剖析严重精神障碍与细胞衰老标志物之间的遗传重叠:多效基因和可药物靶点的鉴定。
Dissecting the genetic overlap between severe mental disorders and markers of cellular aging: Identification of pleiotropic genes and druggable targets.
机构信息
Department of Biomedical Sciences, Section of Neuroscience and Clinical Pharmacology, University of Cagliari, Cagliari, Italy.
Section of Psychiatry, Department of Medical Sciences and Public Health, University of Cagliari, Cagliari, Italy.
出版信息
Neuropsychopharmacology. 2024 May;49(6):1033-1041. doi: 10.1038/s41386-024-01822-5. Epub 2024 Feb 24.
Patients with severe mental disorders such as bipolar disorder (BD), schizophrenia (SCZ) and major depressive disorder (MDD) show a substantial reduction in life expectancy, increased incidence of comorbid medical conditions commonly observed with advanced age and alterations of aging hallmarks. While severe mental disorders are heritable, the extent to which genetic predisposition might contribute to accelerated cellular aging is not known. We used bivariate causal mixture models to quantify the trait-specific and shared architecture of mental disorders and 2 aging hallmarks (leukocyte telomere length [LTL] and mitochondrial DNA copy number), and the conjunctional false discovery rate method to detect shared genetic loci. We integrated gene expression data from brain regions from GTEx and used different tools to functionally annotate identified loci and investigate their druggability. Aging hallmarks showed low polygenicity compared with severe mental disorders. We observed a significant negative global genetic correlation between MDD and LTL (r = -0.14, p = 6.5E-10), and no significant results for other severe mental disorders or for mtDNA-cn. However, conditional QQ plots and bivariate causal mixture models pointed to significant pleiotropy among all severe mental disorders and aging hallmarks. We identified genetic variants significantly shared between LTL and BD (n = 17), SCZ (n = 55) or MDD (n = 19), or mtDNA-cn and BD (n = 4), SCZ (n = 12) or MDD (n = 1), with mixed direction of effects. The exonic rs7909129 variant in the SORCS3 gene, encoding a member of the retromer complex involved in protein trafficking and intracellular/intercellular signaling, was associated with shorter LTL and increased predisposition to all severe mental disorders. Genetic variants underlying risk of SCZ or MDD and shorter LTL modulate expression of several druggable genes in different brain regions. Genistein, a phytoestrogen with anti-inflammatory and antioxidant effects, was an upstream regulator of 2 genes modulated by variants associated with risk of MDD and shorter LTL. While our results suggest that shared heritability might play a limited role in contributing to accelerated cellular aging in severe mental disorders, we identified shared genetic determinants and prioritized different druggable targets and compounds.
患有双相情感障碍 (BD)、精神分裂症 (SCZ) 和重度抑郁症 (MDD) 等严重精神障碍的患者预期寿命明显缩短,合并症的发生率增加,这些合并症通常与老年有关,并改变了衰老的特征。虽然严重精神障碍具有遗传性,但遗传易感性在多大程度上可能导致细胞衰老加速尚不清楚。我们使用双变量因果混合模型来量化精神障碍和 2 个衰老特征(白细胞端粒长度 [LTL] 和线粒体 DNA 拷贝数)的特质特异性和共享结构,以及并发假发现率方法来检测共享的遗传位点。我们整合了来自 GTEx 大脑区域的基因表达数据,并使用不同的工具对鉴定出的位点进行功能注释,并研究它们的可药性。与严重精神障碍相比,衰老特征的多基因性较低。我们观察到 MDD 和 LTL 之间存在显著的负全局遗传相关性(r = -0.14,p = 6.5E-10),而其他严重精神障碍或 mtDNA-cn 则没有显著结果。然而,条件 QQ 图和双变量因果混合模型表明,所有严重精神障碍和衰老特征之间存在显著的多效性。我们鉴定了 LTL 和 BD(n = 17)、SCZ(n = 55)或 MDD(n = 19)或 mtDNA-cn 和 BD(n = 4)、SCZ(n = 12)或 MDD(n = 1)之间存在显著共享的遗传变异体,其影响方向混合。编码参与蛋白质运输和细胞内/细胞间信号转导的逆行体复合物的 SORCS3 基因中的外显子 rs7909129 变体与 LTL 缩短和所有严重精神障碍的易感性增加有关。SCZ 或 MDD 风险和 LTL 缩短的遗传变异体调节不同大脑区域中多个可药物治疗基因的表达。具有抗炎和抗氧化作用的植物雌激素染料木黄酮是与 MDD 和 LTL 缩短相关的风险变体调节的 2 个基因的上游调节剂。虽然我们的研究结果表明,共享的遗传性可能在严重精神障碍导致细胞衰老加速方面的作用有限,但我们鉴定了共享的遗传决定因素,并确定了不同的可药物靶点和化合物。
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