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由网状内皮增生症病毒转化的淋巴样细胞中免疫球蛋白轻链基因的重排与多样化

Rearrangement and diversification of immunoglobulin light-chain genes in lymphoid cells transformed by reticuloendotheliosis virus.

作者信息

Zhang J Y, Bargmann W, Bose H R

机构信息

Department of Microbiology, University of Texas, Austin 78712.

出版信息

Mol Cell Biol. 1989 Nov;9(11):4970-6. doi: 10.1128/mcb.9.11.4970-4976.1989.

Abstract

Avian lymphoid cells transformed by reticuloendotheliosis virus (REV-T) serve as a model to analyze the mechanism by which B-cell differentiation and antibody diversification occur in birds. Immunoglobulin light-chain gene rearrangements, diversification, and expression were analyzed in 72 independently derived REV-T-transformed cell lines. Lymphoid cells transformed as the result of expression of the v-rel oncogene were divided into two distinct groups based on light-chain gene rearrangements. The status of the light-chain gene loci in these REV-T-transformed cell lines was determined in part by the ages of the chickens whose spleen cells were transformed. In embryonic spleen cell lines transformed by the v-rel oncogene, rearrangements were not detected, even after prolonged culture in vitro, indicating that these cells are arrested in B-cell differentiation. REV-T transformants derived from spleens obtained from chickens 2 weeks old or older, however, had at least one light-chain allele rearranged. All of the cell lines analyzed which exhibited rearranged light-chain genes contained light-chain transcripts, and most of the REV-T-transformed cells which displayed light-chain rearrangements expressed immunoglobulin protein. REV-T, therefore, transforms B-lymphoid cells at phenotypically different stages of development. Many REV-T-transformed cells undergo immunoglobulin chain gene rearrangements during prolonged propagation in vitro. Most of the cell lines which rearrange their light-chain alleles also undergo diversification during cultivation in vitro. Light-chain diversification occurs during or after the rearrangement event.

摘要

由网状内皮增生症病毒(REV-T)转化的禽类淋巴细胞可作为一个模型,用于分析鸟类B细胞分化和抗体多样化发生的机制。对72个独立衍生的REV-T转化细胞系进行了免疫球蛋白轻链基因重排、多样化及表达分析。因v-rel癌基因表达而转化的淋巴细胞根据轻链基因重排被分为两个不同的组。这些REV-T转化细胞系中轻链基因位点的状态部分取决于其脾细胞被转化的鸡的年龄。在由v-rel癌基因转化的胚胎脾细胞系中,即使在体外长时间培养后也未检测到重排,这表明这些细胞在B细胞分化过程中停滞。然而,来自2周龄及以上鸡脾脏的REV-T转化子至少有一个轻链等位基因发生了重排。所有分析的显示轻链基因重排的细胞系都含有轻链转录本,并且大多数显示轻链重排的REV-T转化细胞表达免疫球蛋白蛋白。因此,REV-T在表型不同的发育阶段转化B淋巴细胞。许多REV-T转化细胞在体外长时间传代培养过程中经历免疫球蛋白链基因重排。大多数重排其轻链等位基因的细胞系在体外培养过程中也会发生多样化。轻链多样化发生在重排事件期间或之后。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1a8a/363648/3fd70668dd8b/molcellb00059-0395-a.jpg

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