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The epigenetic stability of the locus control region-deficient IgH locus in mouse hybridoma cells is a clonally varying, heritable feature.

机译:小鼠杂交瘤细胞中基因座控制区缺陷型IgH基因座的表观遗传稳定性是克隆变化的,可遗传的特征。

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摘要

Cis-acting elements such as enhancers and locus control regions (LCRs) prevent silencing of gene expression. We have shown previously that targeted deletion of an LCR in the immunoglobulin heavy-chain (IgH) locus creates conditions in which the immunoglobulin micro heavy chain gene can exist in either of two epigenetically inherited states, one in which micro expression is positive and one in which micro expression is negative, and that the positive and negative states are maintained by a cis-acting mechanism. As described here, the stability of these states, i.e., the propensity of a cell to switch from one state to the other, varied among subclones and was an inherited, clonal feature. A similar variation in stability was seen for IgH loci that both lacked and retained the matrix attachment regions associated with the LCR. Our analysis of cell hybrids formed by fusing cells in which the micro expression had different stabilities indicated that stability was also determined by a cis-acting feature of the IgH locus. Our results thus show that a single-copy gene in the same chromosomal location and in the presence of the same transcription factors can exist in many different states of expression.
机译:顺式作用元件,例如增强子和基因座控制区(LCR)可防止基因表达沉默。先前我们已经证明,免疫球蛋白重链(IgH)基因座中LCR的靶向缺失创造了这样的条件,其中免疫球蛋白微重链基因可以以两种表观遗传的状态存在,其中一种是微表达为阳性,另一种是微表达为阳性。微表达为负,并且正和负状态通过顺式作用机制维持。如这里所述,这些状态的稳定性,即细胞从一种状态切换到另一种状态的倾向,在亚克隆之间变化,并且是遗传的克隆特征。对于缺少和保留与LCR相关的基质附着区域的IgH基因座,可以看到相似的稳定性变化。我们对融合微表达具有不同稳定性的细胞形成的细胞杂交体的分析表明,稳定性还取决于IgH基因座的顺式作用特征。因此,我们的结果表明,处于相同染色体位置且存在相同转录因子的单拷贝基因可以以许多不同的表达状态存在。

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