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V(D)J重组酶介导人外周血T细胞中隐蔽重组信号序列处的染色体间次黄嘌呤磷酸核糖转移酶改变。

V(D)J recombinase mediated inter-chromosomal HPRT alterations at cryptic recombination signal sequences in peripheral human T cells.

作者信息

Messier Terri L, O'Neill J Patrick, Finette Barry A

机构信息

Department of Pediatrics, University of Vermont, Burlington, Vermont, USA.

出版信息

Hum Mutat. 2006 Aug;27(8):829. doi: 10.1002/humu.9440.

Abstract

The V(D)J recombinase enzyme complex is responsible for the development of a diverse immune system by catalyzing intra-molecular rearrangements of immunoglobulin (Ig) and T cell receptor (TCR) genes at specific recombination signal sequences (RSSs). This enzyme complex has also been implicated in mediating pathologic and non-pathologic intra- and inter-molecular genomic rearrangements at cryptic (Psi) RSSs outside the immune system loci in lymphoid cells. We describe here two V(D)J recombinase mediated genomic rearrangements resulting in alterations at the HPRT locus in human T-cells. These are inter-chromosomal insertions in which DNA fragments are inserted at breakpoints generated by V(D)J recombinase cleavage at Psi RSS sites in the HPRT locus at Xq26. In the first, a TCR signal ended segment from chromosome 14q11 is inserted at a Psi RSS in intron 1 of the HPRT locus. In the second, a DNA fragment from 9q22 is integrated between the coding ends generated by a V(D)J recombinase mediated HPRT deletion. Identification of these in vivo V(D)J mediated inter-chromosomal insertions at Psi RSSs in the HPRT gene supports the accumulating evidence that V(D)J recombinase can mediate mutagenic rearrangements in humans with potential pathologic consequences.

摘要

V(D)J重组酶复合物通过催化免疫球蛋白(Ig)和T细胞受体(TCR)基因在特定重组信号序列(RSSs)处的分子内重排,负责发育出多样化的免疫系统。该酶复合物还与介导淋巴细胞免疫系统基因座外隐蔽(Psi)RSSs处的病理性和非病理性分子内和分子间基因组重排有关。我们在此描述了两种由V(D)J重组酶介导的基因组重排,导致人类T细胞中次黄嘌呤磷酸核糖转移酶(HPRT)基因座发生改变。这些是染色体间插入,其中DNA片段插入到由V(D)J重组酶在Xq26的HPRT基因座的Psi RSS位点切割产生的断点处。在第一个例子中,来自14q11染色体的TCR信号末端片段插入到HPRT基因座内含子1的一个Psi RSS处。在第二个例子中,来自9q22的一个DNA片段整合到由V(D)J重组酶介导的HPRT缺失产生的编码末端之间。在HPRT基因的Psi RSSs处鉴定出这些体内V(D)J介导的染色体间插入,支持了越来越多的证据,即V(D)J重组酶可以介导人类中的致突变重排,并具有潜在的病理后果。

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