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机制性和选择性限制作用于B细胞库中VλJλ连接的建立。

Mechanistic and selective constraints act on the establishment of V lambda J lambda junctions in the B cell repertoire.

作者信息

Boudinot P, Drapier A M, Cazenave P A, Sanchez P

机构信息

Département d'Immunologie, Institut Pasteur UA CNRS 359, Paris, France.

出版信息

J Immunol. 1994 Mar 1;152(5):2248-55.

PMID:8133038
Abstract

Only four different subtypes of lambda Ig chains have been described in the mouse: lambda 1, lambda 2(V2), lambda 2(Vx), and lambda 3. These chains are encoded by gene segments all sequenced and well localized in chromosome 16. Although the lambda Ig system is both simple and well characterized, no exhaustive analysis has been done concerning V lambda J lambda junctions in nonintentionally stimulated B cells. To get an insight into the lambda B cell repertoire, we analyzed a large number of V lambda J lambda rearrangements isolated from spleen mRNA or genomic DNA of unimmunized adult BALB/c mice. By PCR amplification, more than 160 clones were obtained covering all V lambda J lambda recombinations. Simple recombinations of trimmed gene segments explain most sequences. Certain junctions have been found to be prevalent in each subtype, and an analysis of V lambda J lambda recombination sites shows that the splenic lambda repertoire can result from both differential efficiencies of rearrangement and selective processes.

摘要

在小鼠中仅描述了四种不同亚型的λ免疫球蛋白链:λ1、λ2(V2)、λ2(Vx)和λ3。这些链由已全部测序且定位在16号染色体上的基因片段编码。尽管λ免疫球蛋白系统既简单又特征明确,但尚未对非故意刺激的B细胞中的VλJλ连接进行详尽分析。为深入了解λB细胞库,我们分析了从未免疫的成年BALB/c小鼠脾脏mRNA或基因组DNA中分离出的大量VλJλ重排。通过PCR扩增,获得了160多个克隆,涵盖了所有VλJλ重组。经修剪的基因片段的简单重组解释了大多数序列。已发现某些连接在每个亚型中都很普遍,对VλJλ重组位点的分析表明,脾脏λ库可能源于重排效率差异和选择过程。

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