Full text

Turn on search term navigation

About the Authors:

Akihiro Shindo

* E-mail: [email protected]

Affiliation: Department of Neurology, Mie University Graduate School of Medicine, 2–174 Edobasih, Tsu, Mie, Japan

Hiroshi Tanemura

Affiliation: Department of Neurosurgery, Mie University Graduate School of Medicine, 2–174 Edobashi, Tsu, Mie, Japan

Kenichiro Yata

Affiliation: Department of Neurology, Mie University Graduate School of Medicine, 2–174 Edobasih, Tsu, Mie, Japan

Kazuhide Hamada

Affiliation: Department of Neurosurgery, Mie University Graduate School of Medicine, 2–174 Edobashi, Tsu, Mie, Japan

Masunari Shibata

Affiliation: Department of Neurology, Mie University Graduate School of Medicine, 2–174 Edobasih, Tsu, Mie, Japan

Yasuyuki Umeda

Affiliation: Department of Neurosurgery, Mie University Graduate School of Medicine, 2–174 Edobashi, Tsu, Mie, Japan

Fumio Asakura

Affiliation: Department of Neurosurgery, Mie University Graduate School of Medicine, 2–174 Edobashi, Tsu, Mie, Japan

Naoki Toma

Affiliation: Department of Neurosurgery, Mie University Graduate School of Medicine, 2–174 Edobashi, Tsu, Mie, Japan

Hiroshi Sakaida

Affiliation: Department of Neurosurgery, Mie University Graduate School of Medicine, 2–174 Edobashi, Tsu, Mie, Japan

Takao Fujisawa

Affiliation: Institute for Clinical Research, Mie National Hospital, 357 Ozatokubota, Tsu, Mie, Japan

Waro Taki

Affiliation: Department of Neurosurgery, Mie University Graduate School of Medicine, 2–174 Edobashi, Tsu, Mie, Japan

Hidekazu Tomimoto

Affiliation: Department of Neurology, Mie University Graduate School of Medicine, 2–174 Edobasih, Tsu, Mie, Japan

Introduction

Atherosclerosis is a systemic arterial disease involving the intima of large- and medium-sized systemic arteries, including the aorta, carotid, coronary, and peripheral arteries. Currently, atherosclerosis is assumed to result from complex endothelial dysfunction induced by elevated and modified low-density lipoproteins, hypertension, smoking-induced toxins, free radicals, pathogenic microorganisms, shear stress, and/or a combination of these and other factors that lead to a compensatory inflammatory response [1]. Inflammation is currently recognized as an important factor involved in the development, progression, and rupture of atherosclerotic plaques, and subsequently, thrombosis [2]–[6]. Moreover, endothelial dysfunction is characterized by decreased nitric oxide synthesis and local oxidation of circulating lipoproteins and their entry into the vessel wall [7].

The levels of circulating inflammatory biomarkers, including high-sensitivity C-reactive protein (hs-CRP), and interleukin (IL)-6, are important predictors of future vascular events [8], [9]. Recently, pentraxin 3 (PTX3) has also been implicated in cardiovascular events [10].

PTX3, a prototypical member of the long pentraxin family, has a C-terminal sequence homology with the classic short pentraxins, CRP and serum amyloid P component. PTX3 is abundantly produced by various cells in atherosclerotic lesions, including monocytes, macrophages, endothelial cells, vascular smooth muscle cells, fibroblasts, dendritic cells, and adipocytes, whereas CRP is mainly produced in the liver [11]. These findings suggest that PTX3 levels reflect local inflammation at atherosclerotic lesions more accurately than does CRP.

In this study, we analyzed the relationship between carotid plaque vulnerability and serum inflammatory biomarkers and determined the expression of these soluble factors in carotid plaques.

Materials and Methods

Subjects

Forty-one patients underwent carotid artery stenting (CAS) and 17 patients underwent carotid endarterectomy (CEA) for symptomatic or asymptomatic carotid stenosis at Mie University Hospital between September 2009 and March 2012 in this prospective study. Patients who met our criteria for CAS included those diagnosed with carotid lesions that were either symptomatic with >50% stenosis or were asymptomatic with >80% stenosis, as assessed by digital subtraction angiography performed as described by the North American Symptomatic Carotid Endarterectomy Trial [12]. All patients who underwent CAS had at least one coexisting condition on specific clinical criteria that potentially increased the risk posed by CEA, according to SAPPHIRE study [13]. And we had 20 control subjects who had chronic-stage cerebral infarction without severe carotid artery stenosis (mean age 74, 14 men and 6 women).

Carotid artery stenosis was considered symptomatic if the patient had a history of ipsilateral ischemic events attributed to the affected carotid artery within the previous 120 days before CAS and CEA, and asymptomatic if no ischemic event occurred during this period.

This study was approved by the Ethical Committee of Mie University. Written informed consent was obtained from all the patients.

Magnetic Resonance Imaging Assessments

Three days before CAS, magnetic resonance (MR) examinations, including 3D-T1 gradient echo (GRE) carotid plaque imaging, were performed on all patients after diagnostic angiography. No ischemic events, such as transient ischemic attack or stroke, occurred between pre-procedural MR examinations and CAS. MR imaging was performed using a 3.0-T MR imaging system (Achieva Quasar Dual, Philips Medical Systems, Best, The Netherlands).

3D-T1 GRE carotid plaque imaging was performed in the coronal plane with null blood conditions (effective inversion time, 600 ms; TR/TE, 5.0/2.3 ms) and the water excitation technique to suppress fat signals. Other scanning parameters were as follows: FOV, 260 mm; voxel size, 0.68×0.68×1.00 mm; flip angle, 13°; partitions, 56 partitions covering 70 mm around the carotid bifurcation; and data acquisition time, 4 min 2 s.

MR images were reviewed by a neurointerventionalist blinded to the clinical data. Regions of interest were drawn manually on a workstation around the carotid plaque and the adjacent sternocleidomastoid muscle (SCM) with coronal 3D-T1TFE images that detected the largest carotid plaque segment. The signal intensity ratio (SIR) was defined as the signal intensity of the carotid plaque divided by the signal intensity of SCM, being >1.8 for vulnerable plaques and ≤1.8 for stable plaques, as previously described [14].

Procedures

All patients received aspirin (100 mg/day) and clopidogrel sulfate (75 mg/day), ticlopidine hydrochloride (200 mg/day), or cilostazol (200 mg/day) as anti-platelet therapy for at least 2 weeks before CAS. All CAS procedures were performed under local anesthesia via the percutaneous transfemoral route by an experienced neurointerventional team. Systemic blood samples were obtained via the femoral sheath immediately after insertion. A heparin bolus of 100 U/kg was intravenously administered immediately after the introducer sheath was placed to increase the activated clotting time to a minimum of 300 s. Two different types of distal filter embolic protection devices were used: Angioguard XP (Cordis, Minneapolis, MN) and FilterWire EZ (Boston Scientific, Natic, MA). Before advancing the distal filter device, flow arrest was obtained by temporary balloon occlusion using the Optimo balloon guiding catheter (Tokai Medical Products, Aichi, Japan) in the common carotid artery and PercuSurge GuardWire (Medtronic AVE, Santa Rosa, CA) in the external carotid artery. Then, the local stagnant blood near the atherosclerotic plaque area was slowly aspirated from the guiding catheter and collected as the pre-procedural local blood sample. Under distal filter protection, pre-dilatation with an angioplasty balloon was performed as necessary; a self-expandable stent–Precise (Cordis, Minneapolis, MN) or Carotid Wallstent (Boston Scientific, Natic, MA)–was deployed; and post-dilatation was done as necessary. After these procedures, the local stagnant blood was aspirated with temporary balloon occlusion and collected as the post-procedural local sample. When aspiration was complete, the distal filter device was captured and removed.

Blood sampling of control patients were drawn by veinpuncture.

Blood samples were centrifuged at 3000 rpm for 15 min, and the supernatants were separated and stored at −80°C until analysis. Debris captured by the distal embolic protection devices was fixed in 10% paraformaldehyde, placed in gel, embedded in paraffin, and sliced into 2-µm-thick sections.

All patients treated by CEA underwent general anesthesia. Intraluminal shunt insertion was performed immediately after arterectomy before removing the atherosclerotic plaques to provide immediate reperfusion. Before skin closure, all patients underwent angiography in the operating room to confirm patency of the carotid arteries. Atherosclerotic plaque samples collected during CEA were fixed in 10% formalin, embedded in paraffin, and sliced into 5-µm-thick sections.

Measurement of Blood Inflammatory and Anti-inflammatory Markers

The serum levels of the proinflammatory cytokines: IL-1β, IL-6, interferon gamma (IFNγ), tumor necrosis factor alpha (TNFα), and matrix metalloproteinase (MMP)-9; endothelial activation markers: E-selectin, intracellular adhesion molecule 1 (ICAM-1), and vascular cell adhesion molecule 1 (VCAM-1); and anti-inflammatory cytokines: IL-10 and adiponectin, were measured using a multiplex bead array system (Luminex; Millipore, Billerica, MA, USA). Luminex assays were performed using 96-well microplates according to the manufacturer’s protocol.

A commercially available enzyme-linked immunosorbent assay (ELISA) was used to measure the serum levels of inflammatory markers: hs-CRP (CircuLex, Nagano, Japan) and PTX3 (Aviscera Bioscience, Inc., CA, USA).

Histological Analysis

The samples from the CAS-treated patients were histologically examined to characterize the contents of the debris captured by the distal filter device. Filters were gently rinsed with saline and immediately fixed in 10% formaldehyde. Subsequently, the captured debris was extracted from each filter and placed in agarose gel followed by paraffin embedding.

In the patients who underwent CEA, whole specimens were fixed in 10% formalin, sectioned in 3.0-mm transverse slices, decalcified, and embedded in paraffin. The paraffin-embedded specimens were sectioned at 5-µm thickness stained with hematoxylin and eosin (HE), and subjected to histopathological and immunohistochemical analyses.

The sections obtained from the CEA-treated patients were stained with mouse anti-IL-6 antibody (monoclonal, diluted 1∶200, LifeSpan Biosciences, Seattle, WA, USA); rabbit anti-E-selectin antibody (polyclonal, diluted 1∶100, Santa Cruz Biotechnology, Santa Cruz, CA, USA); and rabbit anti-PTX3 antibody (monoclonal, diluted 1∶100, Enzo Life Sciences, Farmingdale, NY, USA). Deparaffinized sections were incubated with 1% (v/v) H2O2 in methanol for 3 min to eliminate endogenous peroxidase activity. After blocking with 10% (v/v) normal serum, the sections were incubated for 1 h at room temperature with the primary antibodies. After three 5-min washes in phosphate-buffered saline, the sections were incubated with biotinylated secondary antibodies for 1 h and then with the avidin-biotinylated horseradish peroxidase complex (ABC Elite kit, Vector, Burlingame, CA, USA) for 30 min. Peroxidase labeling was visualized using 0.2% (v/v) 3,3′-diaminobenzidine as a chromogen. When using the antibodies, the sections were lightly counterstained with hematoxylin. Morphological characteristics of carotid plaque were established on hematoxylin staining according to the previous classification [15]. The quantification of IL-6, PTX3 and E-selectin positive cells was established from immunohistochemical sections. Quantitative evaluation of 10 optical fields was performed at x100 magnification. Results are expressed as the number of cells per 10 fields.

Data Analysis

During CAS, intracarotid blood samples were slightly diluted in normal saline and iodinated contrast medium. Therefore, the level was normalized for albumin to correct for dilution. Data are reported as means ± IQR (interquartile range). The chi-square test and Wilcoxon’s rank test were used to perform intergroup comparisons about patient characteristics. Shapiro Wilk test was used to evaluate normality, and Kruskal Wallis test was used to evaluate continuous variables for data measured by Luminex and ELISA. The Wilcoxon’s rank test was used for pair comparisons of cell counts about histological analysis. Receiver operating curve was constructed to identify the cutoff point of PTX3. The SPSS Statistics 22 software package was used to perform descriptive statistical analyses. P<0.05 was considered statistically significant.

Results

Patient Characteristics

The baseline characteristics of the patients with CAS are summarized in Table 1. Twenty patients showed SIR >1.8 and were classified into the vulnerable plaque group, while 21 had SIR ≤1.8 and were classified into the stable plaque group. All but 1 patient with vulnerable plaques were males. In terms of other demographic profiles, there were no differences between the 2 groups.

[Figure omitted. See PDF.]

Table 1. Patient characteristics.

https://doi.org/10.1371/journal.pone.0100045.t001

Serum Markers of Inflammation and Endothelial Activation

Investigation of serial changes in cytokines, endothelial activation, and inflammatory markers (Figure 1).

Several significant differences were observed in the IL-6, IL-10, E-selectin, VCAM-1, and PTX3 levels between local and systemic samples. Among proinflammatory markers, levels of IL-6 were higher in the post-procedural local samples than those in the systemic samples. The levels of the markers for endothelial activation–E-selectin and VCAM-1–and of the inflammatory marker PTX3 were also increased. For anti-inflammatory markers, IL-10 levels were higher in the post-procedural local samples than in the systemic samples. A comparison of serial changes in IL-6 and IL-10 levels showed significantly higher values in the post-procedural local samples than in the systemic samples. Further, E-selectin, VCAM-1 and PTX3 levels were significantly higher in the pre- and post-procedural local samples than in the systemic samples. No significant differences were observed in the IL-1β, TNFα, IFNγ, MMP-9, ICAM-1, adiponectin, and hs-CRP levels (Figure S1).

[Figure omitted. See PDF.]

Figure 1. Systemic and local levels of proinflammatory and anti- inflammatory markers.

Serum levels of inflammatory markers in systemic, pre-, and post-procedural local samples were measured by ELISA. Results are expressed as mean ± IQRs. Differences between the samples are not significant, except for those indicated by *P<0.05.

https://doi.org/10.1371/journal.pone.0100045.g001

Comparison between stable and vulnerable plaques (Figure 2).

The levels of proinflammatory cytokines–IL-6 and TNFα; endothelial activation marker–E-selectin; and inflammation markers–hs-CRP and PTX3, were upregulated in the vulnerable plaque group as compared to the stable plaque group. In contrast, the levels of the anti-inflammatory cytokines IL-10 and adiponectin were downregulated in the vulnerable plaque group as compared to the stable plaque group. No significant differences were observed in the IFNγ, MMP-9, and ICAM-1 levels (Figure S2).

[Figure omitted. See PDF.]

Figure 2. Comparison of proinflammatory and anti- inflammatory markers for plaque vulnerability.

Serum levels of proinflammatory and anti-inflammatory markers from vulnerable and stable plaques in systemic, pre-, and post-procedural local samples were measured by ELISA. Results are expressed as mean ± IQRs. Differences between the samples are not significant, except for those indicated by *P<0.05.

https://doi.org/10.1371/journal.pone.0100045.g002

IL-6 levels showed significant differences between the vulnerable and stable plaque groups in the post-procedural and pre-procedural local samples, and TNFα levels differed significantly in the post-local samples. E-selectin levels differed significantly between the systemic and post-procedural local samples in the vulnerable plaque group and between the vulnerable and stable plaque groups in the pre- and post-procedural local samples. Serial VCAM-1 levels also differed significantly between the systemic and post-procedural local samples. Significant differences were observed in the hs-CRP levels in the pre-procedural local samples between the vulnerable and stable plaque groups.

Among these markers, the most distinctive changes were observed in PTX3 levels, which were higher in the vulnerable plaque group than in the stable plaque group for systemic, pre-, and post-procedural local samples. Moreover, PTX3 levels differed significantly between the systemic, pre- and post-procedural local samples in the vulnerable plaque group.

The levels of anti-inflammatory markers IL-10 and adiponectin were higher in the stable plaque group than in the vulnerable plaque group. IL-10 levels differed significantly between the systemic and post-procedural local samples in the stable plaque group and between the vulnerable and stable plaque groups in the post-procedural local samples. The level of adiponectin in the stable group was significantly higher than in the vulnerable plaque group.

Comparison between patients with and without severe carotid artery stenosis (Figure 3).

Significant differences were observed in the adiponectin, hs-CRP, and PTX3 levels. PTX3 was upregulated in the vulnerable plaque group as compared to the stable plaque and control group, and hs-CRP was also upregulated in the vulnerable plaque group as compared to the control. For anti-inflammatory markers, the level of adiponectin was downregulated in the vulnerable plaque group as compared to the stable plaque group. No significant differences were observed in the IL-6, IL-1β, IL-10, TNFα, IFNγ, MMP-9, E-selectin, ICAM-1, and VCAM-1 levels (Figure S3).

[Figure omitted. See PDF.]

Figure 3. Comparison of systemic and control samples.

Serum levels of proinflammatory and anti-inflammatory markers in systemic samples of patients with vulnerable and stable plaques, and controls were measured by ELISA. Results are expressed as mean ± IQRs. Differences between the samples are not significant, except for those indicated by *P<0.05.

https://doi.org/10.1371/journal.pone.0100045.g003

Histological Analysis of Captured Debris and CEA Samples (Figure 4)

To investigate the relationship between atherosclerosis and inflammation, we performed HE staining and immunohistochemical analyses. After histological analysis, the CEA plaques were classified as vulnerable (n = 12) or stable (n = 5). Vulnerable plaques from the CEA-treated patients showed hematomas, lipid-rich cores, and inflammatory cell infiltration, and those from CAS-treated patients showed inflammatory cell infiltration. The debris captured from the stable plaque group of CAS-treated patients showed cholesterin crystals.

[Figure omitted. See PDF.]

Figure 4. Immunochemical staining of atherosclerotic carotid endarterectomy specimens and emboli captured by distal protection devices.

Serial sections were stained with hematoxylin and eosin (HE) (A, B, C, Q, R), anti-IL-6 (D, E, F), anti-PTX3 (G, H, I), and anti-E-selectin (J, K, L) antibodies. Sections from CEA (A to L), quantification of immunohistochemistry analysis of IL-6, PTX3, and E-selectin staining of sections from CEA (M, N, O), and embolic debris from CAS captured by the distal filter device (P, Q, R) are shown. HE staining showed inflammatory cell infiltrations in the vulnerable plaques (A, B, Q) and cholesterin crystals in the stable plaques (C, R). IL-6 staining is observed in the vulnerable plaques with inflammatory cell infiltration (D, E) but not in the stable plaques (F). PTX3 expression is observed in endothelial and perivascular cells and in the basement membrane in the vulnerable plaques (G, H) but not in the stable plaques (I). Immunohistochemistry revealed E-selectin expression in endothelial cells in the vulnerable plaques (J, K) but not in the stable plaques (L). The second line on the left of the vulnerable plaques (B, E, H, K) shows enlargement of the cropped areas. Scale bar, 100 µm.

https://doi.org/10.1371/journal.pone.0100045.g004

All plaques from the CEA-treated patients showed IL-6, PTX3 and E-selectin expression. Quantitative analysis of IL-6-, PTX3- and E-selectin-positive cells was investigated. These three markers are more abundant in vulnerable plaques. IL-6 expression with inflammatory cell infiltration was observed in the vulnerable plaque group, while PTX3 expression was observed sporadically in endothelial and perivascular cells and basement membranes in the vulnerable plaque group of CEA-treated patients. E-selectin expression was observed in endothelial cells in the vulnerable plaque group of CEA-treated patients.

Predictor of Vulnerable Plaque (Figure 5)

Figure 5 shows the receiver-operating curves of PTX3 levels for predicting vulnerable plaques. The area under the curve was 0.877 (95% confidence interval: 0.767 to 0.987; P<0.001). A PTX3 cutoff level of 1.55 pg/ml distinguished vulnerable plaques from stable plaques with 94.7% sensitivity and 71.4% specificity, and a PTX3 cutoff level of 1.93 pg/ml distinguished vulnerable plaques with 68.4% sensitivity and 95.2% specificity.

[Figure omitted. See PDF.]

Figure 5. Receiver-operating curve of PTX3 levels for predicting vulnerable plaque.

The area under the curve of PTX3 levels were obtained from all patients.

https://doi.org/10.1371/journal.pone.0100045.g005

Discussion

The present study revealed the following: (1) the vulnerability of carotid atherosclerosis was associated with certain soluble factors involved in inflammation, (2) PTX3 may become a potential new powerful predictor for determining plaque vulnerability, and (3) IL-10 and adiponectin were associated with plaque stability.

MR plaque imaging represents a new modality for risk assessment in atherosclerosis [16]–[18]. High-resolution MR imaging can detect the following characteristics of a vulnerable plaque: a thin or ruptured fibrous cap, a large lipid or necrotic core, and intraplaque hemorrhage [19]. A recent study reported high signal intensity (SIR >1.8) to be associated with cerebral embolism during CAS [14], and we accordingly categorized plaque vulnerability.

Inflammatory mechanisms are known to play a central role in the pathogenesis and progression of atherosclerosis, plaque rupture, thrombosis, and stroke. Inflammatory biomarkers, such as hs-CRP, IL-6, E-selectin, ICAM-1, and VCAM-1, have been previously identified [20]–[23]. IL-6 has been reported to be higher in local samples from patients with carotid artery plaques, increasing further after CAS with periprocedural new ischemic lesions [24]. In present study, serum IL-6, VCAM-1, E-selectin and PTX3 levels were significantly higher in the post-procedural local samples as compared to the systemic samples. This suggests an association between carotid atherosclerosis and the local production of not only IL-6 but also E-selectin, VCAM-1 and PTX3 (Figure 6).

[Figure omitted. See PDF.]

Figure 6. Proinflammatory and anti-inflammatory biomarkers in vulnerable plaques.

Decreased adiponectin levels induce endothelial cell dysfunction with E-selectin release, with subsequent low IL-10 levels and high TNFα levels. Impaired endothelial cells release E-selectin, PTX3, and TNFα. Macrophages produce PTX3, TNFα, and IL-6.

https://doi.org/10.1371/journal.pone.0100045.g006

Plaque vulnerability is considered to be a major factor in stroke and should be accurately determined. The formation of carotid atherosclerotic plaques is a dynamic process in which modified lipids, extracellular matrix, monocyte-derived macrophages, and activated vascular smooth muscle cells accumulate in the arterial wall. In our study, the levels of several serum proinflammatory and anti-inflammatory markers, such as IL-6, IL-10, TNFα, E-selectin, adiponectin, hs-CRP, and PTX3, differed significantly between the vulnerable and stable plaque groups. Most of these markers occurred at higher levels in the vulnerable plaque group as compared to the stable plaque group, while IL-10 and adiponectin levels were decreased in the vulnerable plaque group. Previous reports have shown these markers to be associated with carotid atherosclerosis [24]–[26]. The present study further demonstrated that the upregulation of these proinflammatory markers and the downregulation of IL-10, an anti-inflammatory marker, were associated with plaque vulnerability. In particular, IL-6 expression was associated with inflammatory cell infiltration in the vulnerable plaques.

E-selectin was localized to the endothelial cells and inflammatory cells in the vulnerable plaques in tissue sections, as reported previously [27]. This finding suggested the occurrence of endothelial activation and a close relationship between plaque vulnerability and the production of these proinflammatory markers. In contrast, upregulated IL-10 and adiponectin expression in stable plaques may suggest a relationship between these cytokines and plaque stability. IL-10 is a potent anti-inflammatory cytokine with macrophage deactivating properties [28]. Adiponectin is an insulin-sensitizing protein expressed in adipose tissue that ostensibly plays a protective role in atherosclerosis and cardiovascular disease [29]. Low adiponectin levels have recently been associated with increased carotid intima-media thickness, which is indicative of atherosclerosis, being related to endothelial cell dysfunction and high E-selectin levels in patients with coronary heart diseases, whereas high adiponectin levels decrease the risk and play a protective role in atherosclerosis [30], [31]. Adiponectin induces IL-10 expression in leukocytes, which is correlated with decreasing IL-6 and TNFα levels [32], [33]. IL-10 inhibits macrophage activation; however, its production is decreased by CRP [34], [35]. Our results correspond with previous findings that have demonstrated an inverse association between adiponectin levels and atherosclerosis.

PTX3 has been suggested as a marker of inflammatory activity and plaque instability. Immunohistochemical studies have demonstrated increased PTX3 expression in atherosclerotic plaques as compared with that in non-atherosclerotic arteries [36], [37]. Matsuura et al have shown that PTX3 is more enhanced in vulnerable plaques than stable plaques in coronary artery of patients with angina pectoris and immunoreactivity for PTX3 is intense in the areas with intraplaque hemorrhage [38]. Previously, deficient symptomatology has indicated the absence of any relationship between PTX3 and the carotid artery [39]. In this study, serum PTX3 levels in both systemic and intracarotid samples before and after CAS were higher in the vulnerable group than in the stable group. And also, PTX3 expression was observed in inflammatory cells and in vascular endothelial and perivascular cells of vulnerable plaques. Therefore, our finding that PTX3 is associated with carotid plaque vulnerability is noteworthy. This finding corresponds to a previous report that suggested a potential association between PTX3 and stroke risk [40]. PTX3 is produced mostly in dendritic cells, endothelial cells, smooth muscle cells, macrophages, and fibroblasts [41]. Furthermore PTX3 may reflect the baseline atherosclerotic burden more accurately than CRP particularly under acute stress conditions, such as stroke, because of differences in amino acid sequences and molecular structures [40]. The close correlation observed between serum PTX3 levels and plaque vulnerability in the present study indicates that PTX3 may be a potential predictor of ischemic stroke.

Our present findings support the theory that PTX3 may be a potentially modifiable risk factor for atherosclerosis and that adiponectin may provide potentially substantial clinical benefits in the stabilization of carotid plaques.

Conclusion

Carotid plaque vulnerability was modulated by the upregulation of proinflammatory factors and the downregulation of anti-inflammatory factors. In particular, PTX3 may be a potential novel indicator of plaque vulnerability.

Supporting Information

[Figure omitted. See PDF.]

Figure S1.

Systemic and local levels of proinflammatory and anti- inflammatory markers. Serum levels of inflammatory markers in systemic, pre-, and post-procedural local samples were measured by ELISA. Results are expressed as mean ± IQRs. No significant differences were observed in the IL-1β, TNFα, IFNγ, MMP-9, ICAM-1, adiponectin, and hs-CRP levels.

https://doi.org/10.1371/journal.pone.0100045.s001

(TIF)

Figure S2.

Comparison of proinflammatory and anti- inflammatory markers for plaque vulnerability. Serum levels of proinflammatory and anti-inflammatory markers from vulnerable and stable plaques in systemic, pre-, and post-procedural local samples were measured by ELISA. Results are expressed as mean ± IQRs. No significant differences were observed in the IL-1β, IFNγ, MMP-9, and ICAM-1 levels.

https://doi.org/10.1371/journal.pone.0100045.s002

(TIF)

Figure S3.

Comparison of systemic and control samples. Serum levels of proinflammatory and anti-inflammatory markers in systemic samples of patients with vulnerable and stable plaques, and controls were measured by ELISA. Results are expressed as mean ± IQRs. No significant differences were observed in the IL-6, IL-1β, IL-10, TNFα, IFNγ, MMP-9, E-selectin, ICAM-1, and VCAM-1 levels.

https://doi.org/10.1371/journal.pone.0100045.s003

(TIF)

Acknowledgments

We thank Ms. Manami Negoro and Chiduru Yamamoto for their technical assistance. We are indebted to Ms. Tomomi Yamada for advising statistical analysis.

Author Contributions

Conceived and designed the experiments: AS. Performed the experiments: AS KY TF. Analyzed the data: AS H. Tanemura KY H. Tomimoto. Contributed reagents/materials/analysis tools: H. Tanemura KH MS YU FA NT HS. Wrote the paper: AS H. Tomimoto. Supervisor: WT H. Tomimoto.

Citation: Shindo A, Tanemura H, Yata K, Hamada K, Shibata M, Umeda Y, et al. (2014) Inflammatory Biomarkers in Atherosclerosis: Pentraxin 3 Can Become a Novel Marker of Plaque Vulnerability. PLoS ONE 9(6): e100045. https://doi.org/10.1371/journal.pone.0100045

References

1. Ross R (1999) Atherosclerosis–an inflammatory disease. N Engl J Med 340: 115–126.

2. Falk E, Shah PK, Fuster V (1995) Coronary plaque disruption. Circulation 92: 657–671.

3. Libby P (1995) Molecular bases of the acute coronary syndromes. Circulation 91: 2844–2850.

4. Libby P (2002) Atherosclerosis: the new view. Sci Am 286: 46–55.

5. Moreno PR, Falk E, Palacios IF, Newell JB, Fuster V, et al. (1994) Macrophage infiltration in acute coronary syndromes. Implications for plaque rupture. Circulation 90: 775–778.

6. Davies MJ (1996) Stability and instability: two faces of coronary atherosclerosis. The Paul Dudley White Lecture 1995. Circulation 94: 2013–2020.

7. Davignon J, Ganz P (2004) Role of endothelial dysfunction in atherosclerosis. Circulation 109: III27–32.

8. Harris TB, Ferrucci L, Tracy RP, Corti MC, Wacholder S, et al. (1999) Associations of elevated interleukin-6 and C-reactive protein levels with mortality in the elderly. Am J Med 106: 506–512.

9. Ridker PM, Hennekens CH, Buring JE, Rifai N (2000) C-reactive protein and other markers of inflammation in the prediction of cardiovascular disease in women. N Engl J Med 342: 836–843.

10. Bonacina F, Baragetti A, Catapano AL, Norata GD (2013) Long pentraxin 3: experimental and clinical relevance in cardiovascular diseases. Mediators Inflamm 2013: 725102.

11. Garlanda C, Bottazzi B, Bastone A, Mantovani A (2005) Pentraxins at the crossroads between innate immunity, inflammation, matrix deposition, and female fertility. Annu Rev Immunol 23: 337–366.

12. North American Symptomatic Carotid Endarterectomy Trial Collaborators (1991) Beneficial effect of carotid endarterectomy in symptomatic patients with high-grade carotid stenosis. N Engl J Med 325: 445–453.

13. Yadav JS, Wholey MH, Kuntz RE, Fayard P, Katzen BT, et al. (2004) Protected carotid-artery stenting versus endarterectomy in high-risk patients. N Engl J Med 351: 1493–1501.

14. Tanemura H, Maeda M, Ichikawa N, Miura Y, Umeda Y, et al. (2013) High-risk plaque for carotid artery stenting evaluated with 3-dimensional t1-weighted gradient echo sequence. Stroke 44: 105–110.

15. Stary HC (2000) Natural history and histological classification of atherosclerotic lesions: an update. Arterioscler Thromb Vasc Biol 20: 1177–1178.

16. Crouse JR 3rd (2006) Thematic review series: patient-oriented research. Imaging atherosclerosis: state of the art. J Lipid Res 47: 1677–1699.

17. Yuan C, Oikawa M, Miller Z, Hatsukami T (2008) MRI of carotid atherosclerosis. J Nucl Cardiol 15: 266–275.

18. Saam T, Hatsukami TS, Takaya N, Chu B, Underhill H, et al. (2007) The vulnerable, or high-risk, atherosclerotic plaque: noninvasive MR imaging for characterization and assessment. Radiology 244: 64–77.

19. Cai JM, Hatsukami TS, Ferguson MS, Small R, Polissar NL, et al. (2002) Classification of human carotid atherosclerotic lesions with in vivo multicontrast magnetic resonance imaging. Circulation 106: 1368–1373.

20. Shenhar-Tsarfaty S, Ben Assayag E, Bova I, Shopin L, Fried M, et al. (2010) Interleukin-6 as an early predictor for one-year survival following an ischaemic stroke/transient ischaemic attack. Int J Stroke 5: 16–20.

21. Cao JJ, Thach C, Manolio TA, Psaty BM, Kuller LH, et al. (2003) C-reactive protein, carotid intima-media thickness, and incidence of ischemic stroke in the elderly: the Cardiovascular Health Study. Circulation 108: 166–170.

22. Blann AD, Waite MA (1996) von Willebrand factor and soluble E-selectin in hypertension: influence of treatment and value in predicting the progression of atherosclerosis. Coron Artery Dis 7: 143–147.

23. Wang JY, Zhou DH, Li J, Zhang M, Deng J, et al. (2006) Association of soluble intercellular adhesion molecule 1 with neurological deterioration of ischemic stroke: The Chongqing Stroke Study. Cerebrovasc Dis 21: 67–73.

24. Abe Y, Sakaguchi M, Furukado S, Fujinaka T, Sakoda S, et al. (2010) Interleukin-6 release after carotid artery stenting and periprocedural new ischemic lesions. J Cereb Blood Flow Metab 30: 857–863.

25. Sakurai S, Kitamura A, Cui R, Yamagishi K, Tanigawa T, et al. (2009) Relationships of soluble E-selectin and high-sensitivity C-reactive protein with carotid atherosclerosis in Japanese men. J Atheroscler Thromb 16: 339–345.

26. Profumo E, Esposito C, Buttari B, Tosti ME, Ortona E, et al. (2007) Intracellular expression of cytokines in peripheral blood from patients with atherosclerosis before and after carotid endarterectomy. Atherosclerosis 191: 340–347.

27. O’Brien KD, McDonald TO, Chait A, Allen MD, Alpers CE (1996) Neovascular expression of E-selectin, intercellular adhesion molecule-1, and vascular cell adhesion molecule-1 in human atherosclerosis and their relation to intimal leukocyte content. Circulation 93: 672–682.

28. de Vries JE (1995) Immunosuppressive and anti-inflammatory properties of interleukin 10. Ann Med 27: 537–541.

29. Wozniak SE, Gee LL, Wachtel MS, Frezza EE (2009) Adipose tissue: the new endocrine organ? A review article. Dig Dis Sci 54: 1847–1856.

30. Gardener H, Sjoberg C, Crisby M, Goldberg R, Mendez A, et al. (2012) Adiponectin and carotid intima-media thickness in the northern Manhattan study. Stroke 43: 1123–1125.

31. El-Mesallamy HO, Hamdy NM, Salman TM, Mahmoud S (2011) Adiponectin and E-selectin concentrations in relation to inflammation in obese type 2 diabetic patients with coronary heart disease(s). Minerva Endocrinol 36: 163–170.

32. Kumada M, Kihara S, Ouchi N, Kobayashi H, Okamoto Y, et al. (2004) Adiponectin specifically increased tissue inhibitor of metalloproteinase-1 through interleukin-10 expression in human macrophages. Circulation 109: 2046–2049.

33. Folco EJ, Rocha VZ, López-Ilasaca M, Libby P (2009) Adiponectin inhibits pro-inflammatory signaling in human macrophages independent of interleukin-10. J Biol Chem 284: 25569–25575.

34. O’Farrell AM, Liu Y, Moore KW, Mui AL (1998) IL-10 inhibits macrophage activation and proliferation by distinct signaling mechanisms: evidence for Stat3-dependent and -independent pathways. EMBO J 17: 1006–1018.

35. Singh U, Devaraj S, Dasu MR, Ciobanu D, Reusch J, et al. (2006) C-reactive protein decreases interleukin-10 secretion in activated human monocyte-derived macrophages via inhibition of cyclic AMP production. Arterioscler Thromb Vasc Biol 26: 2469–2475.

36. Rolph MS, Zimmer S, Bottazzi B, Garlanda C, Mantovani A, et al. (2002) Production of the long pentraxin PTX3 in advanced atherosclerotic plaques. Arterioscler Thromb Vasc Biol 22: e10–14.

37. Savchenko A, Imamura M, Ohashi R, Jiang S, Kawasaki T, et al. (2008) Expression of pentraxin 3 (PTX3) in human atherosclerotic lesions. J Pathol 215: 48–55.

38. Matsuura Y, Hatakeyama K, Imamura T, Tsuruda T, Shibata Y, et al. (2012) Different distribution of pentraxin 3and C-reactive protein in coronary atherosclerotic plaques. J Atheroscler Thromb 19: 837–45.

39. Hermus L, Schuitemaker JH, Tio RA, Breek JC, Slart RH, et al. (2011) Novel serum biomarkers in carotid artery stenosis: useful to identify the vulnerable plaque? Clin Biochem 44: 1292–1298.

40. Ryu WS, Kim CK, Kim BJ, Kim C, Lee SH, at el (2012) Pentraxin 3: a novel and independent prognostic marker in ischemic stroke. Atherosclerosis 220: 581–586.

41. Norata GD, Garlanda C, Catapano AL (2010) The long pentraxin PTX3: a modulator of the immunoinflammatory response in atherosclerosis and cardiovascular diseases. Trends Cardiovasc Med 20: 35–40.

Word count: 5271

Show less

© 2014 Shindo et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License: http://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

Inflammation is crucially involved in the development of carotid plaques. We examined the relationship between plaque vulnerability and inflammatory biomarkers using intraoperative blood and tissue specimens. We examined 58 patients with carotid stenosis. Following carotid plaque magnetic resonance imaging, 41 patients underwent carotid artery stenting (CAS) and 17 underwent carotid endarterectomy (CEA). Blood samples were obtained from the femoral artery (systemic) and common carotid artery immediately before and after CAS (local). Seventeen resected CEA tissue samples were embedded in paraffin, and histopathological and immunohistochemical analyses for IL-6, IL-10, E-selectin, adiponectin, and pentraxin 3 (PTX3) were performed. Serum levels of IL-6, IL-1β, IL-10, TNFα, E-selectin, VCAM-1, adiponectin, hs-CRP, and PTX3 were measured by multiplex bead array system and ELISA. CAS-treated patients were classified as stable plaques (n = 21) and vulnerable plaques (n = 20). The vulnerable group showed upregulation of the proinflammatory cytokines (IL-6 and TNFα), endothelial activation markers (E-selectin and VCAM-1), and inflammation markers (hs-CRP and PTX3) and downregulation of the anti-inflammatory markers (adiponectin and IL-10). PTX3 levels in both systemic and intracarotid samples before and after CAS were higher in the vulnerable group than in the stable group. Immunohistochemical analysis demonstrated that IL-6 was localized to inflammatory cells in the vulnerable plaques, and PTX3 was observed in the endothelial and perivascular cells. Our findings reveal that carotid plaque vulnerability is modulated by the upregulation and downregulation of proinflammatory and anti-inflammatory factors, respectively. PTX3 may thus be a potential predictive marker of plaque vulnerability.

Details

Title
Inflammatory Biomarkers in Atherosclerosis: Pentraxin 3 Can Become a Novel Marker of Plaque Vulnerability
Author
Shindo, Akihiro; Tanemura, Hiroshi; Yata, Kenichiro; Hamada, Kazuhide; Shibata, Masunari; Umeda, Yasuyuki; Asakura, Fumio; Toma, Naoki; Sakaida, Hiroshi; Fujisawa, Takao; Taki, Waro; Tomimoto, Hidekazu
First page
e100045
Section
Research Article
Publication year
2014
Publication date
Jun 2014
Publisher
Public Library of Science
e-ISSN
19326203
Source type
Scholarly Journal
Language of publication
English
DOI
https://doi.org/10.1371/journal.pone.0100045
ProQuest document ID
1984969538
Copyright
© 2014 Shindo et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License: http://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.