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脑蛋白质组全基因组关联研究提示抑郁症发病机制中的新蛋白。

Brain proteome-wide association study implicates novel proteins in depression pathogenesis.

机构信息

Department of Neurology, Emory University School of Medicine, Atlanta, GA, USA.

Department of Human Genetics, Emory University School of Medicine, Atlanta, GA, USA.

出版信息

Nat Neurosci. 2021 Jun;24(6):810-817. doi: 10.1038/s41593-021-00832-6. Epub 2021 Apr 12.

Abstract

Depression is a common condition, but current treatments are only effective in a subset of individuals. To identify new treatment targets, we integrated depression genome-wide association study (GWAS) results (N = 500,199) with human brain proteomes (N = 376) to perform a proteome-wide association study of depression followed by Mendelian randomization. We identified 19 genes that were consistent with being causal in depression, acting via their respective cis-regulated brain protein abundance. We replicated nine of these genes using an independent depression GWAS (N = 307,353) and another human brain proteomic dataset (N = 152). Eleven of the 19 genes also had cis-regulated mRNA levels that were associated with depression, based on integration of the depression GWAS with human brain transcriptomes (N = 888). Meta-analysis of the discovery and replication proteome-wide association study analyses identified 25 brain proteins consistent with being causal in depression, 20 of which were not previously implicated in depression by GWAS. Together, these findings provide promising brain protein targets for further mechanistic and therapeutic studies.

摘要

抑郁症是一种常见病症,但目前的治疗方法仅对一部分人有效。为了确定新的治疗靶点,我们整合了抑郁症全基因组关联研究(GWAS)的结果(N=500199)和人类大脑蛋白质组学(N=376),对抑郁症进行了全蛋白质组关联研究,随后进行了孟德尔随机化分析。我们确定了 19 个与抑郁症因果关系一致的基因,这些基因通过各自的顺式调控脑蛋白丰度发挥作用。我们使用另一个独立的抑郁症 GWAS(N=307353)和另一个人类大脑蛋白质组数据集(N=152)复制了其中的九个基因。在将抑郁症 GWAS 与人类大脑转录组学(N=888)整合后,这 19 个基因中的 11 个也具有与抑郁症相关的顺式调控 mRNA 水平。发现和复制全蛋白质组关联研究分析的荟萃分析确定了 25 个与抑郁症因果关系一致的大脑蛋白质,其中 20 个以前未被 GWAS 提示与抑郁症有关。总之,这些发现为进一步的机制和治疗研究提供了有希望的大脑蛋白质靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f12d/8530461/7ffd8f790462/nihms-1680458-f0001.jpg

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