review aimed to provide an overview of the molecular and cytogenetic landscape of WM and IgM-MGUS, as well as its clinical applications. In recent years, major progress has been made in genomic and transcriptomic profiling, hereby shedding light on the origin and evolution of the disease, unraveling involved pathways and dissecting the heterogeneity within the WM clone, as well as of the TME. Moreover, (cf)DNA and (cf)RNA biomarkers have been proposed that are able to define disease subgroups, are associated with disease progression and therapy response and allow minimally invasive detection of mutations.

An important limitation, however, is the discordancy between studies concerning diagnostic criteria, detection methods with ranging sensitivities and types of specimens analyzed (BM and PB, selected or unselected CD19+ B cells). Moreover, experimental details are often not reported, making data comparison challenging, especially in small patient cohorts such as the infrequent MYD88^WT/CXCR4^WT subgroup. Therefore, we encourage all authors to report sufficient experimental design details in order to allow a reliable comparison among studies. Likewise, there is a current lack of consensus between diagnostic laboratories on how to perform profiling analyses in WM and IgM-MGUS patients, which is the main reason why molecular data are not yet included in the diagnostic criteria. Lastly, studies in patients with familial WM are very limited. Potential contributors to genetic predisposition have been identified and represent possible candidates for validation within different familial WM populations. Family history information should therefore be routinely collected.

In terms of future research directions, since the temporal acquisition of genomic mutations remains unclear, longitudinal studies are needed to explore the dynamics of clonal architecture and to identify driver mutations that play a role in disease course or chemoresistance. Moreover, deciphering the mechanisms of progression in premalignant IgM gammopathies will help to monitor patients at risk of progression. The use of circulating nucleic acids as minimally invasive, disease-specific and dynamic biomarkers is highly promising, but further research is needed to develop signatures with high specificity and sensitivity that can be routinely implemented in clinical practice. In the same regard, an interesting future perspective is combining cell-free DNA and RNA, as well as other cellular molecules, in a multi-omics approach. Lastly, in contrast to different solid and hematological tumors, the role of (epi)miRNAs interaction, lncRNAs and circRNAs have been very sparsely investigated in WM and IgM-MGUS. Including these dimensions could significantly contribute to our understanding of these diseases and ultimately to the development of new biomarkers and therapies.

Publisher’s Note: MDPI stays neutral with regard to jurisdictional claims in published maps and institutional affiliations.

Enlarge this image.

Figure 1. Diagnostic criteria for WM and IgM-MGUS. Serum monoclonal IgM: any concentration according to Owen 2003 (2° IWWM), Swerdlow 2008 (WHO 2008) and Campo 2011 (WHO 2011) [9,11,13] or ≥30 g/L according to Ansell 2010 (mSMART), Swerdlow 2017 and Maqbool 2020 [14,17,19]. BM infiltration: unequivocal BM infiltration by lymphoplasmacytic lymphoma [9,11] or infiltration ≥10% [14,17,19]. Immunophenotype: immunophenotype consistent with WM: CD19+, CD20+, CD22+, CD79+, CD5-, CD10-, CD23-. Of note, 5–10% of WM cases could express CD5 [20,21]. Symptoms: attributable to tumor infiltration (in BM or extramedullary) and/or to the monoclonal protein (related to immunological or chemical properties) [7,8,21]. IgM-related disorders: patients who have clinical features attributable to the IgM monoclonal protein but without overt evidence of LPL in the BM. For cases in which BM infiltration is not confirmed, the immunophenotypic profile is useful to discriminate the pattern of WM from other IgM-related disorders. However, BM infiltration by immunohistochemistry is mandatory for a definitive WM diagnosis. IgM-MGUS: patients with an IgM gammopathy, without evidence of LPL in the BM biopsy and no symptoms. Cases with detectable clonal B cells by immunophenotype and absence of BM infiltration by LPL [9] or BM infiltration <10% and IgM <30 g/L [14,17,19] should be classified as IgM-MGUS. aWM: patients with an IgM gammopathy and BM infiltration by LPL without symptoms. Immunophenotyping is strongly recommended for differential diagnosis. WM: patients with IgM protein of any concentration and unequivocal BM infiltration and symptoms. Immunophenotyping is strongly recommended.

Enlarge this image.

Figure 2. Mutational and cytogenetic landscape of WM. The figure describes the association between genomic abnormalities in WM patients. (A) From the center outward, the distribution and overlap of MYD88L265P mutations, CXCR4MUT mutations, karyotype (K) (Complex K: <5 clonal aberrations; high complex K: ≥5 clonal aberrations), copy number alterations (CNAs) and less frequent mutations (MUTs) are shown, respectively. The color code in the outer ring refers to colors in panels B and C. Relevant up and down-regulated genes (arrows) are reported. DLBCL like mutations: somatic mutations overlapping those detected in diffuse large B cell lymphoma (DLBCL), (i.e., TBL1XR1, PTPN13, MALT1, BCL10, NFKB2, NFKBIB, NFKBIZ, and UDRL1F). (B) Relative distribution of cytogenetic abnormalities. tri: trisomy, del: deletion. (C) Relative distribution of uncommon mutations. The percentage (%) of the most frequent MUTs and CNAs are estimated based on published data, for more details see below.

Enlarge this image.

Figure 3. An illustrative overview of the pathways involved with increased miR-155 expression in WM. MAFB, SHANK2 and SH3PXD2A (italic) are more recently discovered targets of miR-155 in WM and further studies are needed to elucidate their role. Everolimus-dependent anti-WM activity is partially driven by targeting miR-155 (red).

Enlarge this image.

Figure 4. Cell-free DNA (cfDNA) and cell-free RNA (cfRNA) markers in plasma or serum of WM patients. Significant up- and downregulated miRNAs are shown (arrows).

References

1. Ziegler, A.; Koch, A.; Krockenberger, K.; Grosshennig, A. Personalized medicine using DNA biomarkers: A review. Hum. Genet.; 2012; 131, pp. 1627-1638. [DOI: https://dx.doi.org/10.1007/s00439-012-1188-9] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/22752797]

2. Gilboa, T.; Garden, P.M.; Cohen, L. Single-molecule analysis of nucleic acid biomarkers—A review. Anal. Chim. Acta; 2020; 1115, pp. 61-85. [DOI: https://dx.doi.org/10.1016/j.aca.2020.03.001] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/32370870]

3. Braggio, E.; Philipsborn, C.; Novak, A.; Hodge, L.; Ansell, S.; Fonseca, R. Molecular pathogenesis of Waldenstrom’s macroglobulinemia. Haematologica; 2012; 97, pp. 1281-1290. [DOI: https://dx.doi.org/10.3324/haematol.2012.068478] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/22773606]

4. Gertz, M. Waldenström macroglobulinemia: My way. Leuk. Lymphoma; 2013; 54, pp. 464-471. [DOI: https://dx.doi.org/10.3109/10428194.2012.717173]

5. Remstein, E.D.; Hanson, C.A.; Kyle, R.A.; Hodnefield, J.M.; Kurtin, P.J. Despite apparent morphologic and immunophenotypic heterogeneity, Waldenstrom’s macroglobulinemia is consistently composed of cells along a morphologic continuum of small lymphocytes, plasmacytoid lymphocytes, and plasma cells. Semin. Oncol.; 2003; 30, pp. 182-186. [DOI: https://dx.doi.org/10.1053/sonc.2003.50073] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/12720133]

6. Kriangkum, J.; Taylor, B.J.; Treon, S.P.; Mant, M.J.; Belch, A.R.; Pilarski, L.M. Clonotypic IgM V/D/J sequence analysis in Waldenstrom macroglobulinemia suggests an unusual B-cell origin and an expansion of polyclonal B cells in peripheral blood. Blood; 2004; 104, pp. 2134-2142. [DOI: https://dx.doi.org/10.1182/blood-2003-11-4024]

7. Chen, L.Y.; Keddie, S.; Lunn, M.P.; Bomsztyk, J.; Vitsaras, E.; Gupta, R.; D’Sa, S. IgM paraprotein-associated peripheral neuropathy: Small CD20-positive B-cell clones may predict a monoclonal gammopathy of neurological significance and rituximab responsiveness. Br. J. Haematol.; 2020; 188, pp. 511-515. [DOI: https://dx.doi.org/10.1111/bjh.16210]

8. Leung, N.; Bridoux, F.; Nasr, S.H. Monoclonal Gammopathy of Renal Significance. N. Engl. J. Med.; 2021; 384, pp. 1931-1941. [DOI: https://dx.doi.org/10.1056/NEJMra1810907]

9. Owen, R.G.; Treon, S.P.; Al-Katib, A.; Fonseca, R.; Greipp, P.R.; McMaster, M.L.; Morra, E.; Pangalis, G.A.; San Miguel, J.F.; Branagan, A.R. et al. Clinicopathological definition of Waldenstrom’s macroglobulinemia: Consensus Panel Recommendations from the Second International Workshop on Waldenstrom’s Macroglobulinemia. Semin. Oncol.; 2003; 30, pp. 110-115. [DOI: https://dx.doi.org/10.1053/sonc.2003.50082]

10. Varettoni, M.; Zibellini, S.; Defrancesco, I.; Ferretti, V.V.; Rizzo, E.; Malcovati, L.; Gallì, A.; Della Porta, M.G.; Boveri, E.; Arcaini, L. et al. Pattern of somatic mutations in patients with Waldenström macroglobulinemia or IgM monoclonal gammopathy of undetermined significance. Haematologica; 2017; 102, pp. 2077-2085. [DOI: https://dx.doi.org/10.3324/haematol.2017.172718]

11. Campo, E.; Swerdlow, S.H.; Harris, N.L.; Pileri, S.; Stein, H.; Jaffe, E.S. The 2008 WHO classification of lymphoid neoplasms and beyond: Evolving concepts and practical applications. Blood; 2011; 117, pp. 5019-5032. [DOI: https://dx.doi.org/10.1182/blood-2011-01-293050]

12. Gertz, M.A. Waldenström macroglobulinemia: 2021 update on diagnosis, risk stratification, and management. Am. J. Hematol.; 2021; 96, pp. 258-269. [DOI: https://dx.doi.org/10.1002/ajh.26082]

13. Swerdlow, S.; Campo, E.; Harris, N.L.; Jaffe, E.S.; Pileri, S.; Stein, H. WHO Classification of Tumours of Haematopoietic and Lymphoid Tissues; IARC Publications: Lyon, France, 2008; Volume 2.

14. Ansell, S.M.; Kyle, R.A.; Reeder, C.B.; Fonseca, R.; Mikhael, J.R.; Morice, W.G.; Bergsagel, P.L.; Buadi, F.K.; Colgan, J.P.; Dingli, D. et al. Diagnosis and Management of Waldenström Macroglobulinemia: Mayo Stratification of Macroglobulinemia and Risk-Adapted Therapy (mSMART) Guidelines. Mayo Clin. Proc.; 2010; 85, pp. 824-833. [DOI: https://dx.doi.org/10.4065/mcp.2010.0304]

15. Rajkumar, S.V.; Dimopoulos, M.A.; Palumbo, A.; Blade, J.; Merlini, G.; Mateos, M.-V.; Kumar, S.; Hillengass, J.; Kastritis, E.; Richardson, P. et al. International Myeloma Working Group updated criteria for the diagnosis of multiple myeloma. Lancet Oncol.; 2014; 15, pp. e538-e548. [DOI: https://dx.doi.org/10.1016/S1470-2045(14)70442-5]

16. Kapoor, P.; Ansell, S.M.; Fonseca, R.; Chanan-Khan, A.; Kyle, R.A.; Kumar, S.K.; Mikhael, J.R.; Witzig, T.E.; Mauermann, M.; Dispenzieri, A. et al. Diagnosis and Management of Waldenström Macroglobulinemia. JAMA Oncol.; 2017; 3, 1257. [DOI: https://dx.doi.org/10.1001/jamaoncol.2016.5763]

17. Maqbool, M.G.; Tam, C.S.; Morison, I.M.; Simpson, D.; Mollee, P.; Schneider, H.; Chan, H.; Juneja, S.; Harvey, Y.; Nath, L. et al. A practical guide to laboratory investigations at diagnosis and follow up in Waldenström macroglobulinaemia: Recommendations from the Medical and Scientific Advisory Group, Myeloma Australia, the Pathology Sub-committee of the Lymphoma and Related Disease. Pathology; 2020; 52, pp. 167-178. [DOI: https://dx.doi.org/10.1016/j.pathol.2019.11.002]

18. Pratt, G.; El-Sharkawi, D.; Kothari, J.; D’Sa, S.; Auer, R.; McCarthy, H.; Krishna, R.; Miles, O.; Kyriakou, C.; Owen, R. Guidelines on the diagnosis and management of Waldenström macroglobulinaemia—A British Society for Haematology guideline. Br. J. Haematol.; 2022; [DOI: https://dx.doi.org/10.1111/bjh.18036]

19. Swerdlow, S.; Campo, E.; Harris, N.L.; Jaffe, E.S.; Pileri, S.; Stein, H.; Thiele, J. WHO Classification of Tumours of Haematopoietic and Lymphoid Tissues; 4th ed. IARC Publications: Lyon, France, 2017; ISBN 9789283244943

20. Morice, W.G.; Chen, D.; Kurtin, P.J.; Hanson, C.A.; McPhail, E.D. Novel immunophenotypic features of marrow lymphoplasmacytic lymphoma and correlation with Waldenström’s macroglobulinemia. Mod. Pathol.; 2009; 22, pp. 807-816. [DOI: https://dx.doi.org/10.1038/modpathol.2009.34]

21. Askari, E.; Rodriguez, S.; Garcia-Sanz, R. Waldenström’s Macroglobulinemia: An Exploration into the Pathology and Diagnosis of a Complex B-Cell Malignancy. J. Blood Med.; 2021; 12, pp. 795-807. [DOI: https://dx.doi.org/10.2147/JBM.S267938]

22. Kyle, R.A.; Larson, D.R.; Therneau, T.M.; Dispenzieri, A.; Kumar, S.; Cerhan, J.R.; Rajkumar, S.V. Long-Term Follow-up of Monoclonal Gammopathy of Undetermined Significance. N. Engl. J. Med.; 2018; 378, pp. 241-249. [DOI: https://dx.doi.org/10.1056/NEJMoa1709974]

23. Hobbs, M.; Fonder, A.; Hwa, Y.L. Waldenström Macroglobulinemia: Clinical Presentation, Diagnosis, and Management. J. Adv. Pract. Oncol.; 2020; 11, pp. 381-389. [DOI: https://dx.doi.org/10.6004/jadpro.2020.11.4.5]

24. Waldenström, J. Incipient myelomatosis or «essential» hyperglobulinemia with fibrinogenopenia-A new syndrome?. Acta Med. Scand.; 2009; 117, pp. 216-247. [DOI: https://dx.doi.org/10.1111/j.0954-6820.1944.tb03955.x]

25. McMaster, M.L.; Goldin, L.R.; Bai, Y.; Ter-Minassian, M.; Boehringer, S.; Giambarresi, T.R.; Vasquez, L.G.; Tucker, M.A. Genomewide Linkage Screen for Waldenström Macroglobulinemia Susceptibility Loci in High-Risk Families. Am. J. Hum. Genet.; 2006; 79, pp. 695-701. [DOI: https://dx.doi.org/10.1086/507687]

26. Nguyen-Khac, F.; Lambert, J.; Chapiro, E.; Grelier, A.; Mould, S.; Barin, C.; Daudignon, A.; Gachard, N.; Struski, S.; Henry, C. et al. Chromosomal aberrations and their prognostic value in a series of 174 untreated patients with Waldenström’s macroglobulinemia. Haematologica; 2013; 98, pp. 649-654. [DOI: https://dx.doi.org/10.3324/haematol.2012.070458]

27. Treon, S.P.; Xu, L.; Yang, G.; Zhou, Y.; Liu, X.; Cao, Y.; Sheehy, P.; Manning, R.J.; Patterson, C.J.; Tripsas, C. et al. MYD88 L265P somatic mutation in Waldenström’s macroglobulinemia. N. Engl. J. Med.; 2012; 367, pp. 826-833. [DOI: https://dx.doi.org/10.1056/NEJMoa1200710]

28. Hunter, Z.R.; Xu, L.; Yang, G.; Zhou, Y.; Liu, X.; Cao, Y.; Manning, R.J.; Tripsas, C.; Patterson, C.J.; Sheehy, P. et al. The genomic landscape of Waldenstrom macroglobulinemia is characterized by highly recurring MYD88 and WHIM-like CXCR4 mutations, and small somatic deletions associated with B-cell lymphomagenesis. Blood; 2014; 123, pp. 1637-1646. [DOI: https://dx.doi.org/10.1182/blood-2013-09-525808]

29. Kastritis, E.; Morel, P.; Duhamel, A.; Gavriatopoulou, M.; Kyrtsonis, M.C.; Durot, E.; Symeonidis, A.; Laribi, K.; Hatjiharissi, E.; Ysebaert, L. et al. A revised international prognostic score system for Waldenström’s macroglobulinemia. Leukemia; 2019; 33, pp. 2654-2661. [DOI: https://dx.doi.org/10.1038/s41375-019-0431-y]

30. Swerdlow, S.H.; Campo, E.; Pileri, S.A.; Harris, N.L.; Stein, H.; Siebert, R.; Advani, R.; Ghielmini, M.; Salles, G.A.; Zelenetz, A.D. et al. The 2016 revision of the World Health Organization classification of lymphoid neoplasms. Blood; 2016; 127, pp. 2375-2390. [DOI: https://dx.doi.org/10.1182/blood-2016-01-643569]

31. Jansson, M.D.; Lund, A.H. MicroRNA and cancer. Mol. Oncol.; 2012; 6, pp. 590-610. [DOI: https://dx.doi.org/10.1016/j.molonc.2012.09.006]

32. Mercer, T.R.; Dinger, M.E.; Mattick, J.S. Long non-coding RNAs: Insights into functions. Nat. Rev. Genet.; 2009; 10, pp. 155-159. [DOI: https://dx.doi.org/10.1038/nrg2521]

33. Verduci, L.; Tarcitano, E.; Strano, S.; Yarden, Y.; Blandino, G. CircRNAs: Role in human diseases and potential use as biomarkers. Cell Death Dis.; 2021; 12, 468. [DOI: https://dx.doi.org/10.1038/s41419-021-03743-3] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/33976116]

34. Marrugo-Ramírez, J.; Mir, M.; Samitier, J. Blood-Based Cancer Biomarkers in Liquid Biopsy: A Promising Non-Invasive Alternative to Tissue Biopsy. Int. J. Mol. Sci.; 2018; 19, 2877. [DOI: https://dx.doi.org/10.3390/ijms19102877] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/30248975]

35. Serrano, M.J.; Garrido-Navas, M.C.; Diaz Mochon, J.J.; Cristofanilli, M.; Gil-Bazo, I.; Pauwels, P.; Malapelle, U.; Russo, A.; Lorente, J.A.; Ruiz-Rodriguez, A.J. et al. Precision Prevention and Cancer Interception: The New Challenges of Liquid Biopsy. Cancer Discov.; 2020; 10, pp. 1635-1644. [DOI: https://dx.doi.org/10.1158/2159-8290.CD-20-0466] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/33037026]

36. Pantel, K. Liquid Biopsy: Blood-Based Analyses of ctDNA and CTCs. Clin. Chem.; 2021; 67, pp. 1437-1439. [DOI: https://dx.doi.org/10.1093/clinchem/hvab168]

37. Qi, F.; Cao, Z.; Chen, B.; Chai, Y.; Lin, J.; Ye, J.; Wei, Y.; Liu, H.; Han-Zhang, H.; Mao, X. et al. Liquid biopsy in extranodal NK/T-cell lymphoma: A prospective analysis of cell-free DNA genotyping and monitoring. Blood Adv.; 2021; 5, pp. 2505-2514. [DOI: https://dx.doi.org/10.1182/bloodadvances.2020001637]

38. Landgren, O.; Staudt, L. MYD88 L265P somatic mutation in IgM MGUS. N. Engl. J. Med.; 2012; 367, pp. 2255-2256. [DOI: https://dx.doi.org/10.1056/NEJMc1211959#SA1]

39. Gachard, N.; Parrens, M.; Soubeyran, I.; Petit, B.; Marfak, A.; Rizzo, D.; Devesa, M.; Delage-Corre, M.; Coste, V.; Laforêt, M.P. et al. IGHV gene features and MYD88 L265P mutation separate the three marginal zone lymphoma entities and Waldenström macroglobulinemia/lymphoplasmacytic lymphomas. Leukemia; 2013; 27, pp. 183-189. [DOI: https://dx.doi.org/10.1038/leu.2012.257]

40. Xu, L.; Hunter, Z.R.; Yang, G.; Zhou, Y.; Cao, Y.; Liu, X.; Morra, E.; Trojani, A.; Greco, A.; Arcaini, L. et al. MYD88 L265P in Waldenström macroglobulinemia, immunoglobulin M monoclonal gammopathy, and other B-cell lymphoproliferative disorders using conventional and quantitative allele-specific polymerase chain reaction. Blood; 2013; 121, pp. 2051-2058. [DOI: https://dx.doi.org/10.1182/blood-2012-09-454355]

41. Ondrejka, S.L.; Lin, J.J.; Warden, D.W.; Durkin, L.; Cook, J.R.; Hsi, E.D. MYD88 L265P somatic mutation: Its usefulness in the differential diagnosis of bone marrow involvement by B-cell lymphoproliferative disorders. Am. J. Clin. Pathol.; 2013; 140, pp. 387-394. [DOI: https://dx.doi.org/10.1309/AJCP10ZCLFZGYZIP]

42. Jiménez, C.; Sebastián, E.; Chillón, M.C.; Giraldo, P.; Mariano Hernández, J.; Escalante, F.; González-López, T.J.; Aguilera, C.; de Coca, A.G.; Murillo, I. et al. MYD88 L265P is a marker highly characteristic of, but not restricted to, Waldenström’s macroglobulinemia. Leukemia; 2013; 27, pp. 1722-1728. [DOI: https://dx.doi.org/10.1038/leu.2013.62]

43. Poulain, S.; Roumier, C.; Decambron, A.; Renneville, A.; Herbaux, C.; Bertrand, E.; Tricot, S.; Daudignon, A.; Galiègue-Zouitina, S.; Soenen, V. et al. MYD88 L265P mutation in Waldenstrom macroglobulinemia. Blood; 2013; 121, pp. 4504-4511. [DOI: https://dx.doi.org/10.1182/blood-2012-06-436329]

44. Willenbacher, W.; Willenbacher, E.; Brunner, A.; Manzl, C. Improved accuracy of discrimination between IgM Multiple Myeloma and Waldenström Macroglobulinaemia by testing for MYD88 L265P mutations. Br. J. Haematol.; 2013; 161, pp. 902-904. [DOI: https://dx.doi.org/10.1111/bjh.12313]

45. Mori, N.; Ohwashi, M.; Yoshinaga, K.; Mitsuhashi, K.; Tanaka, N.; Teramura, M.; Okada, M.; Shiseki, M.; Tanaka, J.; Motoji, T. L265P Mutation of the MYD88 Gene Is Frequent in Waldenström’s Macroglobulinemia and Its Absence in Myeloma. PLoS ONE; 2013; 8, e80088. [DOI: https://dx.doi.org/10.1371/journal.pone.0080088]

46. Varettoni, M.; Arcaini, L.; Zibellini, S.; Boveri, E.; Rattotti, S.; Riboni, R.; Corso, A.; Orlandi, E.; Bonfichi, M.; Gotti, M. et al. Prevalence and clinical significance of the MYD88 (L265P) somatic mutation in Waldenstrom’s macroglobulinemia and related lymphoid neoplasms. Blood; 2013; 121, pp. 2522-2528. [DOI: https://dx.doi.org/10.1182/blood-2012-09-457101]

47. Argentou, N.; Vassilopoulos, G.; Ioannou, M.; Germenis, A.E.; Speletas, M. Rapid detection of MYD88-L265P mutation by PCR-RFLP in B-cell lymphoproliferative disorders. Leukemia; 2014; 28, pp. 447-449. [DOI: https://dx.doi.org/10.1038/leu.2013.294]

48. Capaldi, I.B.; May, A.M.; Schmitt-Graeff, A.; Follo, M.; Aumann, K.; Kayser, G.; Perazzo, J.C.; Werner, M.; Fisch, P. Detection of MYD88 L265P mutations in formalin-fixed and decalcified BM biopsies from patients with lymphoplasmacytic lymphoma. Exp. Mol. Pathol.; 2014; 97, pp. 57-65. [DOI: https://dx.doi.org/10.1016/j.yexmp.2014.05.005]

49. Petrikkos, L.; Kyrtsonis, M.-C.; Roumelioti, M.; Georgiou, G.; Efthymiou, A.; Tzenou, T.; Panayiotidis, P. Clonotypic analysis of immunoglobulin heavy chain sequences in patients with Waldenström’s macroglobulinemia: Correlation with MYD88 L265P somatic mutation status, clinical features, and outcome. Biomed Res. Int.; 2014; 2014, 809103. [DOI: https://dx.doi.org/10.1155/2014/809103]

50. Ansell, S.M.; Hodge, L.S.; Secreto, F.J.; Manske, M.; Braggio, E.; Price-Troska, T.; Ziesmer, S.; Li, Y.; Johnson, S.H.; Hart, S.N. et al. Activation of TAK1 by MYD88 L265P drives malignant B-cell Growth in non-Hodgkin lymphoma. Blood Cancer J.; 2014; 4, e183. [DOI: https://dx.doi.org/10.1038/bcj.2014.4]

51. Xu, L.; Hunter, Z.R.; Yang, G.; Cao, Y.; Liu, X.; Manning, R.; Tripsas, C.; Chen, J.; Patterson, C.J.; Kluk, M. et al. Detection of MYD88 L265P in peripheral blood of patients with Waldenström’s Macroglobulinemia and IgM monoclonal gammopathy of undetermined significance. Leukemia; 2014; 28, pp. 1698-1704. [DOI: https://dx.doi.org/10.1038/leu.2014.65]

52. Treon, S.P.; Cao, Y.; Xu, L.; Yang, G.; Liu, X.; Hunter, Z.R. Somatic mutations in MYD88 and CXCR4 are determinants of clinical presentation and overall survival in Waldenström macroglobulinemia. Blood; 2014; 123, pp. 2791-2796. [DOI: https://dx.doi.org/10.1182/blood-2014-01-550905]

53. Patkar, N.; Subramanian, P.G.; Deshpande, P.; Ghodke, K.; Tembhare, P.; Mascarenhas, R.; Muranjan, A.; Chaudhary, S.; Bagal, B.; Gujral, S. et al. MYD88 mutant lymphoplasmacytic lymphoma/Waldenström macroglobulinemia has distinct clinical and pathological features as compared to its mutation negative counterpart. Leuk. Lymphoma; 2015; 56, pp. 420-425. [DOI: https://dx.doi.org/10.3109/10428194.2014.924123]

54. Schmidt, J.; Federmann, B.; Schindler, N.; Steinhilber, J.; Bonzheim, I.; Fend, F.; Quintanilla-Martinez, L. MYD88 L265P and CXCR4 mutations in lymphoplasmacytic lymphoma identify cases with high disease activity. Br. J. Haematol.; 2015; 169, pp. 795-803. [DOI: https://dx.doi.org/10.1111/bjh.13361]

55. Shin, S.-Y.; Lee, S.-T.; Kim, H.-Y.; Park, C.-H.; Kim, H.-J.; Kim, J.-W.; Kim, S.J.; Kim, W.S.; Kim, S.-H. Detection of MYD88 L265P in patients with lymphoplasmacytic lymphoma/Waldenstrom macroglobulinemia and other B-cell non-Hodgkin lymphomas. Blood Res.; 2016; 51, pp. 181-186. [DOI: https://dx.doi.org/10.5045/br.2016.51.3.181]

56. Burnworth, B.; Wang, Z.; Singleton, T.P.; Bennington, A.; Fritschle, W.; Bennington, R.; Brodersen, L.E.; Wells, D.A.; Loken, M.R.; Zehentner, B.K. Clone-specific MYD88 L265P and CXCR4 mutation status can provide clinical utility in suspected Waldenström macroglobulinemia/lymphoplasmacytic lymphoma. Leuk. Res.; 2016; 51, pp. 41-48. [DOI: https://dx.doi.org/10.1016/j.leukres.2016.10.008]

57. Correa, J.G.; Cibeira, M.T.; Tovar, N.; Isola, I.; Pedrosa, F.; Díaz, T.; Lozano, E.; Magnano, L.; Rosiñol, L.; Bladé, J. et al. Prevalence and prognosis implication of MYD88 L265P mutation in IgM monoclonal gammopathy of undetermined significance and smouldering Waldenström macroglobulinaemia. Br. J. Haematol.; 2017; 179, pp. 849-851. [DOI: https://dx.doi.org/10.1111/bjh.14266]

58. Baer, C.; Dicker, F.; Kern, W.; Haferlach, T.; Haferlach, C. Genetic characterization of MYD88-mutated lymphoplasmacytic lymphoma in comparison with MYD88-mutated chronic lymphocytic leukemia. Leukemia; 2017; 31, pp. 1355-1362. [DOI: https://dx.doi.org/10.1038/leu.2016.330]

59. Paludo, J.; Abeykoon, J.P.; Kumar, S.; Shreders, A.; Ailawadhi, S.; Gertz, M.A.; Kourelis, T.; King, R.L.; Reeder, C.B.; Leung, N. et al. Dexamethasone, rituximab and cyclophosphamide for relapsed and/or refractory and treatment-naïve patients with Waldenstrom macroglobulinemia. Br. J. Haematol.; 2017; 179, pp. 98-105. [DOI: https://dx.doi.org/10.1111/bjh.14826]

60. Cao, X.-X.; Meng, Q.; Cai, H.; He, T.-H.; Zhang, C.-L.; Su, W.; Sun, J.; Li, Y.; Xu, W.; Zhou, D.-B. et al. Detection of MYD88 L265P and WHIM-like CXCR4 mutation in patients with IgM monoclonal gammopathy related disease. Ann. Hematol.; 2017; 96, pp. 971-976. [DOI: https://dx.doi.org/10.1007/s00277-017-2968-z]

61. Abeykoon, J.P.; Paludo, J.; King, R.L.; Ansell, S.M.; Gertz, M.A.; LaPlant, B.R.; Halvorson, A.E.; Gonsalves, W.I.; Dingli, D.; Fang, H. et al. MYD88 mutation status does not impact overall survival in Waldenström macroglobulinemia. Am. J. Hematol.; 2018; 93, pp. 187-194. [DOI: https://dx.doi.org/10.1002/ajh.24955]

62. Drandi, D.; Genuardi, E.; Dogliotti, I.; Ferrante, M.; Jiménez, C.; Guerrini, F.; Lo Schirico, M.; Mantoan, B.; Muccio, V.; Lia, G. et al. Highly sensitive MYD88^L265P mutation detection by droplet digital PCR in Waldenström Macroglobulinemia. Haematologica; 2018; 103, pp. 1029-1037. [DOI: https://dx.doi.org/10.3324/haematol.2017.186528]

63. Vinarkar, S.; Arora, N.; Chowdhury, S.S.; Saha, K.; Pal, B.; Parihar, M.; Radhakrishnan, V.S.; Chakrapani, A.; Bhartia, S.; Bhave, S. et al. MYD88 and CXCR4 Mutation Profiling in Lymphoplasmacytic Lymphoma/Waldenstrom’s Macroglobulinaemia. Indian J. Hematol. Blood Transfus.; 2019; 35, pp. 57-65. [DOI: https://dx.doi.org/10.1007/s12288-018-0978-1] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/30828149]

64. Nakamura, A.; Ohwada, C.; Takeuchi, M.; Takeda, Y.; Tsukamoto, S.; Mimura, N.; Nagisa, O.-H.; Sugita, Y.; Tanaka, H.; Wakita, H. et al. Detection of MYD88 L265P mutation by next-generation deep sequencing in peripheral blood mononuclear cells of Waldenström’s macroglobulinemia and IgM monoclonal gammopathy of undetermined significance. PLoS ONE; 2019; 14, e0221941. [DOI: https://dx.doi.org/10.1371/journal.pone.0221941] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/31483817]

65. Wu, Y.-Y.; Jia, M.-N.; Cai, H.; Qiu, Y.; Zhou, D.-B.; Li, J.; Cao, X.-X. Detection of the MYD88L265P and CXCR4S338X mutations by cell-free DNA in Waldenström macroglobulinemia. Ann. Hematol.; 2020; 99, pp. 1763-1769. [DOI: https://dx.doi.org/10.1007/s00277-020-04139-7] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/32577844]

66. Wang, Y.; Gali, V.L.; Xu-Monette, Z.Y.; Sano, D.; Thomas, S.K.; Weber, D.M.; Zhu, F.; Fang, X.; Deng, M.; Zhang, M. et al. Molecular and genetic biomarkers implemented from next-generation sequencing provide treatment insights in clinical practice for Waldenström macroglobulinemia. Neoplasia; 2021; 23, pp. 361-374. [DOI: https://dx.doi.org/10.1016/j.neo.2021.02.002] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/33735664]

67. Kofides, A.; Hunter, Z.R.; Xu, L.; Tsakmaklis, N.; Demos, M.G.; Munshi, M.; Liu, X.; Guerrera, M.L.; Leventoff, C.R.; White, T.P. et al. Diagnostic Next-generation Sequencing Frequently Fails to Detect MYD88L265P in Waldenström Macroglobulinemia. HemaSphere; 2021; 5, e624. [DOI: https://dx.doi.org/10.1097/HS9.0000000000000624]

68. Brubaker, S.W.; Bonham, K.S.; Zanoni, I.; Kagan, J.C. Innate Immune Pattern Recognition: A Cell Biological Perspective. Annu. Rev. Immunol.; 2015; 33, pp. 257-290. [DOI: https://dx.doi.org/10.1146/annurev-immunol-032414-112240]

69. Tan, Y.; Kagan, J.C. Innate Immune Signaling Organelles Display Natural and Programmable Signaling Flexibility. Cell; 2019; 177, pp. 384-398.e11. [DOI: https://dx.doi.org/10.1016/j.cell.2019.01.039]

70. Kagan, J.C.; Magupalli, V.G.; Wu, H. SMOCs: Supramolecular organizing centres that control innate immunity. Nat. Rev. Immunol.; 2014; 14, pp. 821-826. [DOI: https://dx.doi.org/10.1038/nri3757]

71. Balka, K.R.; Nardo, D. Understanding early TLR signaling through the Myddosome. J. Leukoc. Biol.; 2019; 105, pp. 339-351. [DOI: https://dx.doi.org/10.1002/JLB.MR0318-096R]

72. Deliz-Aguirre, R.; Cao, F.; Gerpott, F.H.U.; Auevechanichkul, N.; Chupanova, M.; Mun, Y.; Ziska, E.; Taylor, M.J. MyD88 oligomer size functions as a physical threshold to trigger IL1R Myddosome signaling. J. Cell Biol.; 2021; 220, e202012071. [DOI: https://dx.doi.org/10.1083/jcb.202012071]

73. Wang, J.Q.; Jeelall, Y.S.; Beutler, B.; Horikawa, K.; Goodnow, C.C. Consequences of the recurrent MYD88L265P somatic mutation for B cell tolerance. J. Exp. Med.; 2014; 211, pp. 413-426. [DOI: https://dx.doi.org/10.1084/jem.20131424]

74. O’Carroll, A.; Chauvin, B.; Brown, J.W.P.; Meagher, A.; Coyle, J.; Schill, J.; Bhumkhar, A.; Hunter, D.J.B.; Ve, T.; Kobe, B. et al. Pathological mutations differentially affect the self-assembly and polymerisation of the innate immune system signalling adaptor molecule MyD88. BMC Biol.; 2018; 16, 149. [DOI: https://dx.doi.org/10.1186/s12915-018-0611-7]

75. Yang, G.; Buhrlage, S.J.; Tan, L.; Liu, X.; Chen, J.; Xu, L.; Tsakmaklis, N.; Chen, J.G.; Patterson, C.J.; Brown, J.R. et al. HCK is a survival determinant transactivated by mutated MYD88, and a direct target of ibrutinib. Blood; 2016; 127, pp. 3237-3252. [DOI: https://dx.doi.org/10.1182/blood-2016-01-695098]

76. Manček-Keber, M.; Lainšček, D.; Benčina, M.; Chen, J.G.; Romih, R.; Hunter, Z.R.; Treon, S.P.; Jerala, R. Extracellular vesicle–mediated transfer of constitutively active MyD88L265P engages MyD88wt and activates signaling. Blood; 2018; 131, pp. 1720-1729. [DOI: https://dx.doi.org/10.1182/blood-2017-09-805499]

77. Varettoni, M.; Zibellini, S.; Arcaini, L.; Boveri, E.; Rattotti, S.; Pascutto, C.; Mangiacavalli, S.; Gotti, M.; Pochintesta, L.; Paulli, M. et al. MYD88 (L265P) mutation is an independent risk factor for progression in patients with IgM monoclonal gammopathy of undetermined significance. Blood; 2013; 122, pp. 2284-2285. [DOI: https://dx.doi.org/10.1182/blood-2013-07-513366]

78. Sewastianik, T.; Guerrera, M.L.; Adler, K.; Dennis, P.S.; Wright, K.; Shanmugam, V.; Huang, Y.; Tanton, H.; Jiang, M.; Kofides, A. et al. Human MYD88L265P is insufficient by itself to drive neoplastic transformation in mature mouse B cells. Blood Adv.; 2019; 3, pp. 3360-3374. [DOI: https://dx.doi.org/10.1182/bloodadvances.2019000588]

79. Schmidt, K.; Sack, U.; Graf, R.; Winkler, W.; Popp, O.; Mertins, P.; Sommermann, T.; Kocks, C.; Rajewsky, K. B-Cell-Specific Myd88 L252P Expression Causes a Premalignant Gammopathy Resembling IgM MGUS. Front. Immunol.; 2020; 11, 602868. [DOI: https://dx.doi.org/10.3389/fimmu.2020.602868]

80. Rodriguez, S.; Celay, J.; Goicoechea, I.; Jimenez, C.; Botta, C.; Garcia-Barchino, M.-J.; Garces, J.-J.; Larrayoz, M.; Santos, S.; Alignani, D. et al. Preneoplastic somatic mutations including MYD88 L265P in lymphoplasmacytic lymphoma. Sci. Adv.; 2022; 8, eabl4644. [DOI: https://dx.doi.org/10.1126/sciadv.abl4644]

81. Treon, S.P.; Gustine, J.; Xu, L.; Manning, R.J.; Tsakmaklis, N.; Demos, M.; Meid, K.; Guerrera, M.L.; Munshi, M.; Chan, G. et al. MYD88 wild-type Waldenstrom Macroglobulinaemia: Differential diagnosis, risk of histological transformation, and overall survival. Br. J. Haematol.; 2018; 180, pp. 374-380. [DOI: https://dx.doi.org/10.1111/bjh.15049]

82. Hunter, Z.R.; Xu, L.; Tsakmaklis, N.; Demos, M.G.; Kofides, A.; Jimenez, C.; Chan, G.G.; Chen, J.; Liu, X.; Munshi, M. et al. Insights into the genomic landscape of MYD88 wild-Type Waldenström macroglobulinemia. Blood Adv.; 2018; 2, pp. 2937-2946. [DOI: https://dx.doi.org/10.1182/bloodadvances.2018022962]

83. Guerrera, M.L.; Tsakmaklis, N.; Xu, L.; Yang, G.; Demos, M.; Kofides, A.; Chan, G.G.; Manning, R.J.; Liu, X.; Chen, J.G. et al. MYD88 mutated and wild-type Waldenström’s Macroglobulinemia: Characterization of chromosome 6q gene losses and their mutual exclusivity with mutations in CXCR4. Haematologica; 2018; 103, pp. e408-e411. [DOI: https://dx.doi.org/10.3324/haematol.2018.190181]

84. Poulain, S.; Roumier, C.; Venet-Caillault, A.; Figeac, M.; Herbaux, C.; Marot, G.; Doye, E.; Bertrand, E.; Geffroy, S.; Lepretre, F. et al. Genomic Landscape of CXCR4 Mutations in Waldenstro m Macroglobulinemia. Clin. Cancer Res.; 2016; 22, pp. 1480-1488. [DOI: https://dx.doi.org/10.1158/1078-0432.CCR-15-0646]

85. Castillo, J.J.; Xu, L.; Gustine, J.N.; Keezer, A.; Meid, K.; Dubeau, T.E.; Liu, X.; Demos, M.G.; Kofides, A.; Tsakmaklis, N. et al. CXCR4 mutation subtypes impact response and survival outcomes in patients with Waldenström macroglobulinaemia treated with ibrutinib. Br. J. Haematol.; 2019; 187, pp. 356-363. [DOI: https://dx.doi.org/10.1111/bjh.16088]

86. Pozzobon, T.; Goldoni, G.; Viola, A.; Molon, B. CXCR4 signaling in health and disease. Immunol. Lett.; 2016; 177, pp. 6-15. [DOI: https://dx.doi.org/10.1016/j.imlet.2016.06.006]

87. Xu, L.; Hunter, Z.R.; Tsakmaklis, N.; Cao, Y.; Yang, G.; Chen, J.; Liu, X.; Kanan, S.; Castillo, J.J.; Tai, Y.-T. et al. Clonal architecture of CXCR4 WHIM-like mutations in Waldenström Macroglobulinaemia. Br. J. Haematol.; 2016; 172, pp. 735-744. [DOI: https://dx.doi.org/10.1111/bjh.13897]

88. Milanesi, S.; Locati, M.; Borroni, E.M. Aberrant CXCR4 Signaling at Crossroad of WHIM Syndrome and Waldenstrom’s Macroglobulinemia. Int. J. Mol. Sci.; 2020; 21, 5696. [DOI: https://dx.doi.org/10.3390/ijms21165696]

89. Kaiser, L.M.; Hunter, Z.R.; Treon, S.P.; Buske, C. CXCR4 in Waldenström’s Macroglobulinema: Chances and challenges. Leukemia; 2021; 35, pp. 333-345. [DOI: https://dx.doi.org/10.1038/s41375-020-01102-3]

90. Roccaro, A.M.; Sacco, A.; Jimenez, C.; Maiso, P.; Moschetta, M.; Mishima, Y.; Aljawai, Y.; Sahin, I.; Kuhne, M.; Cardarelli, P. et al. C1013G/CXCR4 acts as a driver mutation of tumor progression and modulator of drug resistance in lymphoplasmacytic lymphoma. Blood; 2014; 123, pp. 4120-4131. [DOI: https://dx.doi.org/10.1182/blood-2014-03-564583]

91. Cao, Y.; Hunter, Z.R.; Liu, X.; Xu, L.; Yang, G.; Chen, J.; Patterson, C.J.; Tsakmaklis, N.; Kanan, S.; Rodig, S. et al. The WHIM-like CXCR4(S338X) somatic mutation activates AKT and ERK, and promotes resistance to ibrutinib and other agents used in the treatment of Waldenstrom’s Macroglobulinemia. Leukemia; 2015; 29, pp. 169-176. [DOI: https://dx.doi.org/10.1038/leu.2014.187]

92. Gustine, J.N.; Xu, L.; Yang, G.; Liu, X.; Kofides, A.; Tsakmaklis, N.; Munshi, M.; Demos, M.; Guerrera, M.L.; Meid, K. et al. Bone marrow involvement and subclonal diversity impairs detection of mutated CXCR4 by diagnostic next-generation sequencing in Waldenström macroglobulinaemia. Br. J. Haematol.; 2021; 194, pp. 730-733. [DOI: https://dx.doi.org/10.1111/bjh.17385]

93. Jiménez, C.; Prieto-Conde, M.I.; García-Álvarez, M.; Alcoceba, M.; Escalante, F.; Del Carmen Chillón, M.; García de Coca, A.; Balanzategui, A.; Cantalapiedra, A.; Aguilar, C. et al. Unraveling the heterogeneity of IgM monoclonal gammopathies: A gene mutational and gene expression study. Ann. Hematol.; 2018; 97, pp. 475-484. [DOI: https://dx.doi.org/10.1007/s00277-017-3207-3] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/29353304]

94. Ballester, L.Y.; Loghavi, S.; Kanagal-Shamanna, R.; Barkoh, B.A.; Lin, P.; Medeiros, L.J.; Luthra, R.; Patel, K.P. Clinical Validation of a CXCR4 Mutation Screening Assay for Waldenstrom Macroglobulinemia. Clin. Lymphoma. Myeloma Leuk.; 2016; 16, pp. 395-403.e1. [DOI: https://dx.doi.org/10.1016/j.clml.2016.04.014] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/27268124]

95. Jiménez, C.; Xu, L.; Tsakmaklis, N.; Demos, M.G.; Kofides, A.; Chan, G.G.; Guerrera, M.L.; Chen, J.G.; Liu, X.; Munshi, M. et al. Comparative genomics of CXCR4MUT and CXCR4WT single cells in Waldenström’s macroglobulinemia. Blood Adv.; 2020; 4, pp. 4550-4553. [DOI: https://dx.doi.org/10.1182/bloodadvances.2020001775] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/32956451]

96. Alegría-Landa, V.; Prieto-Torres, L.; Santonja, C.; Córdoba, R.; Manso, R.; Requena, L.; Rodríguez-Pinilla, S.M. MYD88 L265P mutation in cutaneous involvement by Waldenström macroglobulinemia. J. Cutan. Pathol.; 2017; 44, pp. 625-631. [DOI: https://dx.doi.org/10.1111/cup.12944]

97. Gustine, J.; Meid, K.; Xu, L.; Hunter, Z.R.; Castillo, J.J.; Treon, S.P. To select or not to select? The role of B-cell selection in determining the MYD88 mutation status in Waldenström Macroglobulinaemia. Br. J. Haematol.; 2017; 176, pp. 822-824. [DOI: https://dx.doi.org/10.1111/bjh.13996]

98. Poulain, S.; Boyle, E.M.; Roumier, C.; Demarquette, H.; Wemeau, M.; Geffroy, S.; Herbaux, C.; Bertrand, E.; Hivert, B.; Terriou, L. et al. MYD88 L265P mutation contributes to the diagnosis of Bing Neel syndrome. Br. J. Haematol.; 2014; 167, pp. 506-513. [DOI: https://dx.doi.org/10.1111/bjh.13078]

99. Ferrante, M.; Furlan, D.; Zibellini, S.; Borriero, M.; Candido, C.; Sahnane, N.; Uccella, S.; Genuardi, E.; Alessandria, B.; Bianchi, B. et al. MYD88L265P Detection in IgM Monoclonal Gammopathies: Methodological Considerations for Routine Implementation. Diagnostics; 2021; 11, 779. [DOI: https://dx.doi.org/10.3390/diagnostics11050779]

100. Paiva, B.; Corchete, L.A.; Vidriales, M.-B.; Garcia-Sanz, R.; Perez, J.J.; Aires-Mejia, I.; Sanchez, M.-L.; Barcena, P.; Alignani, D.; Jimenez, C. et al. The cellular origin and malignant transformation of Waldenstrom macroglobulinemia. Blood; 2015; 125, pp. 2370-2380. [DOI: https://dx.doi.org/10.1182/blood-2014-09-602565]

101. Ocio, E.M.; Schop, R.F.J.; Gonzalez, B.; Van Wier, S.A.; Hernandez-Rivas, J.M.; Gutierrez, N.C.; Garcia-Sanz, R.; Moro, M.J.; Aguilera, C.; Hernandez, J. et al. 6q deletion in Waldenström macroglobulinemia is associated with features of adverse prognosis. Br. J. Haematol.; 2007; 136, pp. 80-86. [DOI: https://dx.doi.org/10.1111/j.1365-2141.2006.06389.x]

102. Chang, H.; Qi, C.; Trieu, Y.; Jiang, A.; Young, K.H.; Chesney, A.; Jani, P.; Wang, C.; Reece, D.; Chen, C. Prognostic Relevance of 6q Deletion in Waldenström’s Macroglobulinemia: A Multicenter Study. Clin. Lymphoma Myeloma; 2009; 9, pp. 36-38. [DOI: https://dx.doi.org/10.3816/CLM.2009.n.008]

103. García-Sanz, R.; Dogliotti, I.; Zaccaria, G.M.; Ocio, E.M.; Rubio, A.; Murillo, I.; Escalante, F.; Aguilera, C.; García-Mateo, A.; García de Coca, A. et al. 6q deletion in Waldenström macroglobulinaemia negatively affects time to transformation and survival. Br. J. Haematol.; 2021; 192, pp. 843-852. [DOI: https://dx.doi.org/10.1111/bjh.17028]

104. Hunter, Z.R.; Xu, L.; Yang, G.; Tsakmaklis, N.; Vos, J.M.; Liu, X.; Chen, J.J.G.; Manning, R.J.; Chen, J.J.G.; Brodsky, P. et al. Transcriptome sequencing reveals a profile that corresponds to genomic variants in Waldenström macroglobulinemia. Blood; 2016; 128, pp. 827-838. [DOI: https://dx.doi.org/10.1182/blood-2016-03-708263]

105. Schop, R.F.J.; Van Wier, S.A.; Xu, R.; Ghobrial, I.; Ahmann, G.J.; Greipp, P.R.; Kyle, R.A.; Dispenzieri, A.; Lacy, M.Q.; Rajkumar, S.V. et al. 6q deletion discriminates Waldenström macroglobulinemia from IgM monoclonal gammopathy of undetermined significance. Cancer Genet. Cytogenet.; 2006; 169, pp. 150-153. [DOI: https://dx.doi.org/10.1016/j.cancergencyto.2006.04.009]

106. Terré, C.; Nguyen-Khac, F.; Barin, C.; Mozziconacci, M.J.; Eclache, V.; Léonard, C.; Chapiro, E.; Farhat, H.; Bouyon, A.; Rousselot, P. et al. Trisomy 4, a new chromosomal abnormality in Waldenström’s macroglobulinemia: A study of 39 cases. Leukemia; 2006; 20, pp. 1634-1636. [DOI: https://dx.doi.org/10.1038/sj.leu.2404314]

107. Braggio, E.; Keats, J.J.; Leleu, X.; Van Wier, S.; Jimenez-Zepeda, V.H.; Valdez, R.; Schop, R.F.J.J.; Price-Troska, T.; Henderson, K.; Sacco, A. et al. Identification of Copy Number Abnormalities and Inactivating Mutations in Two Negative Regulators of Nuclear Factor- B Signaling Pathways in Waldenstrom’s Macroglobulinemia. Cancer Res.; 2009; 69, pp. 3579-3588. [DOI: https://dx.doi.org/10.1158/0008-5472.CAN-08-3701]

108. Poulain, S.; Braggio, E.; Roumier, C.; Aijjou, R.; Broucqsault, N.; Galiègue-Zouitina, S.; Manier, S.; Soenen, V.; Nibourel, O.; Duthilleul, P. et al. High-Throughput Genomic Analysis in Waldenström’s Macroglobulinemia. Clin. Lymphoma Myeloma Leuk.; 2011; 11, pp. 106-108. [DOI: https://dx.doi.org/10.3816/CLML.2011.n.021]

109. Sekiguchi, N.; Nomoto, J.; Nagata, A.; Kiyota, M.; Fukuda, I.; Yamada, K.; Takezako, N.; Kobayashi, Y. Gene Expression Profile Signature of Aggressive Waldenström Macroglobulinemia with Chromosome 6q Deletion. Biomed Res. Int.; 2018; 2018, 6728128. [DOI: https://dx.doi.org/10.1155/2018/6728128]

110. Krzisch, D.; Guedes, N.; Boccon-Gibod, C.; Baron, M.; Bravetti, C.; Davi, F.; Armand, M.; Smagghe, L.; Caron, J.; Bernard, O.A. et al. Cytogenetic and molecular abnormalities in Waldenström’s macroglobulinemia patients: Correlations and prognostic impact. Am. J. Hematol.; 2021; 96, pp. 1569-1579. [DOI: https://dx.doi.org/10.1002/ajh.26339]

111. Poulain, S.; Roumier, C.; Bertrand, E.; Renneville, A.; Caillault-Venet, A.; Doye, E.; Geffroy, S.; Sebda, S.; Nibourel, O.; Nudel, M. et al. TP53 Mutation and Its Prognostic Significance in Waldenstrom’s Macroglobulinemia. Clin. Cancer Res.; 2017; 23, pp. 6325-6335. [DOI: https://dx.doi.org/10.1158/1078-0432.CCR-17-0007]

112. Roos-Weil, D.; Decaudin, C.; Armand, M.; Della-Valle, V.; Diop, M.K.; Ghamlouch, H.; Ropars, V.; Hérate, C.; Lara, D.; Durot, E. et al. A Recurrent Activating Missense Mutation in Waldenström Macroglobulinemia Affects the DNA Binding of the ETS Transcription Factor SPI1 and Enhances Proliferation. Cancer Discov.; 2019; 9, pp. 796-811. [DOI: https://dx.doi.org/10.1158/2159-8290.CD-18-0873]

113. Treon, S.P.; Meid, K.; Gustine, J.; Yang, G.; Xu, L.; Liu, X.; Patterson, C.J.; Hunter, Z.R.; Branagan, A.R.; Laubach, J.P. et al. Long-Term Follow-Up of Ibrutinib Monotherapy in Symptomatic, Previously Treated Patients With Waldenström Macroglobulinemia. J. Clin. Oncol.; 2021; 39, pp. 565-575. [DOI: https://dx.doi.org/10.1200/JCO.20.00555]

114. Treon, S.P.; Tripsas, C.K.; Meid, K.; Warren, D.; Varma, G.; Green, R.; Argyropoulos, K.V.; Yang, G.; Cao, Y.; Xu, L. et al. Ibrutinib in Previously Treated Waldenström’s Macroglobulinemia. N. Engl. J. Med.; 2015; 372, pp. 1430-1440. [DOI: https://dx.doi.org/10.1056/NEJMoa1501548]

115. Treon, S.P.; Xu, L.; Guerrera, M.L.; Jimenez, C.; Hunter, Z.R.; Liu, X.; Demos, M.; Gustine, J.; Chan, G.; Munshi, M. et al. Genomic landscape of Waldenström macroglobulinemia and its impact on treatment strategies. J. Clin. Oncol.; 2020; 38, pp. 1198-1208. [DOI: https://dx.doi.org/10.1200/JCO.19.02314]

116. Castillo, J.J.; Moreno, D.F.; Arbelaez, M.I.; Hunter, Z.R.; Treon, S.P. CXCR4 mutations affect presentation and outcomes in patients with Waldenström macroglobulinemia: A systematic review. Expert Rev. Hematol.; 2019; 12, pp. 873-881. [DOI: https://dx.doi.org/10.1080/17474086.2019.1649132]

117. Owen, R.G.; McCarthy, H.; Rule, S.; D’Sa, S.; Thomas, S.K.; Tournilhac, O.; Forconi, F.; Kersten, M.J.; Zinzani, P.L.; Iyengar, S. et al. Acalabrutinib monotherapy in patients with Waldenström macroglobulinemia: A single-arm, multicentre, phase 2 study. Lancet Haematol.; 2020; 7, pp. e112-e121. [DOI: https://dx.doi.org/10.1016/S2352-3026(19)30210-8]

118. Tam, C.S.; Opat, S.; D’Sa, S.; Jurczak, W.; Lee, H.-P.; Cull, G.; Owen, R.G.; Marlton, P.; Wahlin, B.E.; Sanz, R.G. et al. A randomized phase 3 trial of zanubrutinib vs. ibrutinib in symptomatic Waldenström macroglobulinemia: The ASPEN study. Blood; 2020; 136, pp. 2038-2050. [DOI: https://dx.doi.org/10.1182/blood.2020006844]

119. Dimopoulos, M.; Sanz, R.G.; Lee, H.-P.P.; Trneny, M.; Varettoni, M.; Opat, S.; D’Sa, S.; Owen, R.G.; Cull, G.; Mulligan, S. et al. Zanubrutinib for the treatment of MYD88 wild-type Waldenström macroglobulinemia: A substudy of the phase 3 ASPEN trial. Blood Adv.; 2020; 4, pp. 6009-6018. [DOI: https://dx.doi.org/10.1182/bloodadvances.2020003010]

120. Jiménez, C.; Alonso-Álvarez, S.; Alcoceba, M.; Ordóñez, G.R.; García-Álvarez, M.; Prieto-Conde, M.I.; Chillón, M.C.; Balanzategui, A.; Corral, R.; Marín, L.A. et al. From Waldenström’s macroglobulinemia to aggressive diffuse large B-cell lymphoma: A whole-exome analysis of abnormalities leading to transformation. Blood Cancer J.; 2017; 7, e591. [DOI: https://dx.doi.org/10.1038/bcj.2017.72]

121. Gustine, J.N.; Tsakmaklis, N.; Demos, M.G.; Kofides, A.; Chen, J.G.; Liu, X.; Munshi, M.; Guerrera, M.L.; Chan, G.G.; Patterson, C.J. et al. TP 53 mutations are associated with mutated MYD 88 and CXCR 4, and confer an adverse outcome in Waldenström macroglobulinaemia. Br. J. Haematol.; 2019; 184, pp. 242-245. [DOI: https://dx.doi.org/10.1111/bjh.15560]

122. Esteller, M. Non-coding RNAs in human disease. Nat. Rev. Genet.; 2011; 12, pp. 861-874. [DOI: https://dx.doi.org/10.1038/nrg3074]

123. Klein, U.; Tu, Y.; Stolovitzky, G.A.; Mattioli, M.; Cattoretti, G.; Husson, H.; Freedman, A.; Inghirami, G.; Cro, L.; Baldini, L. et al. Gene Expression Profiling of B Cell Chronic Lymphocytic Leukemia Reveals a Homogeneous Phenotype Related to Memory B Cells. J. Exp. Med.; 2001; 194, pp. 1625-1638. [DOI: https://dx.doi.org/10.1084/jem.194.11.1625] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/11733577]

124. Chng, W.J.; Schop, R.F.; Price-Troska, T.; Ghobrial, I.; Kay, N.; Jelinek, D.F.; Gertz, M.A.; Dispenzieri, A.; Lacy, M.; Kyle, R.A. et al. Gene-expression profiling of Waldenstrom macroglobulinemia reveals a phenotype more similar to chronic lymphocytic leukemia than multiple myeloma. Blood; 2006; 108, pp. 2755-2763. [DOI: https://dx.doi.org/10.1182/blood-2006-02-005488] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/16804116]

125. Jackson, D.A.; Smith, T.D.; Amarsaikhan, N.; Han, W.; Neil, M.S.; Boi, S.K.; Vrabel, A.M.; Tolosa, E.J.; Almada, L.L.; Fernandez-Zapico, M.E. et al. Modulation of the IL-6 Receptor α Underlies GLI2-Mediated Regulation of Ig Secretion in Waldenström Macroglobulinemia Cells. J. Immunol.; 2015; 195, pp. 2908-2916. [DOI: https://dx.doi.org/10.4049/jimmunol.1402974] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/26238488]

126. Elsawa, S.F.; Novak, A.J.; Ziesmer, S.C.; Almada, L.L.; Hodge, L.S.; Grote, D.M.; Witzig, T.E.; Fernandez-Zapico, M.E.; Ansell, S.M. Comprehensive analysis of tumor microenvironment cytokines in Waldenstrom macroglobulinemia identifies CCL5 as a novel modulator of IL-6 activity. Blood; 2011; 118, pp. 5540-5549. [DOI: https://dx.doi.org/10.1182/blood-2011-04-351742]

127. Hatzimichael, E.C.; Christou, L.; Bai, M.; Kolios, G.; Kefala, L.; Bourantas, K.L. Serum levels of IL-6 and its soluble receptor (sIL-6R) in Waldenström’s macroglobulinemia. Eur. J. Haematol.; 2001; 66, pp. 1-6. [DOI: https://dx.doi.org/10.1034/j.1600-0609.2001.00152.x]

128. Gutiérrez, N.C.; Ocio, E.M.; de las Rivas, J.; Maiso, P.; Delgado, M.; Fermiñán, E.; Arcos, M.J.; Sánchez, M.L.; Hernández, J.M.; San Miguel, J.F. Gene expression profiling of B lymphocytes and plasma cells from Waldenström’s macroglobulinemia: Comparison with expression patterns of the same cell counterparts from chronic lymphocytic leukemia, multiple myeloma and normal individuals. Leukemia; 2007; 21, pp. 541-549. [DOI: https://dx.doi.org/10.1038/sj.leu.2404520]

129. Han, W.; Matissek, S.J.; Jackson, D.A.; Sklavanitis, B.; Elsawa, S.F. Targeting IL-6 receptor reduces IgM levels and tumor growth in Waldenström macroglobulinemia. Oncotarget; 2019; 10, pp. 3400-3407. [DOI: https://dx.doi.org/10.18632/oncotarget.26946]

130. Gaudette, B.T.; Dwivedi, B.; Chitta, K.S.; Poulain, S.; Powell, D.; Vertino, P.; Leleu, X.; Lonial, S.; Chanan-Khan, A.A.; Kowalski, J. et al. Low expression of pro-apoptotic Bcl-2 family proteins sets the apoptotic threshold in Waldenström macroglobulinemia. Oncogene; 2016; 35, pp. 479-490. [DOI: https://dx.doi.org/10.1038/onc.2015.103]

131. Leleu, X.; Eeckhoute, J.; Jia, X.; Roccaro, A.M.; Moreau, A.-S.; Farag, M.; Sacco, A.; Ngo, H.T.; Runnels, J.; Melhem, M.R. et al. Targeting NF-kappaB in Waldenstrom macroglobulinemia. Blood; 2008; 111, pp. 5068-5077. [DOI: https://dx.doi.org/10.1182/blood-2007-09-115170]

132. Hunter, Z.; Cao, Y.; Lewicki, M.; Sun, J.; Tseng, H.; Hanzis, C.; Brodsky, P.; Manning, R.; Xu, L.; Yang, G. et al. Aberrant Expression of Regulatory miRNAs and Transcripts for IRS-PI3K Growth and Survival Signaling In Waldenstrom’s Macroglobulinemia. Blood; 2010; 116, 1912. [DOI: https://dx.doi.org/10.1182/blood.V116.21.1912.1912]

133. Roccaro, A.M.; Sacco, A.; Jia, X.; Azab, A.K.; Maiso, P.; Ngo, H.T.; Azab, F.; Runnels, J.; Quang, P.; Ghobrial, I.M. microRNA-dependent modulation of histone acetylation in Waldenstrom macroglobulinemia. Blood; 2010; 116, pp. 1506-1514. [DOI: https://dx.doi.org/10.1182/blood-2010-01-265686]

134. Sun, J.Y.; Xu, L.; Tseng, H.; Ciccarelli, B.; Fulciniti, M.; Hunter, Z.R.; Maghsoudi, K.; Hatjiharissi, E.; Zhou, Y.; Yang, G. et al. Histone deacetylase inhibitors demonstrate significant preclinical activity as single agents, and in combination with bortezomib in Waldenström’s macroglobulinemia. Clin. Lymphoma Myeloma Leuk.; 2011; 11, pp. 152-156. [DOI: https://dx.doi.org/10.3816/CLML.2011.n.036]

135. Roccaro, A.M.; Sacco, A.; Chen, C.; Runnels, J.; Leleu, X.; Azab, F.; Azab, A.K.; Jia, X.; Ngo, H.T.; Melhem, M.R. et al. MicroRNA expression in the biology, prognosis, and therapy of Waldenström macroglobulinemia. Blood; 2009; 113, pp. 4391-4402. [DOI: https://dx.doi.org/10.1182/blood-2008-09-178228]

136. Fulciniti, M.; Amodio, N.; Bandi, R.L.; Cagnetta, A.; Samur, M.K.; Acharya, C.; Prabhala, R.; D’Aquila, P.; Bellizzi, D.; Passarino, G. et al. MiR-23b/SP1/c-myc forms a feed-forward loop supporting multiple myeloma cell growth. Blood Cancer J.; 2016; 6, e380. [DOI: https://dx.doi.org/10.1038/bcj.2015.106]

137. Caivano, A.; La Rocca, F.; Simeon, V.; Girasole, M.; Dinarelli, S.; Laurenzana, I.; De Stradis, A.; De Luca, L.; Trino, S.; Traficante, A. et al. MicroRNA-155 in serum-derived extracellular vesicles as a potential biomarker for hematologic malignancies—A short report. Cell. Oncol.; 2017; 40, pp. 97-103. [DOI: https://dx.doi.org/10.1007/s13402-016-0300-x]

138. Bouyssou, J.M.; Liu, C.-J.; Bustoros, M.; Sklavenitis-Pistofidis, R.; Aljawai, Y.; Manier, S.; Yosef, A.; Sacco, A.; Kokubun, K.; Tsukamoto, S. et al. Profiling of circulating exosomal miRNAs in patients with Waldenström Macroglobulinemia. PLoS ONE; 2018; 13, e0204589. [DOI: https://dx.doi.org/10.1371/journal.pone.0204589]

139. Hodge, L.S.; Elsawa, S.F.; Grote, D.M.; Price-Troska, T.L.; Asmann, Y.W.; Fonseca, R.; Gertz, M.A.; Witzig, T.E.; Novak, A.J.; Ansell, S.M. MicroRNA expression in tumor cells from Waldenstrom’s macroglobulinemia reflects both their normal and malignant cell counterparts. Blood Cancer J.; 2011; 1, e24. [DOI: https://dx.doi.org/10.1038/bcj.2011.25]

140. Kubiczkova Besse, L.; Sedlarikova, L.; Kryukov, F.; Nekvindova, J.; Radova, L.; Almasi, M.; Pelcova, J.; Minarik, J.; Pika, T.; Pikalova, Z. et al. Combination of serum microRNA-320a and microRNA-320b as a marker for Waldenström macroglobulinemia. Am. J. Hematol.; 2015; 90, pp. E51-E52. [DOI: https://dx.doi.org/10.1002/ajh.23910]

141. Roccaro, A.M.; Sacco, A.; Jia, X.; Banwait, R.; Maiso, P.; Azab, F.; Flores, L.; Manier, S.; Azab, A.K.; Ghobrial, I.M. Mechanisms of Activity of the TORC1 Inhibitor Everolimus in Waldenstrom Macroglobulinemia. Clin. Cancer Res.; 2012; 18, 6609. [DOI: https://dx.doi.org/10.1158/1078-0432.CCR-12-1532]

142. Barh, D.; Malhotra, R.; Ravi, B.; Sindhurani, P. Microrna Let-7: An Emerging Next-Generation Cancer Therapeutic. Curr. Oncol.; 2010; 17, pp. 70-80. [DOI: https://dx.doi.org/10.3747/co.v17i1.356]

143. Kluiver, J.; Poppema, S.; de Jong, D.; Blokzijl, T.; Harms, G.; Jacobs, S.; Kroesen, B.-J.; van den Berg, A. BIC and miR-155 are highly expressed in Hodgkin, primary mediastinal and diffuse large B cell lymphomas. J. Pathol.; 2005; 207, pp. 243-249. [DOI: https://dx.doi.org/10.1002/path.1825] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/16041695]

144. Zhang, Y.; Roccaro, A.M.; Rombaoa, C.; Flores, L.; Obad, S.; Fernandes, S.M.; Sacco, A.; Liu, Y.; Ngo, H.; Quang, P. et al. LNA-mediated anti–miR-155 silencing in low-grade B-cell lymphomas. Blood; 2012; 120, pp. 1678-1686. [DOI: https://dx.doi.org/10.1182/blood-2012-02-410647] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/22797699]

145. Morel, P.; Duhamel, A.; Gobbi, P.; Dimopoulos, M.A.; Dhodapkar, M.V.; McCoy, J.; Crowley, J.; Ocio, E.M.; Garcia-Sanz, R.; Treon, S.P. et al. International prognostic scoring system for Waldenström macroglobulinemia. Blood; 2009; 113, pp. 4163-4170. [DOI: https://dx.doi.org/10.1182/blood-2008-08-174961] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/19196866]

146. Pedersen, I.M.; Otero, D.; Kao, E.; Miletic, A.V.; Hother, C.; Ralfkiaer, E.; Rickert, R.C.; Gronbaek, K.; David, M. Onco-miR-155 targets SHIP1 to promote TNFα-dependent growth of B cell lymphomas. EMBO Mol. Med.; 2009; 1, pp. 288-295. [DOI: https://dx.doi.org/10.1002/emmm.200900028]

147. Esteller, M. Epigenetics in Cancer. N. Engl. J. Med.; 2008; 358, pp. 1148-1159. [DOI: https://dx.doi.org/10.1056/NEJMra072067]

148. Zhang, L.; Lu, Q.; Chang, C. Epigenetics in Health and Disease. Adv. Exp. Med. Biol.; 2020; 1253, pp. 3-55. [DOI: https://dx.doi.org/10.1007/978-981-15-3449-2_1]

149. Amodio, N.; Rossi, M.; Raimondi, L.; Pitari, M.R.; Botta, C.; Tagliaferri, P.; Tassone, P. miR-29s: A family of epi-miRNAs with therapeutic implications in hematologic malignancies. Oncotarget; 2015; 6, pp. 12837-12861. [DOI: https://dx.doi.org/10.18632/oncotarget.3805]

150. Esteller, M. Epigenetics provides a new generation of oncogenes and tumour-suppressor genes. Br. J. Cancer; 2006; 94, pp. 179-183. [DOI: https://dx.doi.org/10.1038/sj.bjc.6602918]

151. Sampath, D.; Liu, C.; Vasan, K.; Sulda, M.; Puduvalli, V.K.; Wierda, W.G.; Keating, M.J. Histone deacetylases mediate the silencing of miR-15a, miR-16, and miR-29b in chronic lymphocytic leukemia. Blood; 2012; 119, pp. 1162-1172. [DOI: https://dx.doi.org/10.1182/blood-2011-05-351510]

152. Braga, T.V.; Evangelista, F.C.G.; Gomes, L.C.; da Silva Araújo, S.S.; das Graças Carvalho, M.; de Paula, A. Evaluation of MiR-15a and MiR-16-1 as prognostic biomarkers in chronic lymphocytic leukemia. Biomed. Pharmacother.; 2017; 92, pp. 864-869. [DOI: https://dx.doi.org/10.1016/j.biopha.2017.05.144]

153. Roccaro, A.M.; Sacco, A.; Thompson, B.; Leleu, X.; Azab, A.K.; Azab, F.; Runnels, J.; Jia, X.; Ngo, H.T.; Melhem, M.R. et al. MicroRNAs 15a and 16 regulate tumor proliferation in multiple myeloma. Blood; 2009; 113, pp. 6669-6680. [DOI: https://dx.doi.org/10.1182/blood-2009-01-198408]

154. Ghobrial, I.M.; Campigotto, F.; Murphy, T.J.; Boswell, E.N.; Banwait, R.; Azab, F.; Chuma, S.; Kunsman, J.; Donovan, A.; Masood, F. et al. Results of a phase 2 trial of the single-agent histone deacetylase inhibitor panobinostat in patients with relapsed/refractory Waldenström macroglobulinemia. Blood; 2013; 121, pp. 1296-1303. [DOI: https://dx.doi.org/10.1182/blood-2012-06-439307]

155. Matissek, S.J.; Han, W.; Karbalivand, M.; Sayed, M.; Reilly, B.M.; Mallat, S.; Ghazal, S.M.; Munshi, M.; Yang, G.; Treon, S.P. et al. Epigenetic targeting of Waldenström macroglobulinemia cells with BET inhibitors synergizes with BCL2 or histone deacetylase inhibition. Epigenomics; 2021; 13, pp. 129-144. [DOI: https://dx.doi.org/10.2217/epi-2020-0189]

156. Peng, W.-X.; Koirala, P.; Mo, Y.-Y. LncRNA-mediated regulation of cell signaling in cancer. Oncogene; 2017; 36, pp. 5661-5667. [DOI: https://dx.doi.org/10.1038/onc.2017.184]

157. Bhan, A.; Soleimani, M.; Mandal, S.S. Long Noncoding RNA and Cancer: A New Paradigm. Cancer Res.; 2017; 77, pp. 3965-3981. [DOI: https://dx.doi.org/10.1158/0008-5472.CAN-16-2634]

158. Garding, A.; Bhattacharya, N.; Claus, R.; Ruppel, M.; Tschuch, C.; Filarsky, K.; Idler, I.; Zucknick, M.; Caudron-Herger, M.; Oakes, C. et al. Epigenetic Upregulation of lncRNAs at 13q14.3 in Leukemia Is Linked to the In Cis Downregulation of a Gene Cluster That Targets NF-kB. PLoS Genet.; 2013; 9, e1003373. [DOI: https://dx.doi.org/10.1371/journal.pgen.1003373]

159. Wang, L.Q.; Wong, K.Y.; Li, Z.H.; Chim, C.S. Epigenetic silencing of tumor suppressor long non-coding RNA BM742401 in chronic lymphocytic leukemia. Oncotarget; 2016; 7, pp. 82400-82410. [DOI: https://dx.doi.org/10.18632/oncotarget.12252]

160. Blume, C.J.; Hotz-Wagenblatt, A.; Hüllein, J.; Sellner, L.; Jethwa, A.; Stolz, T.; Slabicki, M.; Lee, K.; Sharathchandra, A.; Benner, A. et al. p53-dependent non-coding RNA networks in chronic lymphocytic leukemia. Leukemia; 2015; 29, pp. 2015-2023. [DOI: https://dx.doi.org/10.1038/leu.2015.119]

161. Isin, M.; Ozgur, E.; Cetin, G.; Erten, N.; Aktan, M.; Gezer, U.; Dalay, N. Investigation of circulating lncRNAs in B-cell neoplasms. Clin. Chim. Acta; 2014; 431, pp. 255-259. [DOI: https://dx.doi.org/10.1016/j.cca.2014.02.010]

162. Eis, P.S.; Tam, W.; Sun, L.; Chadburn, A.; Li, Z.; Gomez, M.F.; Lund, E.; Dahlberg, J.E. Accumulation of miR-155 and BIC RNA in human B cell lymphomas. Proc. Natl. Acad. Sci. USA; 2005; 102, pp. 3627-3632. [DOI: https://dx.doi.org/10.1073/pnas.0500613102]

163. Sattari, A.; Siddiqui, H.; Moshiri, F.; Ngankeu, A.; Nakamura, T.; Kipps, T.J.; Croce, C.M. Upregulation of long noncoding RNA MIAT in aggressive form of chronic lymphocytic leukemias. Oncotarget; 2016; 7, pp. 54174-54182. [DOI: https://dx.doi.org/10.18632/oncotarget.11099]

164. Ronchetti, D.; Manzoni, M.; Agnelli, L.; Vinci, C.; Fabris, S.; Cutrona, G.; Matis, S.; Colombo, M.; Galletti, S.; Taiana, E. et al. lncRNA profiling in early-stage chronic lymphocytic leukemia identifies transcriptional fingerprints with relevance in clinical outcome. Blood Cancer J.; 2016; 6, e468. [DOI: https://dx.doi.org/10.1038/bcj.2016.77]

165. Ronchetti, D.; Agnelli, L.; Taiana, E.; Galletti, S.; Manzoni, M.; Todoerti, K.; Musto, P.; Strozzi, F.; Neri, A. Distinct lncRNA transcriptional fingerprints characterize progressive stages of multiple myeloma. Oncotarget; 2016; 7, pp. 14814-14830. [DOI: https://dx.doi.org/10.18632/oncotarget.7442]

166. Zhuang, W.; Ge, X.; Yang, S.; Huang, M.; Zhuang, W.; Chen, P.; Zhang, X.; Fu, J.; Qu, J.; Li, B. Upregulation of lncRNA MEG3 Promotes Osteogenic Differentiation of Mesenchymal Stem Cells From Multiple Myeloma Patients By Targeting BMP4 Transcription. Stem Cells; 2015; 33, pp. 1985-1997. [DOI: https://dx.doi.org/10.1002/stem.1989] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/25753650]

167. Pan, Y.; Chen, H.; Shen, X.; Wang, X.; Ju, S.; Lu, M.; Cong, H. Serum level of long noncoding RNA H19 as a diagnostic biomarker of multiple myeloma. Clin. Chim. Acta; 2018; 480, pp. 199-205. [DOI: https://dx.doi.org/10.1016/j.cca.2018.02.019] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/29470951]

168. Pan, Y.; Zhang, Y.; Liu, W.; Huang, Y.; Shen, X.; Jing, R.; Pu, J.; Wang, X.; Ju, S.; Cong, H. et al. LncRNA H19 overexpression induces bortezomib resistance in multiple myeloma by targeting MCL-1 via miR-29b-3p. Cell Death Dis.; 2019; 10, 106. [DOI: https://dx.doi.org/10.1038/s41419-018-1219-0] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/30728351]

169. Kristensen, L.S.; Andersen, M.S.; Stagsted, L.V.W.; Ebbesen, K.K.; Hansen, T.B.; Kjems, J. The biogenesis, biology and characterization of circular RNAs. Nat. Rev. Genet.; 2019; 20, pp. 675-691. [DOI: https://dx.doi.org/10.1038/s41576-019-0158-7] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/31395983]

170. Wu, Z.; Sun, H.; Liu, W.; Zhu, H.; Fu, J.; Yang, C.; Fan, L.; Wang, L.; Liu, Y.; Xu, W. et al. Circ-RPL15: A plasma circular RNA as novel oncogenic driver to promote progression of chronic lymphocytic leukemia. Leukemia; 2020; 34, pp. 919-923. [DOI: https://dx.doi.org/10.1038/s41375-019-0594-6] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/31611623]

171. Xia, L.; Wu, L.; Bao, J.; Li, Q.; Chen, X.; Xia, H.; Xia, R. Circular RNA circ-CBFB promotes proliferation and inhibits apoptosis in chronic lymphocytic leukemia through regulating miR-607/FZD3/Wnt/β-catenin pathway. Biochem. Biophys. Res. Commun.; 2018; 503, pp. 385-390. [DOI: https://dx.doi.org/10.1016/j.bbrc.2018.06.045]

172. Wu, W.; Wu, Z.; Xia, Y.; Qin, S.; Li, Y.; Wu, J.; Liang, J.; Wang, L.; Zhu, H.; Fan, L. et al. Downregulation of circ_0132266 in chronic lymphocytic leukemia promoted cell viability through miR-337-3p/PML axis. Aging; 2019; 11, pp. 3561-3573. [DOI: https://dx.doi.org/10.18632/aging.101997]

173. Dahl, M.; Daugaard, I.; Andersen, M.S.; Hansen, T.B.; Grønbæk, K.; Kjems, J.; Kristensen, L.S. Enzyme-free digital counting of endogenous circular RNA molecules in B-cell malignancies. Lab. Investig.; 2018; 98, pp. 1657-1669. [DOI: https://dx.doi.org/10.1038/s41374-018-0108-6]

174. Liu, H.; Wu, Y.; Wang, S.; Jiang, J.; Zhang, C.; Jiang, Y.; Wang, X.; Hong, L.; Huang, H. Circ-SMARCA5 suppresses progression of multiple myeloma by targeting miR-767-5p. BMC Cancer; 2019; 19, 937. [DOI: https://dx.doi.org/10.1186/s12885-019-6088-0]

175. Feng, Y.; Zhang, L.; Wu, J.; Khadka, B.; Fang, Z.; Gu, J.; Tang, B.; Xiao, R.; Pan, G.; Liu, J. CircRNA circ_0000190 inhibits the progression of multiple myeloma through modulating miR-767-5p/MAPK4 pathway. J. Exp. Clin. Cancer Res.; 2019; 38, 54. [DOI: https://dx.doi.org/10.1186/s13046-019-1071-9]

176. Kyle, R.A.; Benson, J.T.; Larson, D.R.; Therneau, T.M.; Dispenzieri, A.; Kumar, S.; Melton, L.J.; Rajkumar, S.V. Progression in smoldering Waldenstrom macroglobulinemia: Long-term results. Blood; 2012; 119, pp. 4462-4466. [DOI: https://dx.doi.org/10.1182/blood-2011-10-384768]

177. Morra, E.; Cesana, C.; Klersy, C.; Barbarano, L.; Miqueleiz, S.; Varettoni, M.; Lucchesini, C.; Ricci, F.; Lazzarino, M. Prognostic Factors for Transformation in Asymptomatic Immunoglobulin M Monoclonal Gammopathies. Clin. Lymphoma; 2005; 5, pp. 265-269. [DOI: https://dx.doi.org/10.3816/CLM.2005.n.013]

178. Baldini, L.; Goldaniga, M.; Guffanti, A.; Broglia, C.; Cortelazzo, S.; Rossi, A.; Morra, E.; Colombi, M.; Callea, V.; Pogliani, E. et al. Immunoglobulin M monoclonal gammopathies of undetermined significance and indolent Waldenstrom’s macroglobulinemia recognize the same determinants of evolution into symptomatic lymphoid disorders: Proposal for a common prognostic scoring system. J. Clin. Oncol.; 2005; 23, pp. 4662-4668. [DOI: https://dx.doi.org/10.1200/JCO.2005.06.147]

179. Greco, A.; Tedeschi, A.; Varettoni, M.; Nichelatti, M.; Paris, L.; Ricci, F.; Vismara, E.; Morra, E. Factors predicting transformation of asymptomatic IgM monoclonal gammopathy. Clin. Lymphoma Myeloma Leuk.; 2011; 11, pp. 77-79. [DOI: https://dx.doi.org/10.3816/CLML.2011.n.012]

180. Trojani, A.; Greco, A.; Tedeschi, A.; Lodola, M.; Di Camillo, B.; Ricci, F.; Turrini, M.; Varettoni, M.; Rattotti, S.; Morra, E. Microarray Demonstrates Different Gene Expression Profiling Signatures Between Waldenström Macroglobulinemia and IgM Monoclonal Gammopathy of Undetermined Significance. Clin. Lymphoma Myeloma Leuk.; 2013; 13, pp. 208-210. [DOI: https://dx.doi.org/10.1016/j.clml.2013.02.012]

181. Trojani, A.; Di Camillo, B.; Bossi, L.E.; Leuzzi, L.; Greco, A.; Tedeschi, A.; Frustaci, A.M.; Deodato, M.; Zamprogna, G.; Beghini, A. et al. Identification of a Candidate Gene Set Signature for the Risk of Progression in IgM MGUS to Smoldering/Symptomatic Waldenström Macroglobulinemia (WM) by a Comparative Transcriptome Analysis of B Cells and Plasma Cells. Cancers; 2021; 13, 1837. [DOI: https://dx.doi.org/10.3390/cancers13081837]

182. Alix-Panabières, C.; Pantel, K. Liquid Biopsy: From Discovery to Clinical Application. Cancer Discov.; 2021; 11, pp. 858-873. [DOI: https://dx.doi.org/10.1158/2159-8290.CD-20-1311]

183. Decruyenaere, P.; Offner, F.; Vandesompele, J. Circulating RNA biomarkers in diffuse large B-cell lymphoma: A systematic review. Exp. Hematol. Oncol.; 2021; 10, 13. [DOI: https://dx.doi.org/10.1186/s40164-021-00208-3]

184. Rossi, D.; Diop, F.; Spaccarotella, E.; Monti, S.; Zanni, M.; Rasi, S.; Deambrogi, C.; Spina, V.; Bruscaggin, A.; Favini, C. et al. Diffuse large B-cell lymphoma genotyping on the liquid biopsy. Blood; 2017; 129, pp. 1947-1957. [DOI: https://dx.doi.org/10.1182/blood-2016-05-719641]

185. Roschewski, M.; Dunleavy, K.; Pittaluga, S.; Moorhead, M.; Pepin, F.; Kong, K.; Shovlin, M.; Jaffe, E.S.; Staudt, L.M.; Lai, C. et al. Circulating tumour DNA and CT monitoring in patients with untreated diffuse large B-cell lymphoma: A correlative biomarker study. Lancet Oncol.; 2015; 16, pp. 541-549. [DOI: https://dx.doi.org/10.1016/S1470-2045(15)70106-3]

186. Yeh, P.; Hunter, T.; Sinha, D.; Ftouni, S.; Wallach, E.; Jiang, D.; Chan, Y.-C.; Wong, S.Q.; Silva, M.J.; Vedururu, R. et al. Circulating tumour DNA reflects treatment response and clonal evolution in chronic lymphocytic leukaemia. Nat. Commun.; 2017; 8, 14756. [DOI: https://dx.doi.org/10.1038/ncomms14756]

187. Rolfo, C.; Mack, P.C.; Scagliotti, G.V.; Baas, P.; Barlesi, F.; Bivona, T.G.; Herbst, R.S.; Mok, T.S.; Peled, N.; Pirker, R. et al. Liquid Biopsy for Advanced Non-Small Cell Lung Cancer (NSCLC): A Statement Paper from the IASLC. J. Thorac. Oncol.; 2018; 13, pp. 1248-1268. [DOI: https://dx.doi.org/10.1016/j.jtho.2018.05.030]

188. Siravegna, G.; Marsoni, S.; Siena, S.; Bardelli, A. Integrating liquid biopsies into the management of cancer. Nat. Rev. Clin. Oncol.; 2017; 14, pp. 531-548. [DOI: https://dx.doi.org/10.1038/nrclinonc.2017.14]

189. Bagratuni, T.; Ntanasis-Stathopoulos, I.; Gavriatopoulou, M.; Mavrianou-Koutsoukou, N.; Liacos, C.; Patseas, D.; Kanellias, N.; Migkou, M.; Ziogas, D.C.; Eleutherakis-Papaiakovou, E. et al. Detection of MYD88 and CXCR4 mutations in cell-free DNA of patients with IgM monoclonal gammopathies. Leukemia; 2018; 32, pp. 2617-2625. [DOI: https://dx.doi.org/10.1038/s41375-018-0197-7]

190. Demos, M.G.; Hunter, Z.R.; Xu, L.; Tsakmaklis, N.; Kofides, A.; Munshi, M.; Liu, X.; Guerrera, M.L.; Leventoff, C.R.; White, T.P. et al. Cell-free DNA analysis for detection of MYD88L265P and CXCR4S338X mutations in Waldenström macroglobulinemia. Am. J. Hematol.; 2021; 96, pp. E250-E253. [DOI: https://dx.doi.org/10.1002/ajh.26184] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/33819355]

191. Ntanasis-Stathopoulos, I.; Bagratuni, T.; Gavriatopoulou, M.; Patseas, D.; Liacos, C.; Kanellias, N.; Fotiou, D.; Tsiligkeridou, E.; Andreatou, A.; Mavrianou-Koutsoukou, N. et al. Cell-free DNA analysis for the detection of MYD88 and CXCR4 mutations in IgM monoclonal gammopathies; an update with clinicopathological correlations. Am. J. Hematol.; 2020; 95, pp. E148-E150. [DOI: https://dx.doi.org/10.1002/ajh.25802] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/32242972]

192. Bagratuni, T.; Markou, A.; Patseas, D.; Mavrianou-Koutsoukou, N.; Aktypi, F.; Liacos, C.I.; Sklirou, A.D.; Theodorakakou, F.; Ntanasis-Stathopoulos, I.; Gavriatopoulou, M. et al. Determination of MYD88L265P mutation fraction in IgM monoclonal gammopathies. Blood Adv.; 2022; 6, pp. 189-199. [DOI: https://dx.doi.org/10.1182/bloodadvances.2021005354] [PubMed: https://www.ncbi.nlm.nih.gov/pubmed/34788399]

193. Sole, C.; Arnaiz, E.; Manterola, L.; Otaegui, D.; Lawrie, C.H. The circulating transcriptome as a source of cancer liquid biopsy biomarkers. Semin. Cancer Biol.; 2019; 58, pp. 100-108. [DOI: https://dx.doi.org/10.1016/j.semcancer.2019.01.003]

194. Thakur, B.K.; Zhang, H.; Becker, A.; Matei, I.; Huang, Y.; Costa-Silva, B.; Zheng, Y.; Hoshino, A.; Brazier, H.; Xiang, J. et al. Double-stranded DNA in exosomes: A novel biomarker in cancer detection. Cell Res.; 2014; 24, pp. 766-769. [DOI: https://dx.doi.org/10.1038/cr.2014.44]

195. Caivano, A.; Laurenzana, I.; De Luca, L.; La Rocca, F.; Simeon, V.; Trino, S.; D’Auria, F.; Traficante, A.; Maietti, M.; Izzo, T. et al. High serum levels of extracellular vesicles expressing malignancy-related markers are released in patients with various types of hematological neoplastic disorders. Tumor Biol.; 2015; 36, pp. 9739-9752. [DOI: https://dx.doi.org/10.1007/s13277-015-3741-3]

196. Melo, S.A.; Sugimoto, H.; O’Connell, J.T.; Kato, N.; Villanueva, A.; Vidal, A.; Qiu, L.; Vitkin, E.; Perelman, L.T.; Melo, C.A. et al. Cancer Exosomes Perform Cell-Independent MicroRNA Biogenesis and Promote Tumorigenesis. Cancer Cell; 2014; 26, pp. 707-721. [DOI: https://dx.doi.org/10.1016/j.ccell.2014.09.005]

197. Mitsiades, C.S.; Mitsiades, N.S.; Munshi, N.C.; Richardson, P.G.; Anderson, K.C. The role of the bone microenvironment in the pathophysiology and therapeutic management of multiple myeloma: Interplay of growth factors, their receptors and stromal interactions. Eur. J. Cancer; 2006; 42, pp. 1564-1573. [DOI: https://dx.doi.org/10.1016/j.ejca.2005.12.025]

198. Jalali, S.; Ansell, S.M. Bone marrow microenvironment in Waldenstrom’s Macroglobulinemia. Best Pract. Res. Clin. Haematol.; 2016; 29, pp. 148-155. [DOI: https://dx.doi.org/10.1016/j.beha.2016.08.016]