Pathogenesis and Control of Chronic Infections, University of Montpellier, INSERM, EFS, CHU Montpellier, Montpellier, France.
CHU Montpellier, Department of Rheumatology, Montpellier, France.
Front Immunol. 2019 May 29;10:1153. doi: 10.3389/fimmu.2019.01153. eCollection 2019.
Primary Sjögren's syndrome (pSS) is characterized by B cell hyperactivation, production of autoantibodies and increased risk of B cell lymphomas. Serological profile of Epstein-Barr virus (EBV) reactivation and increase EBV DNA levels in exocrine glands are observed in pSS, but whether these abnormalities are accompanied with disturbed systemic EBV control or have any association with pSS activity remains to be investigated. In this observational study, we initially explored anti-EBV antibodies and cell-free DNA in 395 samples from a cross-sectional plasma collection of pSS patients included in ASSESS French national cohort. Results were assessed in relation with disease activity. Further, to assess cell-associated EBV DNA we organized a case-control study including 20 blood samples from pSS patients followed in University Hospital Center of Montpellier. Results were compared with matched controls. Robust response against EBV early antigen (EA) was observed in pSS patients with anti-SSA/B (Sjögren's syndrome A and B) and anti-SSA autoantibodies compared to anti-SSA/B negatives ( < 0.01 and = 0.01, respectively). Increased beta-2 microglobulin, kappa and lambda light chains, and immunoglobulin G levels were more frequently observed in anti-EA seropositive pSS subjects compared to anti-EA negative subjects ( < 0.001; = 0.001; = 0.003, respectively). Beta-2 microglobulin was independently associated with anti-EA positivity in multivariate analysis ( < 0.001). Plasma cell-free EBV DNA and EBV cellular reservoir was not different between pSS patients and controls. We conclude that serological evidence of EBV reactivation was more frequently observed and more strongly associated with anti-SSA/B status and B cell activation markers in pSS. However, serological profile of EBV reactivation was not accompanied by molecular evidence of systemic EBV reactivation. Our data indicated that EBV infection remains efficiently controlled in the blood of pSS patients.
原发性干燥综合征(pSS)的特征是 B 细胞过度激活、自身抗体产生和 B 细胞淋巴瘤风险增加。在 pSS 中观察到 EBV 再激活的血清学特征和外分泌腺中 EBV DNA 水平升高,但这些异常是否伴有系统 EBV 控制的紊乱或与 pSS 活动有任何关联仍有待研究。在这项观察性研究中,我们最初在 ASSESS 法国国家队列的 pSS 患者的横断面血浆采集的 395 个样本中探索了 EBV 抗体和无细胞游离 DNA。结果与疾病活动相关进行评估。此外,为了评估细胞相关 EBV DNA,我们组织了一项包括来自蒙彼利埃大学医院中心的 20 例 pSS 患者的病例对照研究。结果与匹配的对照进行比较。与抗-SSA/B(干燥综合征 A 和 B)和抗-SSA 自身抗体阴性的 pSS 患者相比,具有抗-SSA/B 自身抗体的 pSS 患者中观察到针对 EBV 早期抗原(EA)的强反应(<0.01 和 =0.01)。与抗-EA 阴性患者相比,抗-EA 阳性的 pSS 患者中更频繁地观察到升高的β-2 微球蛋白、kappa 和 lambda 轻链以及免疫球蛋白 G 水平(<0.001;=0.001;=0.003)。在多变量分析中,β-2 微球蛋白与抗-EA 阳性独立相关(<0.001)。pSS 患者和对照组之间的血浆无细胞 EBV DNA 和 EBV 细胞库无差异。我们得出结论,在 pSS 中,EBV 再激活的血清学证据更频繁地观察到,并且与抗-SSA/B 状态和 B 细胞激活标志物的相关性更强。然而,EBV 再激活的血清学特征并不伴有系统 EBV 再激活的分子证据。我们的数据表明,EBV 感染在 pSS 患者的血液中仍得到有效控制。
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