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人类T细胞受体Vβ和Jβ基因库的变异:采用锚定聚合酶链反应进行分析

Variation in human T cell receptor V beta and J beta repertoire: analysis using anchor polymerase chain reaction.

作者信息

Rosenberg W M, Moss P A, Bell J I

机构信息

Institute of Molecular Medicine, John Radcliffe Hospital, Oxford, Great Britain.

出版信息

Eur J Immunol. 1992 Feb;22(2):541-9. doi: 10.1002/eji.1830220237.

Abstract

Anchor polymerase chain reaction has been applied to the study of human T cell receptor beta chain repertoire in peripheral blood. The use of this technique has demonstrated that considerable variation in V beta and J beta usage exists, both within and between individuals. Particular V beta families, including V beta 6, V beta 4 and V beta 12 are commonly utilized, while families such as V beta 10, V beta 11 and V beta 15 are rare in all individuals studied. Marked interindividual variation in V beta usage was detected for V beta 12 and V beta 4. Biased usage of J beta elements is a prominent feature of peripheral repertoire, while there is no evidence for preferential V beta-J beta recombination events. Biased J beta usage in expressed V beta-D beta-J beta-C beta transcripts, subject to selection, was the same as that in aberrant, unselected D beta-J beta-C beta transcripts, implying that bias resulted from events relating to rearrangement itself, in the absence of selection. N-region diversity showed some evidence for preferential insertion of deoxyguanosine, consistent with the action of terminal deoxytransferase. No P-nucleotide incorporation was seen in association with intact J beta elements. These data provide evidence of some of the variation in human T cell receptor beta chain repertoire and provide a basis for comparisons with sequences which may be obtained in autoimmune and superantigen-mediated diseases.

摘要

锚定聚合酶链反应已应用于外周血中人类T细胞受体β链库的研究。该技术的应用表明,个体内部和个体之间在Vβ和Jβ的使用上存在相当大的差异。特定的Vβ家族,包括Vβ6、Vβ4和Vβ12,通常被使用,而Vβ10、Vβ11和Vβ15等家族在所有研究个体中都很少见。检测到Vβ12和Vβ4在Vβ使用上存在明显的个体间差异。Jβ元件的偏向使用是外周库的一个突出特征,而没有证据表明存在优先的Vβ-Jβ重组事件。在经过选择的表达的Vβ-Dβ-Jβ-Cβ转录本中Jβ的偏向使用与异常的、未选择的Dβ-Jβ-Cβ转录本中的相同,这意味着偏向是在没有选择的情况下由与重排本身相关的事件导致的。N区多样性显示出一些脱氧鸟苷优先插入的证据,这与末端脱氧转移酶的作用一致。在完整的Jβ元件中未观察到P核苷酸的掺入。这些数据为人类T细胞受体β链库中的一些变异提供了证据,并为与自身免疫性疾病和超抗原介导的疾病中可能获得的序列进行比较提供了基础。

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