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体内 VL 靶向微生物超抗原诱导 B 细胞库的全局变化。

In vivo VL-targeted microbial superantigen induced global shifts in the B cell repertoire.

机构信息

Department of Medicine, New York University School of Medicine, New York, NY, USA.

出版信息

J Immunol. 2012 Jul 15;189(2):850-9. doi: 10.4049/jimmunol.1200245. Epub 2012 Jun 13.

Abstract

To subvert host defenses, some microbial pathogens produce proteins that interact with conserved motifs in V regions of B cell Ag receptor shared by large sets of lymphocytes, which define the properties of a superantigen. Because the clonal composition of the lymphocyte pool is a major determinant of immune responsiveness, this study was undertaken to examine the in vivo effect on the host immune system of exposure to a B cell superantigen, protein L (PpL), a product of the common commensal bacterial species, Finegoldia magna, which is one of the most common pathogenic species among Gram-positive anaerobic cocci. Libraries of Vκ L chain transcripts were generated from the spleens of control and PpL-exposed mice, and the expressed Vκ rearrangements were characterized by high-throughput sequencing. A total of 120,855 sequencing reads could be assigned to a germline Vκ gene, with all 20 known Vκ subgroups represented. In control mice, we found a recurrent and consistent hierarchy of Vκ gene usage, as well as patterns of preferential Vκ-Jκ pairing. PpL exposure induced significant targeted global shifts in repertoire with reduction of Vκ that contain the superantigen binding motif in all exposed mice. We found significant targeted reductions in the expression of clonotypes encoded by 14 specific Vκ genes with the predicted PpL binding motif. These rigorous surveys document the capacity of a microbial protein to modulate the composition of the expressed lymphocyte repertoire, which also has broad potential implications for host-microbiome and host-pathogen relationships.

摘要

为了颠覆宿主防御,一些微生物病原体产生的蛋白质与大量淋巴细胞共同 B 细胞 Ag 受体的 V 区中的保守基序相互作用,这些基序定义了超抗原的特性。由于淋巴细胞库的克隆组成是免疫反应性的主要决定因素,因此进行了这项研究,以检查暴露于 B 细胞超抗原蛋白 L(PpL)对宿主免疫系统的体内影响,PpL 是常见共生细菌物种丰金黄杆菌的产物,是革兰阳性厌氧球菌中最常见的致病物种之一。从对照和 PpL 暴露的小鼠脾脏中生成了 Vκ L 链转录本文库,并通过高通量测序对表达的 Vκ 重排进行了表征。总共可以将 120855 个测序读段分配给一个胚系 Vκ 基因,所有 20 个已知的 Vκ 亚群都有代表。在对照小鼠中,我们发现了 Vκ 基因使用的反复出现且一致的层次结构,以及 Vκ-Jκ 配对的偏好模式。PpL 暴露诱导了 repertoire 的显著靶向全局变化,所有暴露的小鼠中都降低了含有超抗原结合基序的 Vκ。我们发现,编码 14 个具有预测 PpL 结合基序的特定 Vκ 基因的克隆型的表达显著靶向减少。这些严格的调查记录了微生物蛋白调节表达的淋巴细胞库组成的能力,这也对宿主-微生物群和宿主-病原体关系具有广泛的潜在影响。

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