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下一代抗疟药物:杂合分子作为药物设计的新策略。

Next-Generation Antimalarial Drugs: Hybrid Molecules as a New Strategy in Drug Design.

作者信息

Muregi Francis W, Ishih Akira

机构信息

Department of Infectious Diseases, Hamamatsu University School of Medicine Hamamatsu, Japan.

出版信息

Drug Dev Res. 2010 Feb;71(1):20-32. doi: 10.1002/ddr.20345.

Abstract

Malaria is a disease that affects nearly 40% of the global population, and chemotherapy remains the mainstay of its control strategy. The global malaria situation is increasingly being exacerbated by the emergence of drug resistance to most of the available antimalarials, necessitating search for novel drugs. A recent rational approach of antimalarial drug design characterized as "covalent bitherapy" involves linking two molecules with individual intrinsic activity into a single agent, thus packaging dual-activity into a single hybrid molecule. Current research in this field seems to endorse hybrid molecules as the next-generation antimalarial drugs. If the selective toxicity of hybrid prodrugs can be demonstrated in vivo with good bioavailability at the target site in the parasite, it would offer various advantages including dosage compliance, minimized toxicity, ability to design better drug combinations, and cheaper preclinical evaluation while achieving the ultimate object of delaying or circumventing the development of resistance. This review is focused on several hybrid molecules that have been developed, with particular emphasis on those deemed to have high potential for development for clinical use. Drug Dev Res 71: 20-32, 2010. © 2009 Wiley-Liss, Inc.

摘要

疟疾是一种影响全球近40%人口的疾病,化学疗法仍然是其控制策略的主要手段。大多数现有抗疟药物耐药性的出现日益加剧了全球疟疾形势,因此有必要寻找新型药物。最近一种被称为“共价双疗法”的抗疟药物设计合理方法,是将两个具有各自内在活性的分子连接成一个单一药剂,从而将双重活性包装到一个单一的杂合分子中。该领域目前的研究似乎支持杂合分子作为下一代抗疟药物。如果杂合前药的选择性毒性能够在体内得到证实,且在寄生虫的靶位点具有良好的生物利用度,那么它将具有多种优势,包括剂量依从性、毒性最小化、能够设计出更好的药物组合以及更便宜的临床前评估,同时实现延迟或规避耐药性发展的最终目标。本综述聚焦于已开发的几种杂合分子,特别强调那些被认为具有很高临床开发潜力的分子。药物研发研究71: 20 - 32, 2010。© 2009威利 - 利斯公司。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/29c1/3049227/90d6ae298103/ddr0071-0020-f1.jpg

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