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Transcriptomic Signatures Predict Regulators of Drug Synergy and Clinical Regimen Efficacy against Tuberculosis

机译:转录组签名预测药物协同作用和针对肺结核的临床治疗功效的调节剂

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The rapid spread of multidrug-resistant strains has created a pressing need for new drug regimens to treat tuberculosis (TB), which kills 1.8 million people each year. Identifying new regimens has been challenging due to the slow growth of the pathogen Mycobacterium tuberculosis (MTB), coupled with the large number of possible drug combinations. Here we present a computational model (INDIGO-MTB) that identified synergistic regimens featuring existing and emerging anti-TB drugs after screening in silico more than 1 million potential drug combinations using MTB drug transcriptomic profiles. INDIGO-MTB further predicted the gene Rv1353c as a key transcriptional regulator of multiple drug interactions, and we confirmed experimentally that Rv1353c upregulation reduces the antagonism of the bedaquiline-streptomycin combination. A retrospective analysis of 57 clinical trials of TB regimens using INDIGO-MTB revealed that synergistic combinations were significantly more efficacious than antagonistic combinations ( P value = 1?×?10~(?4)) based on the percentage of patients with negative sputum cultures after 8?weeks of treatment. Our study establishes a framework for rapid assessment of TB drug combinations and is also applicable to other bacterial pathogens.
机译:耐多药菌株的迅速传播已经迫切需要治疗结核病的新药物疗法,每年要杀死180万人。由于病原体结核分枝杆菌(MTB)的缓慢生长以及大量可能的药物组合,因此确定新的治疗方案一直是一项挑战。在此,我们介绍了一种计算模型(INDIGO-MTB),该模型在使用MTB药物转录组资料在计算机上筛选了超过一百万种潜在的药物组合后,确定了以现有和新兴抗结核药物为特征的协同方案。 INDIGO-MTB进一步预测基因Rv1353c是多种药物相互作用的关键转录调节因子,我们通过实验证实Rv1353c的上调减少了苯达喹啉-链霉素组合的拮抗作用。对使用INDIGO-MTB进行的57项TB方案临床试验的回顾性分析表明,根据痰培养阴性患者的百分比,协同组合比拮抗组合有效得多(P值= 1?×?10〜(?4))。治疗8周后。我们的研究建立了快速评估结核病药物组合的框架,也适用于其他细菌性病原体。

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