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青春期后,新皮质RELN启动子甲基化显著增加。

Neocortical RELN promoter methylation increases significantly after puberty.

作者信息

Lintas Carla, Persico Antonio M

机构信息

Laboratory of Molecular Psychiatry and Neurogenetics, University Campus Bio-Medico, IRCCS Fondazione Santa Lucia, Rome, Italy.

出版信息

Neuroreport. 2010 Jan 27;21(2):114-8. doi: 10.1097/WNR.0b013e328334b343.

Abstract

Reelin plays a pivotal role in neurodevelopment. Excessive RELN promoter methylation and/or decreased RELN gene expression have been described in schizophrenia and autism. We assessed RELN promoter methylation in post-mortem temporocortical tissue (Brodmann Area 41/42) of three prepuberal and six postpuberal normal individuals. The former display very little or no methylation, whereas most postpuberal individuals are heavily methylated, especially at CpG positions located between -131 and -98 bp (prepuberal vs. postpuberal, P<0.05). Sex hormones thus seemingly boost DNA methylation at the RELN promoter. This physiological change could significantly contribute to the onset of schizophrenia and the worsening of autistic behaviors, both typically occurring at puberty.

摘要

Reelin在神经发育中起关键作用。精神分裂症和自闭症患者存在RELN启动子过度甲基化和/或RELN基因表达降低的情况。我们评估了3名青春期前和6名青春期后正常个体的死后颞叶皮质组织(布罗德曼区41/42)中的RELN启动子甲基化情况。前者显示出极少或没有甲基化,而大多数青春期后个体甲基化程度很高,尤其是在位于-131至-98 bp之间的CpG位点(青春期前与青春期后相比,P<0.05)。因此,性激素似乎会促进RELN启动子处的DNA甲基化。这种生理变化可能会显著促成精神分裂症的发病以及自闭症行为的恶化,这两种情况通常都发生在青春期。

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