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首页> 外文期刊>The Journal of Immunology: Official Journal of the American Association of Immunologists >Positive and Negative Transcriptional States of a Variegating Immunoglobulin Heavy Chain (IgH) Locus Are Maintained by a cis-Acting Epigenetic Mechanism.
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Positive and Negative Transcriptional States of a Variegating Immunoglobulin Heavy Chain (IgH) Locus Are Maintained by a cis-Acting Epigenetic Mechanism.

机译:多样化的免疫球蛋白重链(IgH)基因座的正和负转录状态通过顺式作用表观遗传机制得以维持。

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摘要

Analyses of transgene expression have defined essential components of a locus control region (LCR) in the J(H)-C micro intron of the IgH locus. Targeted deletion of this LCR from the endogenous IgH locus of hybridoma cells results in variegated expression, i.e., cells can exist in two epigenetically inherited states in which the Ig micro H chain gene is either active or silent; the active or silent state is typically transmitted to progeny cells through many cell divisions. In principle, cells in the two states might differ either in their content of specific transcription factors or in a cis-acting feature of the IgH locus. To distinguish between these mechanisms, we generated LCR-deficient, recombinant cell lines in which the Ig micro H chain genes were distinguished by a silent mutation and fused cells in which the micro gene was active with cells in which micro was silent. Our analysis showed that both parental active and silent transcriptional states were preserved in the hybrid cell, i.e., that two alleles of the same gene in the same nucleus can exist in two different states of expression through many cell divisions. These results indicate that the expression of the LCR-deficient IgH locus is not fully determined by the cellular complement of transcription factors, but is also subject to a cis-acting, self-propagating, epigenetic mark. The methylation inhibitor, 5-azacytidine, reactivated IgH in cells in which this gene was silent, suggesting that methylation is part of the epigenetic mark that distinguishes silent from active transcriptional states.
机译:转基因表达的分析已定义了IgH基因座的J(H)-C微内含子中基因座控制区(LCR)的基本组成部分。从杂交瘤细胞的内源性IgH基因座中有针对性地删除该LCR会导致表达多样化,即​​细胞可以以两种表观遗传的状态存在,其中Ig微H链基因处于活跃或沉默状态。活跃或沉默状态通常通过许多细胞分裂传递给子代细胞。原则上,处于两种状态的细胞在特异性转录因子的含量或IgH基因座的顺式作用特征上可能有所不同。为了区分这些机制,我们生成了LCR缺陷型重组细胞系,其中的Ig微H链基因通过沉默突变来区分,融合细胞中的微型基因与沉默的细胞有活性。我们的分析表明,亲本的活跃和沉默的转录状态都保留在杂交细胞中,即,同一核中同一基因的两个等位基因可以通过许多细胞分裂以两种不同的表达状态存在。这些结果表明,LCR缺陷型IgH基因座的表达不是完全由转录因子的细胞补体决定的,而是还具有顺式作用,自我繁殖的表观遗传标记。甲基化抑制剂5-氮杂胞苷在该基因沉默的细胞中重新激活了IgH,这表明甲基化是表观遗传标记的一部分,可以区分沉默与活跃的转录状态。

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