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Common patterns of B cell perturbation and expanded V4-34 immunoglobulin gene usage in autoimmunity and infection.

机译:在自身免疫和感染中B细胞摄动和扩大的V4-34免疫球蛋白基因使用的常见模式。

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Features of the lymphocyte population in systemic lupus erythematosus (SLE) include a disordered B cell profile and production of autoantibodies. An additional distinctive perturbation is the overexpression of V4-34-encoded serum immunoglobulins (Ig). A similar rise in V4-34-encoded Ig occurs in normal subjects following infection with certain herpesviruses, and is found in Epstein-Barr virus (EBV)-associated infectious mononucleosis (IM). To assess common and distinctive features of B cells in patients with SLE and IM, we compared the B cell profile and V4-34 gene involvement in patients with SLE and IM. B cell profiles from patients with IM paralleled those of patients with SLE, showing a differential loss of naive and memory B cells and the maintenance of plasmablast/early plasma cells. Class-switched V4-34-encoded IgG from plasmablast/early plasma cells was evident both in patients with SLE and IM and revealed common features of oligoclonal expansions with most having undergone somatic hypermutation. It has been proposed that, in healthy individuals, expression of the V4-34 gene is specifically censored prior to isotype switch as a control on autoreactivity. If so, censoring is bypassed following EBV infection, after which equilibrium is restored. Continuing high serum levels in SLE may arise either by disordered regulation, or by subclinical reactivation of endogenous virus.
机译:系统性红斑狼疮(SLE)中淋巴细胞群的特征包括B细胞谱紊乱和自身抗体产生。另一个独特的扰动是V4-34编码的血清免疫球蛋白(Ig)的过表达。 V4-34编码的Ig的类似升高在某些疱疹病毒感染后的正常受试者中发生,并且在与爱泼斯坦-巴尔病毒(EBV)相关的传染性单核细胞增多症(IM)中发现。为了评估SLE和IM患者B细胞的共同和独特特征,我们比较了SLE和IM患者B细胞谱和V4-34基因受累。 IM患者的B细胞谱与SLE患者的B细胞谱相似,显示幼稚B细胞和记忆B细胞的差异丢失以及成浆细胞/早期浆细胞的维持。在SLE和IM患者中,浆母细胞/早期浆细胞的类转换V4-34编码IgG均很明显,并且揭示了寡克隆扩增的共同特征,其中大多数经历了体细胞超突变。已经提出,在健康个体中,在同种型转换之前特异性检查V4-34基因的表达作为自身反应性的对照。如果是这样,则在EBV感染后绕过检查,然后恢复平衡。 SLE的血清水平持续升高可能是由于调节紊乱或内源性病毒的亚临床激活引起的。

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