首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >In psychosis, cortical interneurons overexpress DNA-methyltransferase 1.
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In psychosis, cortical interneurons overexpress DNA-methyltransferase 1.

机译:在精神病中,皮质神经元过表达DNA-甲基转移酶1。

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Cortical DNA-methyltransferase 1 (DNMT1) is preferentially expressed in interneurons secreting GABA where it very likely contributes to promoter CpG island hypermethylation, thus causing a down-regulation of promoter functions. To consolidate and expand on previous findings that, in the cortex of schizophrenia (SZ) brains, glutamic acid decarboxylase 67 (GAD67) expression is down-regulated whereas that of DNMT1 is up-regulated, we studied both parameters in Brodmann's area (BA) 9 from the McLean 66 Cohort Collection (Harvard Brain Tissue Resource Center, Belmont, MA). In BA9 of SZ and bipolar disorder patients with psychosis, DNMT1 mRNA and protein expression preferentially increases in layer I, II, and IV interneurons, and this increase is paralleled by a decreased number of GAD67 mRNA-positive neurons. The increase in DNMT1 and the decrease in GAD67-expressing neurons were unrelated to postmortem interval, pH, RNA quality, or to the presence, dose, or duration of antipsychotic (APS) medication, with the exception of a subgroup of SZ patients treated with a combination of valproate and APS in which the expression of DNMT1 failed to change. The DNMT1 increase and the GAD67 decrease in BA9 interneurons are significant features of SZ and bipolar disorder with psychosis. Interestingly, the DNMT1 increase failed to occur when patients with psychosis received a combination of valproate and APS treatment but not APS monotherapy.
机译:皮质DNA-甲基转移酶1(DNMT1)在分泌GABA的中间神经元中优先表达,在其中它很可能有助于启动子CpG岛超甲基化,从而导致启动子功能的下调。为了巩固和扩展先前的发现,在精神分裂症(SZ)大脑皮层中,谷氨酸脱羧酶67(GAD67)的表达下调,而DNMT1的表达上调,我们研究了布罗德曼区域(BA)的两个参数9来自McLean 66队列研究集(马萨诸塞州贝尔蒙特的哈佛大学脑组织资源中心)。在患有精神病的SZ和双相情感障碍患者的BA9中,DNMT1 mRNA和蛋白质表达优先在I,II和IV层中神经元中增加,并且这种增加与GAD67 mRNA阳性神经元数量减少平行。 DNMT1的增加和表达GAD67的神经元的减少与死后间隔,pH,RNA质量或抗精神病药(APS)的存在,剂量或持续时间无关,但接受SZ治疗的SZ患者亚组除外丙戊酸和APS的组合,其中DNMT1的表达未能改变。 BA9间神经元中DNMT1的增加和GAD67的减少是SZ和精神病双相情感障碍的重要特征。有趣的是,当精神病患者接受丙戊酸盐和APS的联合治疗但未接受APS单药治疗时,DNMT1的升高并未发生。

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