Full text

Turn on search term navigation

About the Authors:

Seiichi Kanzaki

Affiliation: Department of Pathology, Yokohama City University School of Medicine, Yokohama, Japan

Akira Yamaguchi

* E-mail: [email protected]

Affiliation: Department of Pathology, Yokohama City University School of Medicine, Yokohama, Japan

Kayoko Yamaguchi

Affiliation: Department of Pathology, Yokohama City University School of Medicine, Yokohama, Japan

Yoshitsugu Kojima

Affiliation: Department of Microbiology, Yokohama City University School of Medicine, Yokohama, Japan

Kyoko Suzuki

Affiliation: Department of Psychiatry, Yokohama City University School of Medicine, Yokohama, Japan

Noriko Koumitsu

Affiliation: Department of Pathology, Yokohama City University School of Medicine, Yokohama, Japan

Yoji Nagashima

Affiliation: Department of Pathology, Yokohama City University School of Medicine, Yokohama, Japan

Kiyotaka Nagahama

Affiliation: Department of Pathology, Yokohama City University School of Medicine, Yokohama, Japan

Michiko Ehara

Affiliation: Department of Pathology, Yokohama City University School of Medicine, Yokohama, Japan

Yoshio Hirayasu

Affiliation: Department of Psychiatry, Yokohama City University School of Medicine, Yokohama, Japan

Akihide Ryo

Affiliation: Department of Microbiology, Yokohama City University School of Medicine, Yokohama, Japan

Ichiro Aoki

Affiliation: Department of Pathology, Yokohama City University School of Medicine, Yokohama, Japan

Shoji Yamanaka

Affiliation: Department of Pathology, Yokohama City University School of Medicine, Yokohama, Japan

Introduction

Lysosomal storage disorders (LSDs) arise from functional defects in one or more of the proteins essential to normal lysosome function. This typically involves the enzymes that play a critical role in the intracellular digestion of glycoproteins, glycolipids, glycosaminoglycans, or other macromolecules [1]. GM2 gangliosidoses, one of the major LSDs, are caused by an abnormality in the β-hexosaminidases [1], [2]. β-Hexosaminidase A consists of a heterodimer of an α-subunit (HEXA gene product) and a β-subunit (HEXB gene product) whereas β-Hexosaminidase B is a homodimer of β-subunits. Mutations in the HEXA gene cause Tay-Sachs disease, whereas mutations in the HEXB gene cause Sandhoff disease (SD) [1].

Previous studies have shown that the Hexb-deficient (Hexb−/−) mouse develops an SD-like illness and therefore provides a useful animal model for investigating the pathophysiology of SD [3]–[5]. As with many of the other LSDs, neurodegeneration is a prominent feature of SD and since the neurons accumulate a large amount of GM2 ganglioside and GA2 relative to other tissues in this disease, it is generally thought that the nervous system is its main pathological target. The accumulation of GM2 ganglioside or its derivatives in the nervous system is implicated in unscheduled neuronal cell death [6]. However, recent studies have provided good evidence that GM2 ganglioside and GA2 accumulation can not account for all of the nervous system damage in Hexb−/− mice.

For example, bone marrow transplantation from normal (Hexb+/+)to Hexb−/− mice suppresses neuronal death and improves survival ratios despite having no effect on either β-hexosaminidases activities or ganglioside accumulation in the brain [7]–[9].

We have reported in a previous study that an autoimmune response occurs in Hexb−/− mice with accompanying pathophysiological phenotypes [10]. To determine the role of anti-ganglioside autoantibodies in this earlier study, we additionally disrupted the Fc receptor gamma (FcRγ) gene in the Hexb−/− mouse model, as it plays a key role in immune complex-mediated autoimmune diseases. Clinical symptoms were improved and life spans were extended in the resulting double-null (Hexb−/−FcRγ −/−)mice, suggesting that autoantibodies play an important role in the central nervous system (CNS) pathophysiology in SD. Moreover, we found that age-matched Hexb−/−FcRγ−/− mice had a reduced serum titer of anti-GA2 autoantibody when compared with Hexb−/−FcRγ+/+ mice, suggesting that the FcRγ dependent pathway(s) also contribute to the production of autoantibodies [10]. Recently also, autoantibodies have been implicated in several LSDs and their respective mouse models such as MPSIIIB [11], Batten disease [12]–[15], and Gaucher disease [16], [17]. This suggests that the production of autoantibodies is mediated by common pathway(s) among these diseases although the underlying mechanism of production remains unknown.

The thymus is a central or primary lymphoid organ responsible for the production, differentiation and direction of a population of small lymphocytes that are involved primarily with cell-mediated immunity. Such thymus-dependent lymphocytes are known as T-lymphocytes in contrast to the bone marrow dependent B-lymphocytes with which they intimately co-operate. Recently, alterations in the thymus were observed in several LSD model animals such as feline GM1 gangliosidosis [18]–[20], and twitcher mice [21]. In Hexb−/− mice, GM2 and GA2 were found to have accumulated in the thymus [22]. Impaired selection of invariant natural killer T cells was also observed in this same study [22]. However, whether such alterations in the thymus contribute to the LSD pathophysiology remains unknown.

Over the last decade, a family of chemotactic cytokines known as the chemokines has been found to be involved in the trafficking of leukocytes in both normal and pathological states. Several autoimmune diseases, such as rheumatoid arthritis, systemic lupus erythematosus, multiple sclerosis, and myasthenia gravis, are associated with inappropriate activation of the chemokine network [23]. For example, aberrant high expression of Chemokine (C-X-C motif) ligand 13 (CXCL13) in the thymus in aged (NZB × NZW) F1 (BWF1) mice may play a pivotal role in breaking immune tolerance in the thymus and in recruiting autoantibody-producing B1 cells and CD4+T cells during the development of murine lupus [24]–[26]. B1 cells of different origin and function than conventional B cells (B2 cells) have long been considered to be involved in autoantibody production in autoimmune diseases [27]–[29].

In Hexb−/− mice, cDNA microarray analysis of the CNS has previously revealed an upregulation of inflammatory cytokines/chemokines including CXCL13, dominated by activated microglia/macrophages [8]. The expected mechanism underlying this microglia/macrophage activation was the storage of glycolipids from engulfed apoptotic neurons. Normally, most T cells are eliminated within the cortex or at the cortico-medullary junction via programmed cell death. These T cells are usually rapidly engulfed by macrophages without accompanying immune activation. It is thus possible that if the macrophages cannot degrade apoptotic T cell-derived glycolipids, they are also activated.

We hypothesize that the thymus plays an important role in the production of autoantibodies in SD. We have therefore examined the thymic alterations of Hexb−/− mice during the development of mild to severe progressive neurologic disease in our current study and explored the relationship between these thymic abnormalities and autoimmunity.

Results

Hexb−/−FcRγ+/+ mice develop progressive and age-related thymus atrophy

Our initial analysis indicated that Hexb−/−FcRγ+/+ mice with clinically severe neurologic signs had a severely reduced thymic mass (Fig. 1A). In comparison, age-matched Hexb−/−FcRγ−/− mice had only a slight reduction in their thymic mass. To evaluate whether these thymic alterations were due to hypoplasia or premature involution, thymic tissues from younger mice were also examined quantitatively. A comparison of Hexb+/−FcRγ+/+, Hexb−/−FcRγ+/+ and Hexb−/−FcRγ−/− thymic weights is shown in Figure 1B. The 15 week old Hexb−/−FcRγ+/+ mice showed significant (75%) loss of thymic weight when compared with age-matched Hexb+/−FcRγ+/+ mice. In contrast, there were no significant differences between the younger mice of both genotypes. Hexb−/−FcRγ−/− mice had a slight, but statistically significant, reduction in thymic weight when compared with Hexb+/−FcRγ+/+ mice. Flow cytometric analysis further revealed that CD4+/CD8+ immature T cell ratio was dramatically decreased in the 15 week old Hexb−/−FcRγ+/+ thymus compared with that of the Hexb+/−FcRγ+/+ mice (5.8% vs. 88.0%), whereas the CD4+/CD8− and CD4−/CD8+ T cell ratios were markedly increased (Fig. 1C top panel). Moreover, the CD4−/CD8− non T cell population ratio was also increased in Hexb−/−FcRγ+/+ mice. In Hexb−/−FcRγ−/− mice, the percentages of CD4+/CD8+, CD4+/CD8−, CD4−/CD8+, and CD4−/CD8− cells were 87.1%, 6.8%, 3.2%, and 2.9%, respectively. The absolute number of CD4+/CD8+ T cells per thymus was severely reduced in Hexb−/−FcRγ+/+ mice (Fig. 1C bottom panel). In addition, the absolute number of CD4+/CD8−, CD4−/CD8+, and CD4−/CD8− T cells per thymus was also reduced in Hexb−/−FcRγ+/+ mice.

[Figure omitted. See PDF.]

Figure 1. Hexb−/−FcRγ+/+ mice show progressive, age-related thymus atrophy.

(A) The thymus was removed from 15 week old Hexb+/−FcRγ+/+, Hexb−/−FcRγ+/+ and Hexb−/−FcRγ−/− mice. Scale bar, 1 cm. (B) Thymic tissues from Hexb+/−FcRγ+/+, Hexb−/−FcR+/+ and Hexb−/−FcR−/− mice at 11, 13 and 15 weeks of age were removed and weighed. The data shown are expressed as the mean (S.D. of 3–14 mice for each group per time point. *P<0.01. (C) Thymic cells from Hexb+/−FcR+/+, Hexb−/−FcR+/+ and Hexb−/−FcR−/− mice were stained with CD4 and CD8 antibodies. The percentages of T cell subsets were then determined by flow cytometry. The profiles for each genotype are indicated in the top panels. The absolute cell numbers for each subpopulation of the thymus were calculated from the total number of thymic cells (mean (S.D.; n = 3–4). *P<0.05.

https://doi.org/10.1371/journal.pone.0012105.g001

Histological examination of the thymus from Hexb+/−FcRγ+/+, Hexb−/−FcRγ+/+ and Hexb−/−FcRγ−/− mice

We next undertook histological analysis of the thymic tissues from Hexb+/−FcRγ+/+, Hexb−/−FcRγ+/+ and Hexb−/−FcRγ−/− mice. When examined by light microscopy, the histological findings from younger Hexb−/−FcRγ+/+ mice were found not to significantly differ from Hexb+/−FcRγ+/+ mice. In the 15 week old Hexb−/−FcRγ+/+ mice, the cellular density did not appear to be altered in the medulla of the thymus but the cortices or cortico-medullary junctions were frequently indistinct (Fig. 2). Moreover, many foamy macrophages could be observed not only in the medullary area, but also the cortex area in these mice. Some macrophages were also found to contain hematoxylin-positive nuclear particles in their cytoplasm. Cortices or cortico-medullary junctions were clearly detectable in the thymus of Hexb−/−FcRγ−/− mice and foamy macrophages were also present in Hexb−/−FcRγ−/−mice. We also examined the immunofluorescent analysis of GA2 and thymocyte, for each thymus derived from Hexb+/−FcRγ+/+, Hexb−/−FcRγ+/+ and Hexb−/−FcRγ−/− mice. In the 15 week old Hexb+/−FcRγ+/+ mice, GA2 was stained on the cell membrane of CD4 and/or CD8 positive T cells (Fig. S1). Age matched Hexb−/−FcRγ+/+ mice showed the marked decrease of the T cells in the cortex area. In contrast, GA2 was stained in those areas, and it seems to be accumulating in the cytosol of the foamy cells. The decrease of the T cell and the accumulation of GA2 were not more clearly observed in the presymptomatic stage of Hexb−/−FcRγ+/+, and Hexb−/−FcRγ−/− mice. These results suggest the possibility that the localization of GA2 was moved from T cells to foamy macrophages during the involution.

[Figure omitted. See PDF.]

Figure 2. Histological examination of the thymus from Hexb+/−FcRγ+/+, Hexb−/−FcRγ+/+ and Hexb−/−FcRγ−/− mice.

H&E staining of paraffin-embedded thymic sections from 13 week old Hexb+/−FcRγ+/+, 15 week old Hexb+/−FcRγ+/+, Hexb−/−FcRγ+/+ and Hexb−/−FcRγ−/− mice. The bottom panels show a higher magnification image of the framed area in the top panels. Cor, cortex; Med, medulla. Arrows indicate vacuolated cells. Scale bars, top panel, 100 µm; bottom panel, 50 µm.

https://doi.org/10.1371/journal.pone.0012105.g002

Histological examination of a thymus from a human SD patient

To determine whether thymic alterations can also be detected in a human case of SD, we obtained a H&E stained tissue sample from an SD patient for examination. The histology of this thymic sample revealed that the cortical cells were severely reduced and that the cortico-medullary junctions could not be clearly observed (Fig. 3). Furthermore, most of the cortical and medullary cells harbored a vacuolated cytoplasm.

[Figure omitted. See PDF.]

Figure 3. Histological examination of a thymus from an SD patient.

H&E staining of a paraffin-embedded thymic section from an 11 month-old SD patient. The right panel shows a higher magnification of the framed area in the left panel. Scale bars, left panel, 100 µm; right panel, 50 µm.

https://doi.org/10.1371/journal.pone.0012105.g003

Increased cell death in the thymus of 15 week old Hexb−/−FcRγ+/+ mice

The thymic tissues from 15 week old Hexb+/−FcRγ+/+ and Hexb−/−FcRγ+/+ mice were further analyzed by transmission electron microscopy (TEM). In the Hexb−/−FcRγ+/+ mice, the macrophages contained numerous abnormal nuclear-like electron dense particles, which were not evident in the Hexb+/−FcRγ+/+ thymus (Fig. 4A). These macrophages were also found to contain many vacuoles with characteristics of lysosomal storage vessels. To better understand the progressive reduction observed in the number of thymic cells, we analyzed thymic cell death using a TUNEL assay. TUNEL-positive cells were more frequently found in the Hexb−/−FcRγ+/+ cortex and medulla than in the corresponding regions of the Hexb+/−FcRγ+/+ thymus (Fig. 4B). TUNEL-positive particles could be seen inside the macrophages, and were thought to correspond to the nuclear-like particles observed by TEM. We next quantified the number of apoptotic and necrotic cells by flow cytometry. The results showed that the numbers of AnnexinV+/PI− apoptotic cells in Hexb+/−FcRγ+/+, Hexb−/−FcR+/+ and Hexb−/−FcR−/− mice were 1.28±0.44, 7.06±2.32, and 1.79±0.45 respectively. Moreover, AnnexinV+/PI+ late apoptotic/necrotic cells were found to have increased in the Hexb−/−FcR+/+ thymus (1.47±0.68, 6.45±1.87, and 1.85±0.69, respectively; Fig. 4C). Since thymic cell death in the Hexb−/−FcR−/− mice is decreased, we hypothesized that the immune-complex mediated response is responsible for accelerating thymic cell death in Hexb−/−FcR+/+ mice. Indeed, we found a marked increase in the percentage of IgG/TCR-(double positive T cells (0.53±0.20% vs. 1.96±0.67%), suggesting that IgG is bound to the T cell membrane, in the 15 week old Hexb−/−FcR+/+ mice as compared with age-matched Hexb+/−FcR+/+ mice. The 15 week old Hexb−/−FcR−/− mice also showed a reduction in this population of cells (Fig. 4D).

[Figure omitted. See PDF.]

Figure 4. Increased cell death in the thymus of the 15 week old Hexb−/−FcRγ+/+ mouse.

(A) Thymic sections from 15 week old Hexb−/−FcRγ+/+ and Hexb+/−FcRγ+/+ mice were analyzed by TEM. Left panel, at lower magnification many electron dense materials and vacuoles are evident. Middle panel, nucleus-like electron dense particles and vacuoles are visible in the cytoplasm of the macrophages at higher magnification. Right panel, nuclear particles were not confirmed in the thymus of the Hexb+/−FcRγ+/+ mouse.N, nucleus particle-like structure; MN, macrophage nucleus. (B) Paraffin-embedded thymic sections from Hexb+/−FcRγ+/+, Hexb−/−FcRγ+/+ and Hexb−/−FcRγ−/− mice were stained using the TUNEL method. Scale bar, 50((m. A higher magnification image of the arrow position in the middle panel is shown in the right shoulder frame. (C) Thymic cells from Hexb+/−FcR+/+, Hexb−/−FcR+/+ and Hexb−/−FcR−/− mice were stained with FITC conjugated anti-Annexin V antibody and PI, and the percentages of dying cells were determined by flow cytometry (n = 4–8). *P<0.01. (D) IgG deposition in TCR(-positive T cells analyzed by flow cytometry (n = 3–5). *P≤0.01.

https://doi.org/10.1371/journal.pone.0012105.g004

Macrophage activation and expansion in thymus

The swelling of macrophages is a prominent feature of many LSDs. To confirm whether the swollen cells we observed by H&E staining of our thymic sections were macrophages, we stained these samples with Iba-1 and found that positive cells were rarely observed in the cortices of the 15 week old Hexb+/−FcR+/+ mice. 13 week old Hexb−/−FcR+/+ mice were found not to significantly differ from Hexb+/−FcRγ+/+ mice. On the other hand, numerous Iba-1 positive swelling cells were detected in the 15 week old Hexb−/−FcR+/+ thymus, particularly in the cortex. In Hexb−/−FcR−/− mice, at 15 weeks of age, the numbers of both foamy cells and amoeboid, Iba-1-positive thymic macrophages were substantially reduced compared with the Hexb−/−FcR+/+ mice (Fig. 5A). To determine whether the percentage of macrophages among the total thymic cell population was increased, we performed flow cytometric analysis. The percentage of thymic macrophages from 15 week old Hexb+/−FcR+/+, Hexb−/−FcR+/+ and Hexb−/−FcR−/− mice was 0.93±0.38, 4.36±0.66 and 1.48±0.25% respectively (Fig. 5B). Recent studies have reported that the up-regulation of the Mip-1α correlates with monocyte infiltration and the pathogenesis of SD [30]. To quantify the increase in Mip-1α mRNA in the thymus of 15 week old Hexb−/−FcRγ+/+ mice, the gene expression ratios of Mip-1α relative to ribosomal protein s18 were measured by real-time RT-PCR. A 24.6-fold increase in Mip-1α expression was detected in the thymus of Hexb−/−FcRγ+/+ mice in comparison with Hexb+/−FcRγ+/+ mice. In addition, Hexb−/−FcRγ−/− mice showed a 2.69-fold higher expression of Mip-1α mRNA compared with the Hexb+/−FcRγ+/+ mice (Fig. 5C).

[Figure omitted. See PDF.]

Figure 5. Macrophage activation and expansion.

(A) Thymic tissues from 13 week old Hexb+/−FcR+/+, 15 week old Hexb+/−FcR+/+, Hexb−/−FcR+/+ and Hexb+/−FcR+/+ mice were stained with antibodies against the macrophage marker Iba1 and processed using the avidin-biotin-peroxidase complex (ABC) method. The bottom panels show higher magnifications of the framed areas in the top panels. Scale bars, top panel, 100(µm; bottom panel, 50 µm. (B) Thymic cells from15 week old Hexb+/−FcRγ+/+, Hexb−/−FcRγ+/+ and Hexb−/−FcRγ−/− mice were stained with anti-Iba1 followed by Alexa Fluor 488® conjugated anti-rabbit IgG (H+L), and the percentages of macrophages were determined by flow cytometry (n = 4). *p<0.01. (C) Mip-1α mRNA levels in the thymus from 15week old Hexb−/−FcRγ+/+ and Hexb−/−FcRγ−/− mice were assayed by Real-time RT-PCR and these values were compared with those of the Hexb+/−FcRγ+/+ mouse (mean ± S.D.; n = 5–9). *P<0.05.

https://doi.org/10.1371/journal.pone.0012105.g005

mRNA expression profile in the thymus of Hexb−/−FcRγ+/+mouse

To further elucidate the molecular basis of thymic involution, we performed cDNA microarray analysis to identify the changes in gene expression that accompanied the involution of the thymus. Thymic gene expression of 15 week old Hexb+/−FcRγ+/+ and Hexb−/−FcRγ+/+ mice were examined with Affymetrix® Mouse Genome 430 2.0 Array containing 45101unique mouse gene sequences. The gene expression profile reported in this paper has been deposited in the Gene Expression Omnibus (GEO) database (http://www.ncbi.nlm.nih.gov/geo: accession no. GSE19641). 8018 probes were found to be relatively increased in the thymus of the Hexb−/−FcRγ+/+ mice compared with that of the Hexb+/−FcRγ+/+ mice. On the other hand, the expression of 7604 probes was relatively decreased. The cohort of up-regulated sequences was dominated by genes that play a role in the immune response. In addition, some of these genes are expressed in macrophage lineages such as macrophage expressed gene 1, and colony stimulating factor 2 receptor beta 1. Th2 cytokines were mostly upregulated in the Hexb−/−FcRγ+/+ mice, although Th1 cytokines did not show this increase (Table 1). In addition, B cell-related genes such as CD19, CXCL13 were increased, whereas the T cell-related genes were mostly decreased, in Hexb−/−FcRγ+/+ mice compared with Hexb+/−FcRγ+/+ mice.

[Figure omitted. See PDF.]

Table 1. mRNA expression profile in the thymus of the 15 week old Hexb−/−FcRγ+/+ mouse.

https://doi.org/10.1371/journal.pone.0012105.t001

Marked increase in CXCL13 expression in the thymus of the Hexb−/−FcRγ+/+ mouse

Quantitative differences in CXCL13 expression in the thymus between Hexb+/−FcRγ+/+, Hexb−/−FcRγ+/+ and Hexb−/−FcRγ−/− mice were assayed by real-time RT-PCR (Fig. 6A). There were no significant differences found in 11 or 13 week old Hexb+/−FcRγ+/+, Hexb−/−FcRγ+/+ and Hexb−/−FcRγ−/− mice. However, an extremely high level of CXCL13 expression was observed in the thymus of 15 week old Hexb−/−FcRγ+/+ mice compared with the normalized CXCL13 levels in Hexb+/−FcRγ+/+ (23.3-fold) and Hexb−/−FcRγ−/− mice. The expression of several other cytokines/chemokines such as SDF-1 and TNF-α was not increased in Hexb−/−FcRγ+/+ mice compared with Hexb+/−FcRγ+/+ mice (data not shown). To assess whether the abnormal CXCL13 mRNA expression is thymus-specific, we quantified the CXCL13 mRNA levels in other lymphoid organs. The upregulation of CXCL13 was not found in the lymph nodes or spleen (Fig. 6B). In the thymus of 15week old Hexb−/−FcRγ+/+ mice, the normal architecture was lost and CXCL13 was diffusely distributed throughout the entire region (Fig. 6C). Real-time RT-PCR analysis of magnetic cell sorted leukocyte subpopulations demonstrated that CXCL13 is highly expressed in thymic CD11b-positive cells, which are putatively regarded as macrophages, and also in dendritic cells obtained from 15 week old Hexb−/−FcRγ+/+ mice, but not in CD11b-negative cells from these animals (Fig. 6D).

[Figure omitted. See PDF.]

Figure 6. CXCL13 expression is markedly increased in the thymus of the 15 week old Hexb−/−FcRγ+/+ mouse.

(A) The CXCL13 mRNA levels in the thymus from each of the Hexb+/−FcRγ+/+, Hexb−/−FcRγ+/+ and Hexb−/−FcRγ−/− mice at 11, 13 and 15 weeks of age were determined by real-time RT-PCR and compared with the levels in the Hexb+/−FcRγ+/+ mouse (mean ± S.D.;n = 3–8). *P<0.05. (B) The CXCL13 mRNA levels in the thymus, spleen and lymph nodes from 15 weeks old Hexb+/−FcRγ+/+, Hexb−/−FcRγ+/+ and Hexb−/−FcRγ−/− mice was also measured using real-time RT-PCR and compared with the levels in Hexb+/−FcRγ+/+ mice (mean ± S.D.; n = 4–8). *P<0.05. (C) Thymus cryosections from 13 week old Hexb+/−FcRγ+/+, 15 week old Hexb+/−FcRγ+/+, Hexb−/−FcRγ+/+ and Hexb−/−FcRγ−/− mice were stained with CXCL13 antibodies and detected using DAB. Arrows indicate CXCL13-positive cells. Scale bar, 50 µm. (D) Thymic cells from 15 week old Hexb−/−FcRγ+/+ mice were cell sorted using MACS. The CXCL13 mRNA levels in the CD11b+ and CD11b− cell populations are expressed relative to the normalized CXCL13 levels in whole thymic cells (mean ± S.D.; n = 4). *P<0.05.

https://doi.org/10.1371/journal.pone.0012105.g006

The B1 and B2 cell populations are markedly increased in the thymus of Hexb−/−FcRγ+/+ mouse

The aberrantly high expression of CXCL13 in the thymus of mice with murine lupus plays a pivotal role in recruiting autoantibody-producing B cells. We evaluated whether B cells are increased also in the thymus of 15 week old Hexb−/−FcRγ+/+ mice. By histological examination, we detected massive CD19-positive B cell infiltration and/or expansion in the thymus of the 15 week old Hexb−/−FcRγ+/+ mice (Fig. 7A). In 13 week old Hexb−/−FcRγ+/+ and 15 week old Hexb−/−FcRγ−/− mice, we did not see this B cell expansion. The percentages of CD19+/CD5+/B220lo B1 cells were 0.12±0.04, 0.68±0.28 and 0.23±0.07% in the thymus of 15 week old Hexb+/−FcRγ+/+, Hexb−/−FcRγ+/+ and Hexb−/−FcRγ−/− mice, respectively, and those of CD19+/CD5−/B220hi B2 cells were 0.11±0.05, 0.53±0.19 and 0.17±0.06% respectively (Fig. 7B).

[Figure omitted. See PDF.]

Figure 7. Significant increase in the B1 and B2 cell number in the thymus of 15 week old Hexb−/−FcRγ+/+ mouse.

(A) Thymus cryosections from 13 week old Hexb+/−FcRγ+/+, 15 week old Hexb+/−FcRγ+/+, Hexb−/−FcRγ+/+ and Hexb−/−FcRγ−/− mice were stained with CD19 monoclonal antibodies and detected using the ABC method. The bottom panels show higher magnification images of the framed areas in the top panels. Scale bars, 50 µm. (B) Thymic cells from 15 week old Hexb+/−FcRγ+/+, Hexb−/−FcRγ+/+ and Hexb−/−FcRγ−/− mice were stained with FITC-CD5, PE-B220 and PE-Cy5-CD19 antibodies and the percentages of the B cell subsets were determined by flow cytometry (mean ± S.D.; n = 6–9). *P<0.01.

https://doi.org/10.1371/journal.pone.0012105.g007

Discussion

Sandhoff disease is a lysosomal storage disorder characterized by the absence of β-hexosaminidase and storage of GM2 ganglioside and related glycolipids. It is widely postulated that the CNS is the main pathological target of GM2 gangliosidosis. However, we have previously found that the production of autoantibodies plays an important role in the pathogenesis of neuropathy in Sandhoff disease [10]. In our present study, we observed a dramatic involution of the thymus in 15 week old Hexb−/−FcRγ+/+ mouse. The thymus plays a crucial role in immune system homeostasis, and thymic abnormalities have been previously reported in many autoimmune diseases, such as myasthenia gravis [31], systemic sclerosis [32], in a mouse model of systemic lupus erythematosus [24], and multiple sclerosis [33]. Since autoimmunity is found also in SD, the contribution of thymus abnormalities to the pathogenesis of this disease seems plausible. We therefore tested for immunological alterations in the thymus of Hexb−/−FcR+/+ mice during the development of mild to severe progressive neurologic disease and explored the relationship between thymic abnormalities and autoimmunity.

The thymus of the Hexb−/−FcR+/+ mouse was found to be drastically involuted at the late stages, whereas this degree of involution was reduced in the Hexb−/−FcRγ−/− mouse (Fig. 1A, B), suggesting that this process is dependent on the FcR(chain. The involution itself was found to contain a markedly decreased percentage of immature CD4+/CD8+ T cells and significantly increased populations of CD4+/CD8- cells, CD4-/CD8+ T cells and CD4-/CD8- cells (Fig. 1C, top panel). The absolute number of each subpopulation was decreased, suggesting that the changes in cell number are strongly dependent on the decreased number of CD4+/CD8+ T cells, rather than the increase in CD4+/CD8- cells, CD4-/CD8+ T cells and CD4-/CD8- cells. In contrast, no differences could be clearly observed in the younger Hexb−/−FcR+/+mice. Zhou and co-workers have also shown in their previous study that the development of classical, naive, and memory CD4 and CD8 T cells is unaffected by a Hexb deficiency [34]. The authors did not however discuss the state of the thymus in later stages. In other LSDs, alterations in the last stage thymus have been previously reported in feline GM1 gangliosidosis [19], [20]. Flow cytometric analyses showed a marked decrease in the percentage of immature CD4+/CD8+ T cells and a significant increase in CD4−/CD8+ cells in GM1 mutant cats of greater than 210 days of age when compared with normal age matched cats [19]. Thymic involution has also been described in twitcher mice [21] and may therefore be a common pathological state among the LSDs.

We next examined for histological abnormalities in the thymus of Hexb−/−FcRγ+/+ mice. In the 15 week old animals, the cellular density of the thymic cortices was found to be severely reduced as a result of a decreased number of CD4+/CD8+ cells (Fig. 2). However, numerous macrophages with a “foamy” appearance were found instead in this region. Some of these macrophages contained hematoxylin-positive particles in their cytoplasm, suggesting that the population of apoptotic thymic cells was rapidly increased and/or that the macrophages had a diminished phagocytic capacity. Importantly, a pathology similar to that evident in mouse models appears to exist also in human SD (Fig. 3). Moreover, atrophy of the thymus has previously been described in an autopsy case report by Takahashi et al. [35], and in a personal communication from Tatematsu et al. [36]. These observations suggest that thymic alterations occur in SD in both mouse and human via a common mechanism.

We next found in our mouse model that during thymic involution, nuclear particles in the cytoplasm of the macrophages, apoptotic thymic cells, and IgG deposition to the thymic cells were all increased, particularly in the cortex (Fig. 4). Most thymic lymphocytes are cleared by normal apoptotic processes but increased apoptosis can be observed in some animal models of LSD such as twitcher mice, and feline GM1 gangliosidosis. It is thought that the accumulation of GM2 induces neuronal cell death in GM2 gangliosidosis. Various extra-neural organs also contain many minor ganglioside components. In particular, the thymus has been found to have a very complex and characteristic spectrum of ganglioside species [37], [38]. Gadola et al have previously observed that glycolipids are stored in the thymus [22]. In addition, Zhou et al. have reported that GM1, GM2, GM3, and GT1b can induce apoptosis in thymocytes in vitro [18]. We have also confirmed in our experiments that GM2 enhances thymic cell death, resulting in the formation of in vivo-like T cell subpopulations in vitro (data not shown). However, we also found that the apoptosis and necrosis of thymic cells is decreased in 15 week old Hexb−/−FcRγ−/− mice, although the accumulation levels did not obviously differ from Hexb−/−FcRγ+/+ mice (data not shown). This result suggests that the Fc receptor plays a role in thymic cell death in Hexb−/−FcRγ+/+ mice. We have previously detected the presence of anti-GM2 and anti-GA2 autoantibodies in end stage Hexb−/−FcRγ+/+ mice [10] and also other autoantibodies such as anti-ssDNA (unpublished data), which suggests the presence of polyclonal antibodies in Hexb−/−FcRγ+/+ mice. In our present study, we observed the deposition of IgG on T cell membranes (Fig. 4E). These findings suggest that an anti-T cell autoantibody is produced during the last stages in Hexb−/−FcRγ+/+ mice and that an IgG-FcR mediated pathway plays a role in the thymic involution seen in Hexb−/−FcRγ+/+ mice.The thymus from Hexb−/−FcRγ+/+ mice older than 15 weeks showed a marked increase in the percentage of macrophages, particularly in the cortex (Fig. 5A, B). Additionally, these macrophages were found to contain many nuclear particles in the cytoplasm. These results are consistent with the findings of previous histological experiments using H&E, TEM and TUNEL analyses. Mip-1α which is an important molecule in the pathogenesis of Hexb−/− mice [39], is upregulated in the thymus of 15 week old Hexb−/−FcRγ+/+ mice. The evidence suggests therefore that the increase in the number of macrophages is partly due events that occur peripherally to the thymus.

To better understand the molecular basis of thymic involution, we performed cDNA microarray analysis to identify the changes in gene expression that accompanied involution in this gland. The results revealed an upregulation of immune response associated genes dominated by macrophages. A question that then emerged was how the macrophages were activated at this stage. It is very possible that enhanced cell death and/or the FcRγ dependent signaling pathway is involved in the mechanism. Further analysis is needed to determine whether the FcRγ pathway does contribute to gene expression changes in the thymus. On the other hand, prior to autoantibody production, FcRγ independent pathways may induce thymic alterations. In this regard, previous reports have indicated that in the CNS of Hexb−/− mice, the accumulation of undegraded glycolipids in glial cells might be a trigger of pro-inflammatory cytokine/chemokine production [8], [40]. It has also been reported that the induction of Mip-1α might coincide with the accumulation of N-acetylhexosaminyl glycoconjugates due to a Hexb deficiency in glial cells [31]. It is also known that macrophages accumulate considerable levels of glycolipids within late endosomes/lysosomes during the onset of Sandhoff disease [22].

We detected many vacuoles in the cytoplasm of thymic macrophages, which we speculated to be lysosomal storage (Fig. 4A). Moreover, Periodic acid-Schiff (PAS) positive glycoconjugates were found to accumulate in the cytoplasm of thymic macrophages (data not shown). Previously, Kawane et al. found that DNaseII-deficient mice developed a rheumatoid arthritis-like disease [41] and concluded that, if macrophages cannot degrade mammalian DNA from erythroid precursors and apoptotic cells, they produce TNF-α, which activates synovial cells to produce various cytokines, leading to the development of chronic polyarthritis. DNaseII-deficient mice and Hexb−/−FcRγ+/+ mice have a common phenotype in which undegraded substances accumulate in the macrophages. It has been postulated that a Toll-like receptor independent pathway underlies the molecular mechanism by which cells sense the DNA that has escaped from degradation and initiate an autoimmune response. Other recent reports suggest also that the NALP3 inflammasome senses lysosomal damage as an endogenous ‘danger’ signal and thus induces inflammation in many diseases [42]–[46]. The accumulation of glycolipids within macrophages, and also following the activation of the inflammasome, may therefore be related to the gene expression changes we observe in the thymus of Hexb−/−FcRγ+/+ mice.

CXCL13, an upregulated gene in end stage Hexb−/−FcRγ+/+ mice, was found to be specifically expressed in the thymus, and B1 cells were also detected at increased levels in the thymus (Fig. 6A, B, 7). High expression of CXCL13 has been found previously in many autoimmune diseases, such as myasthenia gravis [31], multiple sclerosis [33], and in a model mouse of SLE [26], and is considered to be associated with autoantibody production. We have shown also in our previous study that a significant elevation of serum antibody levels occurs in the terminal stages of Hexb−/−FcRγ+/+ mice of more than 14 weeks of age [10]. Thus, a high expression of CXCL13 and infiltration of B1 cells in Hexb−/−FcRγ+/+ mice may be a reflection of autoantibody production.

Based on our current results, we propose a mechanism by which thymic alterations occur in Hexb deficient mice as follows. The apoptosis of immature T cells occurs normally in Hexb−/−FcRγ+/+ mice and these apoptotic T cells are engulfed by macrophages. However, macrophages cannot degrade the glycolipids from apoptotic T cells in these animals because of their Hexb deficiency, and thus accumulate these molecules in lysosomes. The macrophages are then activated and produce CXCL13, which promotes chemotaxis toward B1 cells and thus leads to the development of autoimmunity. Once autoantibodies against T cells are produced, the storage of T cell-derived glycolipids by macrophages is enhanced via the autoantibody-dependent phagocytosis of T cells. This undesired loop results in a disrupted immune system and in the production of autoantibodies against neuronal cell antigens or neuronal cell - T cell common antigens such as GA2. Deletion of FcRγ may thus prevent thymic involution by blocking the autoantibody dependent phagocytosis of T cells and suppressing specific gene expression. A reduction of the serum titer against GM2 and GA2 in Hexb−/−FcRγ−/− mice [10] might be related to thymic integrity. Further studies involving other factors, such as functional testing of single lymphocytes and innate immunity, will be needed to further our understanding of autoimmunity in GM2 gangliosidoses.

Materials and Methods

Animals

All mice used in this study were bred and housed under specific pathogen-free (SPF) conditions. All mouse experiments were approved by the Animal Committee at Yokohama City University. SD model mice (Hexb−/− mice; C57BL/6×129/Sv background) were kindly provided by R. L. Proia (NIH, Bethesda, MD) and were bred in a closed colony over 30 generations to inbreed for C57BL/6- and 129/Sv-derived genes [4]. FcRγ gene deficient Hexb−/− mice (Hexb−/−FcRγ−/−) were generated by described as previously [10]. Each experiment utilized tissue from Hexb+/−FcRγ+/+, Hexb−/−FcRγ+/+ and Hexb−/− FcRγ−/− mice. All mice were euthanized by inhalation of sevoflurane and the thymus in each case was collected aseptically for further analysis.

Human thymus

A hematoxylin and eosin (H&E) stained slide of a human thymus, dissected from an 11-month-old male with SD who was autopsied at Kobe Children's Hospital [47], was kindly loaned by Dr. H. Itoh.

Histopathology

The mice were perfused with 10% buffered formalin (Sigma-Aldrich Corp. St. Louis, MO) and processed for paraffin embedding. Deparaffinized and rehydrated sections (4 µm) were stained with H&E or used for immunostaining. Apoptosis was detected via the in situ terminal deoxy nucleotidyl transferase-mediated dUTP nick end labeling (TUNEL) method using an ApopTag® kit (Millipore, Billerica, MA). For staining ionized calcium binding adaptor molecule 1 (Iba-1), sections were treated with antigen retrieval reagent and then incubated with rabbit anti-Iba-1 antibody (Wako Pure Chemical Industries, Ltd., Osaka, Japan) overnight at 4°C. The washed sections were incubated with biotinylated anti-rabbit IgG antibody (Nichirei, Tokyo, Japan) and subsequently incubated with horseradish peroxidase (HRP) labeled streptavidin (Nichirei). The peroxidase reaction was visualized by diaminobenzidine (DAB) and hydrogen peroxide. For frozen sections, the thymus of each mouse were embedded in OCT compound (Sakura Finetek, Torrance, CA) and quickly frozen in dry ice. For the staining of CXCL13, frozen sections (7 µm) were stained with goat anti-CXCL13 pAb (R&D Systems, Inc., Minneapolis, MN), followed by HRP labeled goat anti-rat IgG (Nichirei). For the staining of CD19, frozen sections (7 µm) were stained with Rat anti-CD19 mAb (6D5; Chemicon International, inc., Temecula, CA), followed by HRP labeled goat anti-rat IgG (Nichirei). For Transmission electron microscopy (TEM), thymic tissues was prefixed with 2.5% glutaraldehyde (Merck & Co., Inc., Whitehouse Station, NJ) and postfixed with 1% osmium tetroxide (Wako Pure Chemical). The samples were embedded in Epon 812 resin (TAAB Laboratories, Aldermaston, Berkshire, UK). Ultrathin sections were stained with uranyl acetate and lead citrate (Wako Pure Chemical). Samples were observed with an H-7500 electron microscope (Hitachi, Tokyo, Japan).

Flow cytometry

The remaining thymus samples were gently mechanically dispersed into PBS containing 3% fetal bovine serum (staining buffer) and filtered through a BD Falcon™ Cell Strainer (70 µm pore size; BD Biosciences, Franklin, NJ) to produce single cell suspensions and washed twice with staining buffer. Aliquots of 1×106 thymic cells were incubated with PE-labeled anti-CD4 (GK1.5; eBioscience, Inc., San Diego, CA) and FITC-conjugated anti-CD8 (53-7.6; eBioscience) mouse monoclonal antibodies (mAbs). For three color staining, thymic cells were stained with PE-labeled anti-B220/CD45R (RA3-6B2; BD Biosciences) and FITC-conjugated anti-CD5 (53-7.3RRH; eBioscience) and PE-Cy5 conjugated CD19 (MB19-1; eBioscience) mAbs. For the staining of thymic macrophages, the thymic cells were stained with anti-Iba1 (Wako Pure Chemical), followed by Alexa Fluor ®-488 labeled anti-rabbit IgG (H+L) (Invitrogen, Carlsbad, CA). For the detection of autoantibody deposition on T cells, thymic cells were stained with Goat anti-mouse IgG (Southern Biotech, Birmingham, AL) followed by Alexa Fluor®-488 labeled Donkey anti-Goat IgG (H+L) (Invitrogen) and PE labeled anti-TCRβ (H57-597; eBioscience). Flow cytometric analysis was carried out using FACScan™ with CELLQuest™ software (BD Biosciences) or with FACS Canto II™ with FACSDiva™ software (BD Biosciences).

cDNA microarray

Pooled thymic RNA samples were obtained from two 15 weeks old Hexb−/− mice and two strain-matched, 15 weeks old Hexb+/−mice. cDNA were synthesized by GeneChip T7-Oligo(dT) Promoter Primer Kit (Affymetrix, Inc, Santa Clara, CA) and TaKaRa cDNA Synthesis Kit (TaKaRa Bio Inc, Shiga, Japan) from 10 µg total RNA. Biotinylated cRNA were synthesized by IVT Labeling Kit (Affymetrix). Following fragmentation, 10 µg of cRNA were hybridized for 16 hr at 45°C on GeneChip Mouse Genome 430 2.0 Array (Affymetrix) containing 45101 unique mouse genes. GeneChips were washed and stained in the Affymetrix Fluidics Station 450. GeneChips were scanned using GeneChip Scanner 3000 7G. Single Array Analysis were calculated by Microarray Suite version 5.0 (MAS5.0) with Affymetrix default setting and global scaling as normalization method. The trimmed mean target intensity of each array was arbitrarily set to 500. Signals were calculated using the One-Step Tukey's Biweight Estimate which yields a robust weighted mean. The signal log ratio was computed using a one-step Tukey's Biweight method by taking a mean of the log ratios of the probe pair intensities across the two arrays. All data is MIAME compliant and that the raw data has been deposited in GEO.

Real-time RT-PCR

Total RNA was purified with TRIzol Reagent (Invitrogen). To determine the high CXCL13-expressing cells, a magnetic cell sorting system was used for the RNA preparation. Briefly, a 1×106 thymic cell suspension from 15 week old Hexb−/−FcRγ+/+ mice was stained with CD11b MicroBeads (Miltenyi Biotec, Bergisch Gladbach, Germany) and separated using an MS Column (Miltenyi Biotec), and a MiniMACS® Separator (Miltenyi Biotec). cDNA was synthesized from total RNA by reverse transcription using a commercial cDNA synthesis kit (TaKaRa Bio Inc). cDNA synthesized from 500 ng of total RNA was used as the template in each reaction. The relative gene expression levels were determined using the SYBR® Premix Ex Taq™ II (TaKaRa Bio Inc). The primer sets for ribosomal protein s18 (Rps18) and tumor necrosis factor-alpha (TNF-α) were obtained from TaKaRa Bio. The primer set for macrophage inflammatory protein-1 alpha (Mip-1α) has been described previously [31]. The primers used to amplify Chemokine (C-X-C motif) ligand 13 (CXCL13) are 5′-TCTCTCCAGGCCACGGTATTCT-3′ (forward, F) and, 5′-ACCATTTGGCACGAGGATTCAC (reverse, R) and for stromal cell-derived factor 1 (SDF-1) are 5′-GAGCCAACGTCAAGCATCTG-3′ (F) and 5′-CGGGTCAATGCACACTTGTC-3′ (R). Rps18 was amplified in each reaction simultaneously as a standard control. The fluorescence changes from each well were monitored using an ABI PRISM® 7500 Sequence Detection System (Perkin Elmer, Inc, Waltham, MA).

Statistical analysis

Statistical analysis was performed using the Student's t test. A 95% confidence limit was taken as significant.

Supporting Information

[Figure omitted. See PDF.]

Figure S1.

Immunofluorescent analysis of GA2 and thymocyte, for each thymus derived from Hexb+/−FcRγ+/+, Hexb−/−FcRγ+/+ and Hexb−/−FcRγ−/− mice. Frozen section of the thymus from 15 week old Hexb+/−FcRγ+/+, Hexb−/−FcRγ+/+ and Hexb−/−FcRγ−/− and 13 week old Hexb−/−FcRγ+/+ mice were labeled GA2 with Alexa Fluor®-488, CD4 and CD8 with Alexa Fluor®-594, and nuclear with Hoechst 33258, respectively. Arrows indicate the deposition of GA2 in the cytosol of the CD4/8 negative cells. Scale bar, 20 μm.

https://doi.org/10.1371/journal.pone.0012105.s001

(0.43 MB PDF)

Acknowledgments

We thank Dr. Richard L. Proia for providing the Hexb−/− mice, Dr. Toshiyuki Takai for providing the FcRγ−/− mice, Dr. Hiroshi Ito for providing the H&E stained human SD autopsy tissue slides, Dr. Masae Tatematsu for personal communications of relevance to this study, and Dr. Haruto Hojo for advice and expertise in performing TEM. We additionally thank Tamiyo Taniguchi, Shizuko Kobayashi and Sayuri Kanaya for their technical and secretarial assistance.

Author Contributions

Conceived and designed the experiments: SK AY SY. Performed the experiments: SK AY KY YK KS NK ME. Analyzed the data: SK AY IA SY. Contributed reagents/materials/analysis tools: KS YN KN YH AR IA. Wrote the paper: SK AY SY.

Citation: Kanzaki S, Yamaguchi A, Yamaguchi K, Kojima Y, Suzuki K, Koumitsu N, et al. (2010) Thymic Alterations in GM2 Gangliosidoses Model Mice. PLoS ONE5(8): e12105. https://doi.org/10.1371/journal.pone.0012105

References

1. Neufeld EF (1991) Lysosomal storage diseases. Annu Rev Biochem 60: 257–280.EF Neufeld1991Lysosomal storage diseases.Annu Rev Biochem60257280

2. Gravel RA, Clarke JTR, Kaback MM, Mahuran D, Sandhoff K, et al. (2001) The GM2 gangliosidoses. In: Scriver CR, Beaudet AL, Sly WS, editors. The metabolic and molecular basis of inherited disease. 7th ed. New York: McGraw-Hill. New York. pp. 3827–3876.RA GravelJTR ClarkeMM KabackD. MahuranK. Sandhoff2001The GM2 gangliosidoses.CR ScriverAL BeaudetWS SlyThe metabolic and molecular basis of inherited disease. 7th edNew YorkMcGraw-Hill. New York38273876

3. Yamanaka S, Johnson ON, Norflus F, Boles DJ, Proia RL (1994) Structure and expression of the mouse β-hexosaminidase genes, Hexa and Hexb. Genomics 1994 21: 588–596.S. YamanakaON JohnsonF. NorflusDJ BolesRL Proia1994Structure and expression of the mouse β-hexosaminidase genes, Hexa and Hexb.Genomics 199421588596

4. Sango K, Yamanaka S, Hoffmann A, Okuda Y, Grinberg A, et al. (1995) Mouse models of Tay-Sachs and Sandhoff diseases differ in neurologic phenotype and ganglioside metabolism. Mice lacking both subunits of lysosomal β-hexosaminidase display gangliosidosis and mucopolysaccharidosis. Nat Genet 11: 170–176.K. SangoS. YamanakaA. HoffmannY. OkudaA. Grinberg1995Mouse models of Tay-Sachs and Sandhoff diseases differ in neurologic phenotype and ganglioside metabolism. Mice lacking both subunits of lysosomal β-hexosaminidase display gangliosidosis and mucopolysaccharidosis.Nat Genet11170176

5. Phaneuf D, Wakamatsu N, Huang J-Q, Borowski A, Peterson AC, et al. (1996) Dramatically different phenotypes in mouse models of human Tay-Sachs and Sandhoff diseases. Hum Mol Genet 5: 1–14.D. PhaneufN. WakamatsuJ-Q HuangA. BorowskiAC Peterson1996Dramatically different phenotypes in mouse models of human Tay-Sachs and Sandhoff diseases.Hum Mol Genet5114

6. Huang JQ, Trasler JM, Igdoura S, Michaud J, Hanal N, et al. (1997) Apoptotic cell death in mouse models of GM2 gangliosidosis and observations on human Tay-Sachs and Sandhoff diseases. Hum Mol Genet 6: 1879–1885.JQ HuangJM TraslerS. IgdouraJ. MichaudN. Hanal1997Apoptotic cell death in mouse models of GM2 gangliosidosis and observations on human Tay-Sachs and Sandhoff diseases.Hum Mol Genet618791885

7. Norflus F, Tifft CJ, McDonald MP, Goldstein G, Crawley JN, et al. (1999) Bone marrow transplantation prolongs life span and ameliorates neurologic manifestations in Sandhoff disease mice. J Clin Invest 101: 1881–1888.F. NorflusCJ TifftMP McDonaldG. GoldsteinJN Crawley1999Bone marrow transplantation prolongs life span and ameliorates neurologic manifestations in Sandhoff disease mice.J Clin Invest10118811888

8. Wada R, Tifft CJ, Proia RL (2000) Microglial activation precedes acute neurodegeneration in Sandhoff disease and is suppressed by bone marrow transplantation. Proc Natl Acad Sci USA 97: 10954–10959.R. WadaCJ TifftRL Proia2000Microglial activation precedes acute neurodegeneration in Sandhoff disease and is suppressed by bone marrow transplantation.Proc Natl Acad Sci USA971095410959

9. Castaneda JA, Lim MJ, Cooper JD, Pearce DA (2008) Immune system irregularities in lysosomal storage disorders. Acta Neuropathol 115: 159–174.JA CastanedaMJ LimJD CooperDA Pearce2008Immune system irregularities in lysosomal storage disorders.Acta Neuropathol115159174

10. Yamaguchi A, Katsuyama K, Nagahama K, Takai T, Aoki I, et al. (2004) Possible role of autoantibodies in the pathophysiology of GM2 gangliosidoses. J Clin Invest 113: 200–208.A. YamaguchiK. KatsuyamaK. NagahamaT. TakaiI. Aoki2004Possible role of autoantibodies in the pathophysiology of GM2 gangliosidoses.J Clin Invest113200208

11. DiRosario J, Divers E, Wang C, Etter J, Charrier A, et al. (2008) Innate and adaptive immune activation in the brain of MPS IIIB mouse model. J Neurosci Res 87: 978–990.J. DiRosarioE. DiversC. WangJ. EtterA. Charrier2008Innate and adaptive immune activation in the brain of MPS IIIB mouse model.J Neurosci Res87978990

12. Chattopadhyay S, Ito M, Cooper JD, Brooks AI, Curran TM, et al. (2002) An autoantibody inhibitory to glutamic acid decarboxylase in the neurodegenerative disorder Batten disease. Hum Mol Genet 11: 1421–1431.S. ChattopadhyayM. ItoJD CooperAI BrooksTM Curran2002An autoantibody inhibitory to glutamic acid decarboxylase in the neurodegenerative disorder Batten disease.Hum Mol Genet1114211431

13. Lim MJ, Alexander N, Benedict JW, Chattopadhyay S, Shemilt SJA, et al. (2007) IgG entry and deposition are components of the neuroimmune response in Batten disease. Neurobiol Dis 25: 239–251.MJ LimN. AlexanderJW BenedictS. ChattopadhyaySJA Shemilt2007IgG entry and deposition are components of the neuroimmune response in Batten disease.Neurobiol Dis25239251

14. Ramirez-Montealegre D, Chattopadhyay S, Curran TM, Wasserfall C, Pritchard L, et al. (2005) Autoimmunity to glutamic acid decarboxylase in the neurodegenerative disorder Batten disease. Neurology 64: 743–745.D. Ramirez-MontealegreS. ChattopadhyayTM CurranC. WasserfallL. Pritchard2005Autoimmunity to glutamic acid decarboxylase in the neurodegenerative disorder Batten disease.Neurology64743745

15. Pearce DA, Atkinson M, Tagle DA (2004) Glutamic acid decarboxylase autoimmunity in Batten disease and other disorders. Neurology 63: 2001–2005.DA PearceM. AtkinsonDA Tagle2004Glutamic acid decarboxylase autoimmunity in Batten disease and other disorders.Neurology6320012005

16. Shoenfeld Y, Beresovski A, Zharhary D, Tomer Y, Swissa M, et al. (1995) Natural autoantibodies in sera of patients with Gaucher's disease. J Clin Immunol 15: 363–372.Y. ShoenfeldA. BeresovskiD. ZharharyY. TomerM. Swissa1995Natural autoantibodies in sera of patients with Gaucher's disease.J Clin Immunol15363372

17. Balreira A, Lacerda L, Miranda CS, Arosa FA (2005) Evidence for a link between sphingolipid metabolism and expression of CD1d and MHC-class II: monocytes from Gaucher disease patients as a model. Br J Haematol 129: 667–676.A. BalreiraL. LacerdaCS MirandaFA Arosa2005Evidence for a link between sphingolipid metabolism and expression of CD1d and MHC-class II: monocytes from Gaucher disease patients as a model.Br J Haematol129667676

18. Zhou J, Shao H, Cox NR, Baker HJ, Ewald SJ (1998) Gangliosides enhance apoptosis of thymocytes. Cell Immunol 183: 90–98.J. ZhouH. ShaoNR CoxHJ BakerSJ Ewald1998Gangliosides enhance apoptosis of thymocytes.Cell Immunol1839098

19. Cox NR, Ewald SJ, Morrison NE, Gentry AS, Schuler M, et al. (1998) Thymic alterations in feline GM1 gangliosidosis. Vet Immunol Immunopathol 63: 335–353.NR CoxSJ EwaldNE MorrisonAS GentryM. Schuler1998Thymic alterations in feline GM1 gangliosidosis.Vet Immunol Immunopathol63335353

20. Zhou J, Cox NR, Ewald SJ, Morrison NE, Basker HJ (1998) Evaluation of GM1 ganglioside-mediated apoptosis in feline thymocytes. Vet Immunol Immunopathol 66: 25–42.J. ZhouNR CoxSJ EwaldNE MorrisonHJ Basker1998Evaluation of GM1 ganglioside-mediated apoptosis in feline thymocytes.Vet Immunol Immunopathol662542

21. Galbiati F, Basso V, Cantuti L, Givogri MI, Lopez-Rosas A, et al. (2007) Autonomic denervation of lymphoid organs leads to epigenetic immune atrophy in a mouse model of Krabbe disease. J Neurosci 27: 13730–13738.F. GalbiatiV. BassoL. CantutiMI GivogriA. Lopez-Rosas2007Autonomic denervation of lymphoid organs leads to epigenetic immune atrophy in a mouse model of Krabbe disease.J Neurosci271373013738

22. Gadola SD, Silk JD, Jeans A, Illarionov PA, Salio M, et al. (2006) Impaired selection of invariant natural killer T cells in diverse mouse models of glycosphingolipid lysosomal storage diseases. J Exp Med 203: 2293–2303.SD GadolaJD SilkA. JeansPA IllarionovM. Salio2006Impaired selection of invariant natural killer T cells in diverse mouse models of glycosphingolipid lysosomal storage diseases.J Exp Med20322932303

23. Gerard C, Rollins BJ (2001) Chemokines and disease. Nat Immunol 2: 108–115.C. GerardBJ Rollins2001Chemokines and disease.Nat Immunol2108115

24. Ishikawa S, Sato T, Abe M, Nagai S, Onai N, et al. (2001) Aberrant high expression of B lymphocyte chemokine (BLC/CXCL13) by CD11b+CD11c+ dendritic cells in murine lupus and preferential chemotaxis of B1 cells towards BLC. J Exp Med 193: 1393–1402.S. IshikawaT. SatoM. AbeS. NagaiN. Onai2001Aberrant high expression of B lymphocyte chemokine (BLC/CXCL13) by CD11b+CD11c+ dendritic cells in murine lupus and preferential chemotaxis of B1 cells towards BLC.J Exp Med19313931402

25. Sato T, Ishikawa S, Akadegawa K, Ito T, Yurino H, et al. (2004) Aberrant B1 cell migration into the thymus results in activation of CD4 T cells through its potent antigen-presenting activity in the development of murine lupus. Eur J Immunol 34: 3346–3358.T. SatoS. IshikawaK. AkadegawaT. ItoH. Yurino2004Aberrant B1 cell migration into the thymus results in activation of CD4 T cells through its potent antigen-presenting activity in the development of murine lupus.Eur J Immunol3433463358

26. Ishikawa S, Matsushima K (2007) Aberrant B1 cell trafficking in a murine model for lupus. Front Biosci 12: 1790–1803.S. IshikawaK. Matsushima2007Aberrant B1 cell trafficking in a murine model for lupus.Front Biosci1217901803

27. Hayakawa K, Hardy RR, Parks DR, Herzenberg LA (1983) The “Ly-1 B” cell subpopulations in normal, immunodefective, and autoimmune mice. J Exp Med 157: 202–218.K. HayakawaRR HardyDR ParksLA Herzenberg1983The “Ly-1 B” cell subpopulations in normal, immunodefective, and autoimmune mice.J Exp Med157202218

28. Herzenberg LA, Stall AM, Lalor PA, Sidman C, Moore WA, et al. (1986) The Ly-1 B cell lineage. Immunol Rev 93: 81–102.LA HerzenbergAM StallPA LalorC. SidmanWA Moore1986The Ly-1 B cell lineage.Immunol Rev9381102

29. Herzenberg LA (2000) B-1 cells: the lineage question revisited. Immunol Rev 175: 9–22.LA Herzenberg2000B-1 cells: the lineage question revisited.Immunol Rev175922

30. Wu Y-P, Proia RL (2004) Deletion of macrophage-inflammatory protein 1α retards neurodegeneration in Sandhoff disease mice. Proc Natl Acad Sci U S A 101: 8425–8430.Y-P WuRL Proia2004Deletion of macrophage-inflammatory protein 1α retards neurodegeneration in Sandhoff disease mice.Proc Natl Acad Sci U S A10184258430

31. Meraouna A, Cizeron-Clairac G, Panse RL, Bismuth J, Truffault F, et al. (2006) The chemokine CXCL13 is a key molecule in autoimmune myasthenia gravis. Blood 108: 432–440.A. MeraounaG. Cizeron-ClairacRL PanseJ. BismuthF. Truffault2006The chemokine CXCL13 is a key molecule in autoimmune myasthenia gravis.Blood108432440

32. Ferri C, Colaci M, Battolla L, Giuggioli D, Sebastiani M (2006) Thymus alterations and systemic sclerosis. Rheumatology (Oxford) 45: 72–75.C. FerriM. ColaciL. BattollaD. GiuggioliM. Sebastiani2006Thymus alterations and systemic sclerosis.Rheumatology (Oxford)457275

33. Cavallotti D, D'Andrea V, Pastore FS, Leali FMT, Cavallotti C (2005) Pathogenesis of some neurological immune ultrastructural and morphometrical observations on rat thymus. Neurol Res 27: 41–46.D. CavallottiV. D'AndreaFS PastoreFMT LealiC. Cavallotti2005Pathogenesis of some neurological immune ultrastructural and morphometrical observations on rat thymus.Neurol Res274146

34. Zhou D, Mattner J, Cantu C, Schrantz N, Yin N, Gao Y, et al. (2004) Lysosomal glycosphingolipid recognition by NKT cells. Science 306: 1786–1789.D. ZhouJ. MattnerC. CantuN. SchrantzN. YinY. Gao2004Lysosomal glycosphingolipid recognition by NKT cells.Science30617861789

35. Takahashi A, Saito K, Koizumi Y (1974) An autopsy case of Sandhoff disease. Beitr Pathol 152: 418–28.A. TakahashiK. SaitoY. Koizumi1974An autopsy case of Sandhoff disease.Beitr Pathol15241828

36. Tatematsu M, Imaida K, Ito N, Togari H, Suzuki Y, et al. (1981) Sandhoff disease. Acta Pathol Jpn 31: 503–512.M. TatematsuK. ImaidaN. ItoH. TogariY. Suzuki1981Sandhoff disease.Acta Pathol Jpn31503512

37. Schwarting GA, Gajewski A (1981) Glycolipids of murine lymphocyte subpopulations: a defect in the levels of sialidase-sensitive sialosylated asialo GM1 in beige mouse lymphocytes. J Immunol 126: 2403–2407.GA SchwartingA. Gajewski1981Glycolipids of murine lymphocyte subpopulations: a defect in the levels of sialidase-sensitive sialosylated asialo GM1 in beige mouse lymphocytes.J Immunol12624032407

38. Schwarting GA, Gajewski A (1983) Glycolipids of murine lymphocyte subpopulations. Structural characterization of thymus gangliosides. J Biol Chem 258: 5893–5898.GA SchwartingA. Gajewski1983Glycolipids of murine lymphocyte subpopulations. Structural characterization of thymus gangliosides.J Biol Chem25858935898

39. Tsuji D, Kuroki A, Ishibashi Y, Itakura T, Kuwahara J, et al. (2005) Specific induction of macrophage inflammatory protein 1-α in glial cells of Sandhoff disease model mice associated with accumulation of N-acetylhexosaminyl glycoconjugates. J Neurochem 92: 1497–1507.D. TsujiA. KurokiY. IshibashiT. ItakuraJ. Kuwahara2005Specific induction of macrophage inflammatory protein 1-α in glial cells of Sandhoff disease model mice associated with accumulation of N-acetylhexosaminyl glycoconjugates.J Neurochem9214971507

40. Jeyakumar M, Thomas R, Elliot-Smith E, Smith DA, van der Spoel AC, et al. (2003) Central nervous system inflammation is a hallmark of pathogenesis in mouse models of GM1 and GM2 gangliosidosis. Brain 126: 974–987.M. JeyakumarR. ThomasE. Elliot-SmithDA SmithAC van der Spoel2003Central nervous system inflammation is a hallmark of pathogenesis in mouse models of GM1 and GM2 gangliosidosis.Brain126974987

41. Kawane K, Ohtani M, Miwa K, Kizawa T, Kanbara Y, et al. (2004) Chronic polyarthritis caused by mammalian DNA that escapes from degradation in macrophages. Nature 443: 998–1002.K. KawaneM. OhtaniK. MiwaT. KizawaY. Kanbara2004Chronic polyarthritis caused by mammalian DNA that escapes from degradation in macrophages.Nature4439981002

42. Halle A, Hornung V, Petzold GC, Stewart CR, Monks BG, et al. (2008) The NALP3 inflammasome is involved in the innate immune response to amyloid-β. Nat Immunol 9: 857–865.A. HalleV. HornungGC PetzoldCR StewartBG Monks2008The NALP3 inflammasome is involved in the innate immune response to amyloid-β.Nat Immunol9857865

43. Hornung V, Bauernfeind F, Halle A, Samstad EO, Kono H, et al. (2008) Silica crystals and aluminum salts activate the NALP3 inflammasome through phagosomal destabilization. Nat Immunol 9: 847–856.V. HornungF. BauernfeindA. HalleEO SamstadH. Kono2008Silica crystals and aluminum salts activate the NALP3 inflammasome through phagosomal destabilization.Nat Immunol9847856

44. Dostert C, Petrilli V, Van BR, Steele C, Mossman BT, et al. (2008) Innate immune activation through Nalp3 inflammasome sensing of asbestos and silica. Science 320: 674–677.C. DostertV. PetrilliBR VanC. SteeleBT Mossman2008Innate immune activation through Nalp3 inflammasome sensing of asbestos and silica.Science320674677

45. Muruve DA, Petrilli V, Zaiss AK, White LR, Clark SA, et al. (2008) The inflammasome recognizes cytosolic microbial and host DNA and triggers an innate immune response. Nature 452: 103–107.DA MuruveV. PetrilliAK ZaissLR WhiteSA Clark2008The inflammasome recognizes cytosolic microbial and host DNA and triggers an innate immune response.Nature452103107

46. Petrilli V, Dostert C, Muruve DA, Tschopp J (2007) The inflammasome: a danger sensing complex triggering innate immunity. Curr Opin Immunol 19: 615–622.V. PetrilliC. DostertDA MuruveJ. Tschopp2007The inflammasome: a danger sensing complex triggering innate immunity.Curr Opin Immunol19615622

47. Itoh H, Tanaka J, Morihana Y, Tamaki T (1984) The fine structure of cytoplasmic inclusions in brain and other visceral organs in Sandhoff disease. Brain Dev 6: 467–474.H. ItohJ. TanakaY. MorihanaT. Tamaki1984The fine structure of cytoplasmic inclusions in brain and other visceral organs in Sandhoff disease.Brain Dev6467474

Word count: 8618

Show less

© 2010 Kanzaki et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License: https://creativecommons.org/licenses/by/4.0/ (the “License”), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. Notwithstanding the ProQuest Terms and Conditions, you may use this content in accordance with the terms of the License.

Abstract

Background

Sandhoff disease is a lysosomal storage disorder characterized by the absence of β-hexosaminidase and storage of GM2 ganglioside and related glycolipids. We have previously found that the progressive neurologic disease induced in Hexb−/− mice, an animal model for Sandhoff disease, is associated with the production of pathogenic anti-glycolipid autoantibodies.

Methodology/Principal Findings

In our current study, we report on the alterations in the thymus during the development of mild to severe progressive neurologic disease. The thymus from Hexb−/− mice of greater than 15 weeks of age showed a marked decrease in the percentage of immature CD4+/CD8+ T cells and a significantly increased number of CD4+/CD8− T cells. During involution, the levels of both apoptotic thymic cells and IgG deposits to T cells were found to have increased, whilst swollen macrophages were prominently observed, particularly in the cortex. We employed cDNA microarray analysis to monitor gene expression during the involution process and found that genes associated with the immune responses were upregulated, particularly those expressed in macrophages. CXCL13 was one of these upregulated genes and is expressed specifically in the thymus. B1 cells were also found to have increased in the thy mus. It is significant that these alterations in the thymus were reduced in FcRγ additionally disrupted Hexb−/− mice.

Conclusions/Significance

These results suggest that the FcRγ chain may render the usually poorly immunogenic thymus into an organ prone to autoimmune responses, including the chemotaxis of B1 cells toward CXCL13.

Details

Title
Thymic Alterations in GM2 Gangliosidoses Model Mice
Author
Kanzaki, Seiichi; Yamaguchi, Akira; Yamaguchi, Kayoko; Kojima, Yoshitsugu; Suzuki, Kyoko; Koumitsu, Noriko; Nagashima, Yoji; Nagahama, Kiyotaka; Ehara, Michiko; Hirayasu, Yoshio; Akihide Ryo; Aoki, Ichiro; Yamanaka, Shoji
First page
e12105
Section
Research Article
Publication year
2010
Publication date
Aug 2010
Publisher
Public Library of Science
e-ISSN
19326203
Source type
Scholarly Journal
Language of publication
English
DOI
https://doi.org/10.1371/journal.pone.0012105
ProQuest document ID
1292249085
Copyright
© 2010 Kanzaki et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License: https://creativecommons.org/licenses/by/4.0/ (the “License”), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. Notwithstanding the ProQuest Terms and Conditions, you may use this content in accordance with the terms of the License.