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逆转录病毒诱导的小鼠艾滋病中抗体库的异常选择。

Abnormal selection of antibody repertoires in retrovirus-induced murine AIDS.

作者信息

Portnoï D, Viale A C, Colle J H

机构信息

Laboratory of Immunobiology, CNRS URA 359, Institut Pasteur, Paris, France.

出版信息

J Immunol. 1993 Nov 1;151(9):5073-80.

PMID:8409457
Abstract

The mature B cell repertoire in the course of murine AIDS (MAIDS) was investigated. The polymerase chain reaction (PCR) was used to amplify a large diversity of rearranged Ig H chain genes in normal or infected mice, 2 and 8 wk after virus inoculation. Libraries were constructed from the polymerase chain reaction products. By sequencing V-D-J clones in these libraries and analyzing the respective complementary determining region 3 (CDR3), we have shown at 8 wk the emergence of a population of B cells with significantly less N diversity, some sequences lacking any N addition, a typical feature of fetal repertoires known for degeneracy, and autoreactivities. This decreased N diversity was not present 2 wk after inoculation and could not be related to a defect in terminal deoxytransferase expression because the steady-state levels of terminal deoxytransferase mRNA were found normal in MAIDS bone marrow 8 wk after inoculation. FACS analyses revealed a decreased number of bone marrow B cells (B220+, sIgM+) in MAIDS already present at 2 wk, suggesting an alteration in the pathway of B cell differentiation and resulting in a decrease of peripheral B cells renewal. A relative enrichment of spleen cells in long lived B cells as a consequence of this blockade may participate in the abnormal antibody repertoire selection occurring in MAIDS. These data suggest in the MAIDS pathogeny the relationship between an abnormal repertoire selection and the pathologic process.

摘要

我们研究了鼠类获得性免疫缺陷综合征(MAIDS)病程中成熟B细胞库的情况。在病毒接种后2周和8周,使用聚合酶链反应(PCR)扩增正常或感染小鼠中大量重排的Ig H链基因。从聚合酶链反应产物构建文库。通过对这些文库中的V-D-J克隆进行测序并分析各自的互补决定区3(CDR3),我们发现在8周时出现了一群B细胞,其N多样性显著降低,一些序列没有任何N添加,这是已知的胎儿库以简并性为特征的典型特征,并且存在自身反应性。接种后2周不存在这种N多样性降低的情况,并且这与末端脱氧转移酶表达缺陷无关,因为在接种后8周的MAIDS骨髓中发现末端脱氧转移酶mRNA的稳态水平正常。流式细胞术分析显示,MAIDS中骨髓B细胞(B220 +,sIgM +)数量在2周时就已减少,这表明B细胞分化途径发生改变,导致外周B细胞更新减少。由于这种阻断,长寿命B细胞中脾细胞的相对富集可能参与了MAIDS中发生的异常抗体库选择过程。这些数据表明在MAIDS发病机制中,异常库选择与病理过程之间存在关联。

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