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Characterization of drug-induced transcriptional modules: towards drug repositioning and functional understanding

机译:药物诱导的转录模块的表征:对药物重新定位和功能的理解

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摘要

In pharmacology, it is crucial to understand the complex biological responses that drugs elicit in the human organism and how well they can be inferred from model organisms. We therefore identified a large set of drug-induced transcriptional modules from genome-wide microarray data of drug-treated human cell lines and rat liver, and first characterized their conservation. Over 70% of these modules were common for multiple cell lines and 15% were conserved between the human in vitro and the rat in vivo system. We then illustrate the utility of conserved and cell-type-specific drug-induced modules by predicting and experimentally validating (i) gene functions, e.g., 10 novel regulators of cellular cholesterol homeostasis and (ii) new mechanisms of action for existing drugs, thereby providing a starting point for drug repositioning, e.g., novel cell cycle inhibitors and new modulators of >α-adrenergic receptor, peroxisome proliferator-activated receptor and estrogen receptor. Taken together, the identified modules reveal the conservation of transcriptional responses towards drugs across cell types and organisms, and improve our understanding of both the molecular basis of drug action and human biology.
机译:在药理学中,至关重要的是要了解药物在人体内引起的复杂的生物学反应以及从模型生物中推断出药物的效果。因此,我们从药物治疗的人细胞系和大鼠肝脏的全基因组微阵列数据中识别出一大组药物诱导的转录模块,并首先对其保守性进行了表征。这些模块中有70%以上是多种细胞系所共有的,而在人类体外系统和大鼠体内系统之间则保留了15%。然后,我们通过预测和实验验证(i)基因功能,例如细胞胆固醇稳态的10种新型调节剂和(ii)现有药物的新作用机制,来说明保守的和特定于细胞类型的药物诱导模块的实用性为药物重新定位提供了起点,例如>α-肾上腺素能受体,过氧化物酶体增殖物激活受体和雌激素受体的新型细胞周期抑制剂和新调节剂。总之,确定的模块揭示了跨细胞类型和生物体对药物的转录反应的保守性,并增进了我们对药物作用的分子基础和人类生物学的理解。

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