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结构杂交是否为抗疟药物发现研究带来了新的维度?

Is structural hybridization invoking new dimensions for antimalarial drug discovery research?

作者信息

Sharma Bhawana, Agarwal Alka, Awasthi Satish Kumar

机构信息

Chemical Biology Laboratory, Department of Chemistry, University of Delhi Delhi-110007 India

Department of Medicinal Chemistry, Institute of Medical Sciences, Banaras Hindu University Varanasi-221005 Uttar Pradesh India

出版信息

RSC Med Chem. 2023 May 4;14(7):1227-1253. doi: 10.1039/d3md00083d. eCollection 2023 Jul 20.

Abstract

Despite effective prevention methods, malaria is a devastating, persistent infection caused by protozoal parasites that result in nearly half a million fatalities annually. Any progress made thus far in the eradication of the disease is jeopardized by the expansion of malaria parasites that have evolved to become resistant to a wide range of drugs, including first-line therapy. To surmount this significant obstacle, it is necessary to develop newly synthesized drugs with multiple modes of action that may have a novel target in various stages of parasite development and this is made possible by the hybridization concept. Hybridization is the combination of at least two diverse pharmacophore units with some linkers bringing about a single molecule with a diverse mode of action. It intensifies a drug's physiological and chemical characteristics, such as absorption, cellular target contact, metabolism, excretion, distribution, and toxicity. This review article outlines the currently published most potent hybrid drugs against the species.

摘要

尽管有有效的预防方法,但疟疾是由原生动物寄生虫引起的一种毁灭性的持续性感染,每年导致近50万人死亡。迄今为止,在根除该疾病方面取得的任何进展都受到疟原虫扩散的威胁,这些疟原虫已经进化到对包括一线治疗在内的多种药物产生抗性。为了克服这一重大障碍,有必要开发具有多种作用模式的新合成药物,这些药物可能在寄生虫发育的各个阶段具有新的靶点,而杂交概念使这成为可能。杂交是至少两个不同的药效团单元与一些连接基的组合,从而产生具有多种作用模式的单个分子。它增强了药物的生理和化学特性,如吸收、细胞靶点接触、代谢、排泄、分布和毒性。这篇综述文章概述了目前已发表的针对该物种最有效的杂交药物。

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