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Allelic exclusion of the immunoglobulin heavy chain locus is independent of its nuclear localization in mature B cells

机译:免疫球蛋白重链基因座的等位基因排斥反应与其在成熟B细胞中的核定位无关

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摘要

In developing B cells, the immunoglobulin heavy chain (IgH) locus is thought to move from repressive to permissive chromatin compartments to facilitate its scheduled rearrangement. In mature B cells, maintenance of allelic exclusion has been proposed to involve recruitment of the non-productive IgH allele to pericentromeric heterochromatin. Here, we used an allele-specific chromosome conformation capture combined with sequencing (4C-seq) approach to unambigously follow the individual IgH alleles in mature B lymphocytes. Despite their physical and functional difference, productive and non-productive IgH alleles in B cells and unrearranged IgH alleles in T cells share many chromosomal contacts and largely reside in active chromatin. In brain, however, the locus resides in a different repressive environment. We conclude that IgH adopts a lymphoid-specific nuclear location that is, however, unrelated to maintenance of allelic exclusion. We additionally find that in mature B cells-but not in T cells-the distal V-H regions of both IgH alleles position themselves away from active chromatin. This, we speculate, may help to restrict enhancer activity to the productively rearranged V-H promoter element.
机译:在发育中的B细胞中,免疫球蛋白重链(IgH)基因座被认为从抑制染色质区室转移到允许染色质区室,以促进其预定的重排。在成熟的B细胞中,已提出维持等位基因排斥的方法涉及将非生产性IgH等位基因募集到着丝粒异体染色质上。在这里,我们使用等位基因特异性染色体构象捕获与测序(4C-seq)方法相结合,明确地跟踪了成熟B淋巴细胞中的各个IgH等位基因。尽管在物理和功能上存在差异,但B细胞中的生产性和非生产性IgH等位基因以及T细胞中未重排的IgH等位基因共享许多染色体接触,并主要存在于活性染色质中。然而,在大脑中,基因座位于不同的抑制环境中。我们得出的结论是,IgH具有特定于淋巴的核位置,但与维持等位基因排斥无关。我们还发现,在成熟的B细胞而非T细胞中,两个IgH等位基因的远端V-H区将自身定位为远离活性染色质。我们推测,这可能有助于将增强子活性限制在生产性重排的V-H启动子元件上。

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