Epigenetic profiling reveals a developmental decrease in promoter accessibility during cortical maturation in vivo

Neuroepigenetics Pub Date : 2016-12-01 DOI:10.1016/j.nepig.2016.10.002

Ishwariya Venkatesh, Matthew T. Simpson, Denise M. Coley, Murray G. Blackmore

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引用次数: 24

Abstract

Axon regeneration in adult central nervous system (CNS) is limited in part by a developmental decline in the ability of injured neurons to re-express needed regeneration associated genes (RAGs). Adult CNS neurons may lack appropriate pro-regenerative transcription factors, or may display chromatin structure that restricts transcriptional access to RAGs. Here we performed epigenetic profiling around the promoter regions of key RAGs, and found progressive restriction across a time course of cortical maturation. These data identify a potential intrinsic constraint to axon growth in adult CNS neurons. Neurite outgrowth from cultured postnatal cortical neurons, however, proved insensitive to treatments that improve axon growth in other cell types, including combinatorial overexpression of AP1 factors, overexpression of histone acetyltransferases, and pharmacological inhibitors of histone deacetylases. This insensitivity could be due to intermediate chromatin closure at the time of culture, and highlights important differences in cell culture models used to test potential pro-regenerative interventions.

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表观遗传分析揭示了在体内皮层成熟过程中启动子可及性的发育减少

成人中枢神经系统(CNS)的轴突再生在一定程度上受到损伤神经元重新表达所需再生相关基因(RAGs)的能力发育下降的限制。成年中枢神经系统神经元可能缺乏适当的促再生转录因子，或者可能显示限制转录途径的染色质结构。在这里，我们在关键破布的启动子区域周围进行了表观遗传分析，并发现在皮质成熟的时间过程中进行性限制。这些数据确定了成年中枢神经系统神经元轴突生长的潜在内在约束。然而，从培养的出生后皮质神经元中生长出来的神经突对其他细胞类型中改善轴突生长的处理不敏感，包括AP1因子的组合过表达、组蛋白乙酰转移酶的过表达和组蛋白去乙酰化酶的药物抑制剂。这种不敏感可能是由于培养时的中间染色质关闭，并且突出了用于测试潜在促再生干预的细胞培养模型的重要差异。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Neuroepigenetics

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