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Nuclear aggregation of olfactory receptor genes governs their monogenic expression

机译:嗅觉受体基因的核聚集决定着它们的单基因表达

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摘要

Gene positioning and regulation of nuclear architecture are thought to influence gene expression. Here, we show that, in mouse olfactory neurons, silent olfactory receptor (OR) genes from different chromosomes converge in a small number of heterochromatic foci. These foci are OR exclusive and form in a cell-type-specific and differentiation-dependent manner. The aggregation of OR genes is developmentally synchronous with the downregulation of lamin b receptor (LBR) and can be reversed by ectopic expression of LBR in mature olfactory neurons. LBR-induced reorganization of nuclear architecture and disruption of OR aggregates perturbs the singularity of OR transcription and disrupts the targeting specificity of the olfactory neurons. Our observations propose spatial sequestering of heterochromatinized OR family members as a basis of monogenic and monoallelic gene expression. PaperClip:
机译:基因定位和核结构的调节被认为影响基因表达。在这里,我们显示,在小鼠嗅觉神经元中,来自不同染色体的沉默嗅觉受体(OR)基因会聚在少量的异色病灶中。这些灶是异或的,并以细胞类型特异性和分化依赖性方式形成。 OR基因的聚集与lamin b受体(LBR)的下调在发育上同步,并且可以通过在成熟的嗅觉神经元中异位表达LBR来逆转。 LBR诱导的核结构重组和OR聚集体的破坏扰乱了OR转录的奇异性,并破坏了嗅觉神经元的靶向特异性。我们的观察结果提出异染色质OR家庭成员的空间隔离作为单基因和单等位基因表达的基础。回形针:

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