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免疫球蛋白的分子遗传学

Molecular genetics of immunoglobulins.

作者信息

Taussig M J

机构信息

Department of Immunology, AFRC Institute of Animal Physiology and Genetics Research, Babraham, Cambridge, U.K.

出版信息

Immunol Suppl. 1988;1:7-15.

PMID:3133312
Abstract

At the protein level, antibodies show several types of variability. One is the diversity of the variable (V) regions of heavy (H) and light (L) chains, leading to antibody-combining site specificity; another is the existence of two types of light chain (kappa and lambda); a third is the diversity of heavy chain-constant (CH) regions associated with different effector functions. At the DNA level, V-region variability is coded partly through the large number of VL- and VH-region genes and partly generated by integrating complete V genes from combinations of shorter segments (VL-JL for the light chain, VH-D-JH for the heavy chains), together with somatic mutational events (Tonegawa, 1983). kappa, lambda and H chains are coded independently on different chromosomes and have their own V- and C-region genes (Honjo, 1983). CH-region diversity results from a set of CH genes corresponding to the different Ig subclasses. During B-cell development, rearrangement of DNA occurs both in the VL/VH- and CH-region genes. V-region rearrangements take place at the pre-B-cell stage and produce the complete V-region genes for the heavy and light chains which will permanently characterize an individual clone; CH-region rearrangements enable mature B cells to secrete their V regions on different Ig classes (class switching). This article will review the structure and organization of V and C genes and the control of their expression.

摘要

在蛋白质水平上,抗体表现出几种类型的变异性。一种是重链(H)和轻链(L)可变(V)区的多样性,导致抗体结合位点的特异性;另一种是存在两种类型的轻链(κ链和λ链);第三种是与不同效应功能相关的重链恒定(CH)区的多样性。在DNA水平上,V区变异性部分通过大量的VL和VH区基因编码,部分通过将较短片段组合(轻链为VL-JL,重链为VH-D-JH)中的完整V基因整合,以及体细胞突变事件产生(利根川进,1983年)。κ链、λ链和H链在不同染色体上独立编码,并有各自的V区和C区基因(本庶佑,1983年)。CH区多样性源于一组对应于不同Ig亚类的CH基因。在B细胞发育过程中,VL/VH区和CH区基因都会发生DNA重排。V区重排在前B细胞阶段发生,产生重链和轻链的完整V区基因,这些基因将永久表征单个克隆;CH区重排使成熟B细胞能够分泌不同Ig类别的V区(类别转换)。本文将综述V基因和C基因的结构与组织及其表达调控。

相似文献

1
Molecular genetics of immunoglobulins.免疫球蛋白的分子遗传学
Immunol Suppl. 1988;1:7-15.
2
[Genetic bases of antibody diversity].[抗体多样性的遗传基础]
Genetika. 1984 Sep;20(9):1397-413.
3
Unusual immunoglobulin DNA sequences from the nonexpressed chromosome of mouse normal B lymphocytes: implications for allelic exclusion and the DNA rearrangement process.来自小鼠正常B淋巴细胞非表达染色体的异常免疫球蛋白DNA序列:对等位基因排斥和DNA重排过程的影响。
J Immunol. 1987 Sep 1;139(5):1718-26.
4
Recombination between immunoglobulin variable region gene segments is enhanced by transcription.免疫球蛋白可变区基因片段之间的重组通过转录得到增强。
Nature. 1986;324(6097):585-9. doi: 10.1038/324585a0.
5
Restricted Ig variable region gene expression among Ly-1+ B cell lymphomas.Ly-1+ B细胞淋巴瘤中免疫球蛋白可变区基因表达受限。
J Immunol. 1988 Oct 15;141(8):2788-96.
6
DNA rearrangements of immunoglobulin genes correlate with phenotypic markers in B-cell malignancies.免疫球蛋白基因的DNA重排与B细胞恶性肿瘤中的表型标志物相关。
Mol Biol Med. 1984 Feb;2(1):63-79.
7
Recombination between an expressed immunoglobulin heavy-chain gene and a germline variable gene segment in a Ly 1+ B-cell lymphoma.在一个Ly 1+ B细胞淋巴瘤中,一个表达的免疫球蛋白重链基因与一个种系可变基因片段之间的重组。
Nature. 1986;322(6082):843-6. doi: 10.1038/322843a0.
8
Limited junctional diversity in kappa light chains. Junctional sequences from CD43+B220+ early B cell progenitors resemble those from peripheral B cells.κ轻链的连接多样性有限。CD43+B220+早期B细胞祖细胞的连接序列与外周B细胞的相似。
J Immunol. 1994 Apr 1;152(7):3467-75.
9
Ig heavy chain protein controls B cell development by regulating germ-line transcription and retargeting V(D)J recombination.免疫球蛋白重链蛋白通过调节种系转录和重新靶向V(D)J重组来控制B细胞发育。
J Immunol. 1994 Aug 15;153(4):1645-57.
10
Differential usage of VH gene segments is mediated by cis elements.VH基因片段的差异使用由顺式元件介导。
J Immunol. 1998 Oct 1;161(7):3444-54.

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