Breakthroughs in the development of antibiotics, antifungals and antiparasitics targeting the pathogens' respiratory chain.

IF 6.4 2区 生物学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
Jennifer M Sorescu, Martín A González-Montalvo, Ming Yuan, Joseph De Paolo-Boisvert, Corina Diana Ceapă, Rodolfo Garcia-Contreras, Oscar Flores-Herrera, Michael E Shea, Karina Tuz, Oscar X Juárez
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引用次数: 0

Abstract

The aerobic respiratory chain is vital to bacterial and eukaryotic cell energy transformation. Embedded in the mitochondrial inner membrane and the bacterial plasma membrane, the respiratory chain couples sequential redox reactions with ion pumping, thereby generating the motive force that is used to drive ATP synthesis. Due to the essential role of oxidative phosphorylation in cellular life, the electron transport chain proteins, their cofactors, and ATP synthase components serve as a target for antibacterial, antifungal, and antiparasitic drugs. Whether by (1) inhibition of electron flow through transport chain complexes, (2) collapsing of the motive force, (3) competitive inhibition, or (4) blocking proton flow through the catalytic subunits of ATP synthase, small molecules can selectively inhibit bacterial, fungal, and parasitic life while not showing high toxicity in mammalian systems. Because of robust antimicrobial resistance against the traditional mechanisms of microbial control (cell wall integrity, protein synthesis, nucleotide and nucleic acid synthesis, etc.), the study of alternative targets, such as the respiratory chain, is prudent and timely. This review summarizes the current research on small molecule and peptide inhibition of the aerobic respiratory chain complexes, electron flow, and ion translocation in a series of human and plant pathogens.

针对病原体呼吸链的抗生素、抗真菌药和抗寄生虫药研发取得突破。
有氧呼吸链对细菌和真核细胞的能量转化至关重要。呼吸链嵌于线粒体内膜和细菌质膜中,将连续氧化还原反应与离子泵送耦合,从而产生驱动ATP合成的动力。由于氧化磷酸化在细胞生命中的重要作用,电子传递链蛋白及其辅助因子和ATP合酶成分可作为抗菌、抗真菌和抗寄生虫药物的靶标。无论是通过(1)抑制通过传递链复合物的电子流,(2)破坏动力,(3)竞争抑制,还是(4)阻断通过ATP合酶催化亚基的质子流,小分子都可以选择性地抑制细菌、真菌和寄生生命,同时在哺乳动物系统中没有显示出高毒性。由于对微生物控制的传统机制(细胞壁完整性、蛋白质合成、核苷酸和核酸合成等)具有强大的耐药性,因此对呼吸链等替代靶点的研究是谨慎和及时的。本文综述了小分子和多肽在一系列人类和植物病原体中对有氧呼吸链复合物、电子流和离子转运的抑制作用。
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来源期刊
CiteScore
14.90
自引率
0.00%
发文量
6
期刊介绍: As the discipline of biochemistry and molecular biology have greatly advanced in the last quarter century, significant contributions have been made towards the advancement of general medicine, genetics, immunology, developmental biology, and biophysics. Investigators in a wide range of disciplines increasingly require an appreciation of the significance of current biochemical and molecular biology advances while, members of the biochemical and molecular biology community itself seek concise information on advances in areas remote from their own specialties. Critical Reviews in Biochemistry and Molecular Biology believes that well-written review articles prove an effective device for the integration and meaningful comprehension of vast, often contradictory, literature. Review articles also provide an opportunity for creative scholarship by synthesizing known facts, fruitful hypotheses, and new concepts. Accordingly, Critical Reviews in Biochemistry and Molecular Biology publishes high-quality reviews that organize, evaluate, and present the current status of high-impact, current issues in the area of biochemistry and molecular biology. Topics are selected on the advice of an advisory board of outstanding scientists, who also suggest authors of special competence. The topics chosen are sufficiently broad to interest a wide audience of readers, yet focused enough to be within the competence of a single author. Authors are chosen based on their activity in the field and their proven ability to produce a well-written publication.
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