An overview of current strategies and future prospects in drug repurposing in tuberculosis

Q4 Biochemistry, Genetics and Molecular Biology
Dilpreet Singh, Amrinder Singh, P. Chawla
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Abstract

A large number of the population faces mortality as an effect of tuberculosis (TB). The line of treatment in the management of TB faces a jolt with ever-increasing multi-drug resistance (DR) cases. Further, the drugs engaged in the treatment of TB are associated with different toxicities, such as renal and hepatic toxicity. Different combinations are sought for effective anti-tuberculosis (anti-TB) effects with a decrease in toxicity. In this regard, drug repurposing has been very promising in improving the efficacy of drugs by enhancement of bioavailability and widening the safety margin. The success in drug repurposing lies in specified binding and inhibition of a particular target in the drug molecule. Different drugs have been repurposed for various ailments like cancer, Alzheimer’s disease, acquired immunodeficiency syndrome (AIDS), hair loss, etc. Repurposing in anti-TB drugs holds great potential too. The use of whole-cell screening assays and the availability of large chemical compounds for testing against Mycobacterium tuberculosis poses a challenge in this development. The target-based discovery of sites has emerged in the form of phenotypic screening as ethionamide R (EthR) and malate synthase inhibitors are similar to pharmaceuticals. In this review, the authors have thoroughly described the drug repurposing techniques on the basis of pharmacogenomics and drug metabolism, pathogen-targeted therapy, host-directed therapy, and bioinformatics approaches for the identification of drugs. Further, the significance of repurposing of drugs elaborated on large databases has been revealed. The role of genomics and network-based methods in drug repurposing has been also discussed in this article.
结核病药物再利用的当前策略和未来前景综述
由于结核病的影响,大量人口面临死亡。随着多药耐药(DR)病例的不断增加,结核病的治疗路线面临着巨大的冲击。此外,用于治疗结核病的药物具有不同的毒性,例如肾毒性和肝毒性。寻求不同的组合以获得有效的抗结核(抗结核)效果,同时降低毒性。在这方面,药物再利用通过提高生物利用度和扩大安全边际来提高药物的疗效是非常有希望的。药物再利用的成功在于药物分子中特定靶点的特定结合和抑制。不同的药物被用于治疗各种疾病,如癌症、阿尔茨海默病、获得性免疫缺陷综合症(艾滋病)、脱发等。抗结核药物的再利用也有很大的潜力。全细胞筛选试验的使用和用于检测结核分枝杆菌的大化合物的可用性对这一发展提出了挑战。基于靶标的位点发现以表型筛选的形式出现,因为乙硫酰胺R (EthR)和苹果酸合成酶抑制剂类似于药物。本文综述了基于药物基因组学和药物代谢、病原体靶向治疗、宿主靶向治疗和生物信息学方法的药物再利用技术。此外,揭示了在大型数据库中详细说明的药物重新利用的重要性。本文还讨论了基因组学和基于网络的方法在药物再利用中的作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
2.10
自引率
0.00%
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0
审稿时长
13 weeks
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