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Transcriptomic profiling of human hippocampal progenitor cells treated with antidepressants and its application in drug repositioning

机译:抗抑郁药对人海马祖细胞的转录组谱分析及其在药物重新定位中的应用

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摘要

Current pharmacological treatments for major depressive disorder (MDD) are ineffective in a significant proportion of patients, and the identification of new antidepressant compounds has been difficult. ‘Connectivity mapping’ is a method that can be used to identify drugs that elicit similar downstream effects on mRNA levels when compared to current treatments, and thus may point towards possible repositioning opportunities. We investigated genome-wide transcriptomic changes to human hippocampal progenitor cells treated with therapeutically relevant concentrations of a tricyclic antidepressant (nortriptyline) and a selective serotonin reuptake inhibitor (escitalopram). We identified mRNA changes common to both drugs to create an ‘antidepressant mRNA signature’. We used this signature to probe the Library of Integrated Network-based Cellular Signatures (LINCS) and to identify other compounds that elicit similar changes to mRNA in neural progenitor cells. Results from LINCS revealed that the tricyclic antidepressant clomipramine elicited mRNA changes most similar to our mRNA signature, and we identified W-7 and vorinostat as functionally relevant drug candidates, which may have repositioning potential. Our results are encouraging and represent the first attempt to use connectivity mapping for drug repositioning in MDD.
机译:当前用于重度抑郁症(MDD)的药物治疗在相当大比例的患者中无效,并且很难鉴定新的抗抑郁化合物。 “连通性作图”是一种可用于识别与当前治疗方法相比对mRNA水平产生类似下游影响的药物的方法,因此可能指出可能的重新定位机会。我们研究了用治疗相关浓度的三环抗抑郁药(去甲替林)和选择性5-羟色胺再摄取抑制剂(依他普仑)治疗的人海马祖细胞的全基因组转录组变化。我们确定了这两种药物共有的mRNA变化,以产生“抗抑郁剂mRNA签名”。我们使用此签名来探查基于集成网络的细胞签名库(LINCS),并确定引起神经祖细胞mRNA相似变化的其他化合物。 LINCS的结果显示,三环抗抑郁药氯米帕明引起的mRNA变化与我们的mRNA信号最相似,并且我们将W-7和伏立诺他确定为功能相关的候选药物,可能具有重新定位的潜力。我们的结果令人鼓舞,并且代表了使用连接映射在MDD中进行药物重新定位的首次尝试。

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