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锂和丙戊酸分子靶点的相互作用网络揭示了细胞凋亡功能簇和神经营养因子信号的惊人富集。

Interaction networks of lithium and valproate molecular targets reveal a striking enrichment of apoptosis functional clusters and neurotrophin signaling.

机构信息

Human Genetics Branch, National Institute of Mental Health, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

Pharmacogenomics J. 2012 Aug;12(4):328-41. doi: 10.1038/tpj.2011.9. Epub 2011 Mar 8.

Abstract

The overall neurobiological mechanisms by which lithium and valproate stabilize mood in bipolar disorder patients have yet to be fully defined. The therapeutic efficacy and dissimilar chemical structures of these medications suggest that they perturb both shared and disparate cellular processes. To investigate key pathways and functional clusters involved in the global action of lithium and valproate, we generated interaction networks formed by well-supported drug targets. Striking functional similarities emerged. Intersecting nodes in lithium and valproate networks highlighted a strong enrichment of apoptosis clusters and neurotrophin signaling. Other enriched pathways included MAPK, ErbB, insulin, VEGF, Wnt and long-term potentiation indicating a widespread effect of both drugs on diverse signaling systems. MAPK1/3 and AKT1/2 were the most preponderant nodes across pathways suggesting a central role in mediating pathway interactions. The convergence of biological responses unveils a functional signature for lithium and valproate that could be key modulators of their therapeutic efficacy.

摘要

锂盐和丙戊酸盐稳定双相情感障碍患者情绪的整体神经生物学机制尚未完全确定。这些药物的治疗功效和不同的化学结构表明,它们会干扰共同和不同的细胞过程。为了研究锂盐和丙戊酸盐的全局作用所涉及的关键途径和功能簇,我们生成了由经过充分支持的药物靶点形成的相互作用网络。出现了惊人的功能相似性。锂盐和丙戊酸盐网络中的相交节点突出了细胞凋亡簇和神经营养因子信号的强烈富集。其他富集的途径包括 MAPK、ErbB、胰岛素、VEGF、Wnt 和长时程增强,表明这两种药物对多种信号系统都有广泛的影响。MAPK1/3 和 AKT1/2 是各条途径中最重要的节点,这表明它们在介导途径相互作用方面起着核心作用。生物反应的收敛揭示了锂盐和丙戊酸盐的功能特征,这可能是它们治疗效果的关键调节剂。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c7ef/3134562/11105f10c483/nihms268954f1.jpg

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