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前额叶皮层星形胶质细胞在重度抑郁症中的作用:探索发病机制和潜在治疗靶点。

Prefrontal cortex astrocytes in major depressive disorder: exploring pathogenic mechanisms and potential therapeutic targets.

机构信息

Department of Pharmacology, School of Integrated Chinese and Western Medicine, Anhui University of Chinese Medicine, Hefei, 230012, China.

Department of Gynecology, Anhui Maternal and Child Health Hospital, Hefei, 230012, China.

出版信息

J Mol Med (Berl). 2024 Nov;102(11):1355-1369. doi: 10.1007/s00109-024-02487-9. Epub 2024 Sep 14.

Abstract

Major depressive disorder (MDD) is a prevalent mental health condition characterized by persistent feelings of sadness and hopelessness, affecting millions globally. The precise molecular mechanisms underlying MDD remain elusive, necessitating comprehensive investigations. Our study integrates transcriptomic analysis, functional assays, and computational modeling to explore the molecular landscape of MDD, focusing on the DLPFC. We identify key genomic alterations and co-expression modules associated with MDD, highlighting potential therapeutic targets. Functional enrichment and protein-protein interaction analyses emphasize the role of astrocytes in MDD progression. Machine learning is employed to develop a predictive model for MDD risk assessment. Single-cell and spatial transcriptomic analyses provide insights into cell type-specific expression patterns, particularly regarding astrocytes. We have identified significant genomic alterations and co-expression modules associated with MDD in the DLPFC. Key genes involved in neuroactive ligand-receptor interaction pathways, notably in astrocytes, have been highlighted. Additionally, we developed a predictive model for MDD risk assessment based on selected key genes. Single-cell and spatial transcriptomic analyses underscored the role of astrocytes in MDD. Virtual screening of compounds targeting GPR37L1, KCNJ10, and PPP1R3C proteins has identified potential therapeutic candidates. In summary, our comprehensive approach enhances the understanding of MDD's molecular underpinnings and offers promising opportunities for advancing therapeutic interventions, ultimately aiming to alleviate the burden of this debilitating mental health condition. KEY MESSAGES: Our investigation furnishes insightful revelations concerning the dysregulation of astrocyte-associated processes in MDD. We have pinpointed specific genes, namely KCNJ10, PPP1R3C, and GPR37L1, as potential candidates warranting further exploration and therapeutic intervention. We incorporate a virtual screening of small molecule compounds targeting KCNJ10, PPP1R3C, and GPR37L1, presenting a promising trajectory for drug discovery in MDD.

摘要

重度抑郁症(Major depressive disorder,MDD)是一种常见的精神健康疾病,其特征是持续的悲伤和绝望感,影响着全球数百万人。MDD 的精确分子机制仍不清楚,需要进行全面的研究。我们的研究综合了转录组分析、功能测定和计算模型,以探索 MDD 的分子图谱,重点是 DLPFC。我们确定了与 MDD 相关的关键基因组改变和共表达模块,突出了潜在的治疗靶点。功能富集和蛋白质-蛋白质相互作用分析强调了星形胶质细胞在 MDD 进展中的作用。机器学习被用于开发 MDD 风险评估的预测模型。单细胞和空间转录组分析提供了关于细胞类型特异性表达模式的见解,特别是关于星形胶质细胞。我们已经确定了与 DLPFC 中的 MDD 相关的重要基因组改变和共表达模块。涉及神经活性配体-受体相互作用途径的关键基因,特别是星形胶质细胞中的关键基因,已被突出显示。此外,我们基于选定的关键基因开发了用于 MDD 风险评估的预测模型。单细胞和空间转录组分析强调了星形胶质细胞在 MDD 中的作用。针对 GPR37L1、KCNJ10 和 PPP1R3C 蛋白的化合物虚拟筛选已确定潜在的治疗候选物。总之,我们的综合方法增强了对 MDD 分子基础的理解,并为推进治疗干预提供了有希望的机会,最终旨在减轻这种使人衰弱的心理健康状况的负担。关键信息:我们的研究提供了关于 MDD 中星形胶质细胞相关过程失调的深入了解。我们已经确定了特定的基因,即 KCNJ10、PPP1R3C 和 GPR37L1,作为值得进一步探索和治疗干预的潜在候选基因。我们结合了针对 KCNJ10、PPP1R3C 和 GPR37L1 的小分子化合物虚拟筛选,为 MDD 中的药物发现提供了有前途的途径。

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