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人类VλVIII种系基因的分子特征分析

Molecular characterization of a human V lambda VIII germline gene.

作者信息

Ch'ang L Y, Schell M, Ringelberg C, Weiss D T, Solomon A

机构信息

Department of Medicine, University of Tennessee Medical Center/Graduate School of Medicine, Knoxville 37920.

出版信息

Mol Immunol. 1995 Jan;32(1):49-55. doi: 10.1016/0161-5890(94)00135-n.

Abstract

Human lambda light chains of the recently recognized variable region (VL) subgroup V lambda VIII can be distinguished from proteins of other V lambda gene families on the basis of distinctive chemical and serologic properties and by their preferential association with certain types of autoantibodies, i.e. rheumatoid factors (RFs). We now report that we have cloned from a human placental library a V lambda VIII-encoding germline gene, designated IGLV8A1, using as a molecular probe a partial V lambda VIII fragment generated by polymerase chain reaction (PCR) from genomic DNA. IGLV8A1 contained all the requisite elements of a potentially functional gene, including a V lambda exon with an open reading frame encoding 103 residues. Its expressed products were identified through analyses of cDNA cloned from two different monoclonal lambda VIII B-cell populations. The primary structure of lambda VIII light chains differed from that of lambda I, lambda II, lambda III, lambda IV and lambda VI proteins by the presence of distinctive residues within the first framework region (FR1) and an 11- rather than 7-residue second complementarity-determining region (CDR2). Remarkably, the IGLV8A1 gene was more homologous to the two functional rabbit V lambda germline genes, RV lambda 2 and RV lambda 3 (including the presence of one extra codon within the leader sequence), and to the murine V lambda x gene. Light chains encoded by the human, rabbit and mouse lambda VIII-related genes shared certain unique primary structural features, notably the four additional CDR2 residues. The evolutionary conserved nature of the human V lambda gene and, in particular, the apparently novel tertiary structural effects induced by an elongated CDR2 provide evidence for the biological and functional importance of the V lambda VIII subgroup.

摘要

最近发现的可变区(VL)亚组VλVIII的人λ轻链,可根据其独特的化学和血清学特性,以及它们与某些自身抗体(即类风湿因子,RFs)的优先结合,与其他Vλ基因家族的蛋白质区分开来。我们现在报告,我们从人胎盘文库中克隆了一个编码VλVIII的种系基因,命名为IGLV8A1,使用的分子探针是通过聚合酶链反应(PCR)从基因组DNA产生的部分VλVIII片段。IGLV8A1包含一个潜在功能基因的所有必要元件,包括一个带有编码103个残基的开放阅读框的Vλ外显子。通过对从两个不同的单克隆λVIII B细胞群体克隆的cDNA进行分析,鉴定了其表达产物。λVIII轻链的一级结构与λI、λII、λIII、λIV和λVI蛋白的一级结构不同,其在第一个构架区(FR1)内存在独特的残基,并且第二个互补决定区(CDR2)有11个而非7个残基。值得注意的是,IGLV8A1基因与两个功能性兔Vλ种系基因RVλ2和RVλ3(包括前导序列中有一个额外的密码子)以及小鼠Vλx基因更同源。由人、兔和小鼠λVIII相关基因编码的轻链具有某些独特的一级结构特征,特别是四个额外的CDR2残基。人Vλ基因的进化保守性质,特别是由延长的CDR2诱导的明显新颖的三级结构效应,为VλVIII亚组的生物学和功能重要性提供了证据。

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