首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Organization and sequences of the diversity joining and constant region genes of the human T-cell receptor beta chain.
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Organization and sequences of the diversity joining and constant region genes of the human T-cell receptor beta chain.

机译:人T细胞受体β链的多样性连接和恒定区基因的组织和序列。

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摘要

The organization and sequences of the human beta-chain T-cell receptor diversity, joining, and constant region segments are described. The beta chain of the human T-cell receptor, analogous to the mouse counterpart, consists of two distinct constant region genes approximately equal to 10 kilobases apart. The two constant region genes, C beta 1 and C beta 2, are very similar not only in sequence but also in genomic organization. The coding sequences of each of these C beta constant region genes are divided into four exons. The first two exons encode most of the extracellular constant domain. The third exon encodes a major part of the presumed transmembrane portion, and the last exon contains the cytoplasmic coding sequence as well as 3' untranslated sequences. Except for a stretch of approximately equal to 95 highly conserved nucleotides extending 3' of the first exon of the C region genes, little homology can be found between the intron sequences of C beta 1 and C beta 2. A small cluster of joining region (J beta) gene segments is located approximately equal to 5 kilobases upstream of each of these two constant regions. The first cluster, J beta 1, contains six functional J gene segments while the second, J beta 2, contains seven functional J gene segments. In addition, diversity region (D beta) gene segments are located approximately equal to 600 base pairs upstream of each J beta. Recombinational signals containing highly conserved heptamer and nonamer sequences separated by 12 or 23 bases are found adjacent to all of these D beta and J beta gene segments. These signal sequences are thought to be involved in the somatic recombination processes. These results indicate that what appears to be a gene duplication event giving rise to these two distinct regions must have arisen a long time ago in the evolution of this gene locus.
机译:描述了人类β链T细胞受体多样性,连接和恒定区区段的组织和序列。人类T细胞受体的β链类似于小鼠对应物,由两个不同的恒定区基因组成,它们之间的距离大约等于10千个碱基。两个恒定区基因C beta 1和C beta 2不仅在序列上而且在基因组组织上都非常相似。这些Cβ恒定区基因每个的编码序列分为四个外显子。前两个外显子编码大多数细胞外恒定结构域。第三个外显子编码假定的跨膜部分的主要部分,而最后一个外显子包含细胞质编码序列以及3'非翻译序列。除了延伸约等于C区基因第一个外显子3'的95个高度保守的核苷酸外,C beta 1和C beta 2的内含子序列之间几乎没有同源性。 Jβ)基因区段的位置大约等于这两个恒定区各自上游的5个碱基。第一个簇J beta 1包含六个功能性J基因片段,第二个簇J beta 2包含七个功能性J基因片段。此外,多样性区域(D beta)基因片段的位置大约等于每个J beta上游的600个碱基对。发现与所有这些D beta和J beta基因区段相邻的包含高度保守的七聚体和九聚体序列的重组信号(由12或23个碱基分隔)。这些信号序列被认为与体细胞重组过程有关。这些结果表明,引起这两个不同区域的似乎是基因复制事件必须早已在该基因基因座的进化中发生。

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