首页> 外文OA文献 >Rearrangement and expression of T-cell antigen receptor genes in human T-lymphocyte tumor lines and normal human T-cell clones: evidence for allelic exclusion of Ti beta gene expression and preferential use of a J beta 2 gene segment.
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Rearrangement and expression of T-cell antigen receptor genes in human T-lymphocyte tumor lines and normal human T-cell clones: evidence for allelic exclusion of Ti beta gene expression and preferential use of a J beta 2 gene segment.

机译:人T淋巴细胞肿瘤系和正常人T细胞克隆中T细胞抗原受体基因的重排和表达:等位基因排除Ti beta基因表达并优先使用J beta 2基因区段的证据。

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摘要

The gene encoding the beta chain of the human T-cell receptor for antigen is composed of variable (V), diversity (D), joining (J), and constant (C) gene segments which undergo specific rearrangements during T-lymphocyte ontogeny. Southern blot analyses of seven human T-cell tumor lines and normal human T-lymphocyte clones revealed that most of these T-cell lines rearrange their Ti beta genes differently. The T-cell tumor line HPB-MLT rearranges and transcribes both of its Ti beta genes. Cloning and sequencing of the Ti beta cDNAs corresponding to these rearrangements revealed that one of the rearranged Ti beta genes is defective, while the other is functional and corresponds to the Ti beta protein expressed on the surface of these cells. Thus, this cell line displays a pattern of allelic exclusion of Ti beta gene expression. A comparison of four C beta 2-containing Ti beta cDNAs from three different cell lines revealed that three of the four utilize the same J beta 2.5 gene segment joined to different D beta and V beta genes, suggesting that there may be preferential use of this J gene during J beta 2 rearrangements. Hybridization analyses with probes for the alpha and beta genes of the T-cell receptor and the T-cell-specific T gamma gene revealed that HPB-MLT cells appear to express approximately equivalent amounts of RNA corresponding to each of the rearranged Ti alpha and Ti beta genes. However, they express a much lower level of T gamma RNA.
机译:编码人类T细胞抗原抗原的β链的基因由可变(V),多样性(D),连接(J)和恒定(C)基因片段组成,这些片段在T淋巴细胞发生期间会发生特定的重排。对七个人T细胞肿瘤细胞系和正常人T淋巴细胞克隆的Southern印迹分析表明,大多数这些T细胞系以不同的方式重新排列其Tiβ基因。 T细胞肿瘤系HPB-MLT重排和转录了两个Tiβ基因。与这些重排相对应的Ti beta cDNA的克隆和测序表明,重排的Ti beta基因之一是有缺陷的,而另一个具有功能并与这些细胞表面表达的Ti beta蛋白相对应。因此,该细胞系显示出Tiβ基因表达的等位基因排斥的模式。比较来自三个不同细胞系的四个含C beta 2的Ti beta cDNA,发现四个中的三个利用连接到不同D beta和V beta基因的相同J beta 2.5基因片段,这表明可能优先使用J beta 2重排过程中的J基因。用探针对T细胞受体的α和β基因以及T细胞特异性Tγ基因进行的杂交分析表明,HPB-MLT细胞似乎表达约等量的RNA,分别对应于重排的Tiα和Ti β基因。但是,它们表达的TγRNA水平要低得多。

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