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编码人κ型免疫球蛋白可变区的基因座的一大段发生了重复。

A large section of the gene locus encoding human immunoglobulin variable regions of the kappa type is duplicated.

作者信息

Pech M, Smola H, Pohlenz H D, Straubinger B, Gerl R, Zachau H G

出版信息

J Mol Biol. 1985 Jun 5;183(3):291-9. doi: 10.1016/0022-2836(85)90001-4.

Abstract

The structure of a new segment of the gene locus encoding the variable regions of human immunoglobulins of the Kappa type (VK) has been elucidated. This segment (cluster B) encompasses six VK sequences, which belong to three different subgroups and which are arranged in the same transcriptional orientation. Part of cluster B was found to be very similar to another region of the VK gene locus, which was cloned previously (cluster A). Sequence differences between the homologous region of clusters A and B range from 0.2% to 3.7% depending on the position of the VK sequences. The divergence is in the same range for genes and pseudogenes. Hybridization experiments with DNAs from different individuals clearly demonstrate that the two segments are located at different positions within the VK locus and do not represent allelic variants. The sequence homology between clusters A and B is higher than the homology of both clusters to an allelic variant, which is represented by a DNA segment that had been isolated from another individual. These results, together with a report in the literature of two other homologous regions in the VK locus, make it very likely that a major part of even the whole locus is duplicated. In this case, VK gene numbers would be higher than previously estimated on the basis of hybridization studies. An inverse orientation of VK gene clusters would explain published data on rearrangement products in B-cells if an inversion-deletion mechanism is assumed.

摘要

编码人类κ型免疫球蛋白可变区(VK)的基因座新片段的结构已被阐明。该片段(B簇)包含六个VK序列,它们属于三个不同的亚组,并以相同的转录方向排列。发现B簇的一部分与VK基因座的另一个先前克隆的区域(A簇)非常相似。根据VK序列的位置,A簇和B簇同源区域之间的序列差异在0.2%至3.7%之间。基因和假基因的差异也在同一范围内。用来自不同个体的DNA进行的杂交实验清楚地表明,这两个片段位于VK基因座内的不同位置,并不代表等位基因变体。A簇和B簇之间的序列同源性高于这两个簇与一个等位基因变体的同源性,该等位基因变体由从另一个个体分离的DNA片段代表。这些结果,连同文献中关于VK基因座另外两个同源区域的报道,使得很可能甚至整个基因座的大部分都是重复的。在这种情况下,VK基因的数量将高于先前基于杂交研究估计的数量。如果假设存在倒位-缺失机制,VK基因簇的反向排列将解释已发表的关于B细胞重排产物的数据。

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