非洲锥虫的糖酵解:靶向酶及其亚细胞区室用于治疗发展。

Molecular biology international Pub Date : 2011-01-01 Epub Date: 2011-04-11 DOI:10.4061/2011/123702
April F Coley, Heidi C Dodson, Meredith T Morris, James C Morris
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引用次数: 33

摘要

引起人类非洲锥虫病的非洲锥虫亚种布鲁氏锥虫由采采蝇传播,其传播必需的生命周期阶段发生在昆虫媒介和人类宿主中。在感染人类宿主期间,寄生虫仅限于利用宿主糖的糖酵解来生产ATP。这种对葡萄糖分解的依赖为潜在的治疗开发提供了一系列靶点,其中许多靶点已被探索并通过实验验证为治疗靶点。这些包括直接参与葡萄糖代谢的酶(例如,锥虫己糖激酶),以及发育和维持必需的亚细胞区室所需的细胞成分,这些亚细胞区室容纳了该途径的主要部分,糖体。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Glycolysis in the african trypanosome: targeting enzymes and their subcellular compartments for therapeutic development.

Glycolysis in the african trypanosome: targeting enzymes and their subcellular compartments for therapeutic development.

Glycolysis in the african trypanosome: targeting enzymes and their subcellular compartments for therapeutic development.

Glycolysis in the african trypanosome: targeting enzymes and their subcellular compartments for therapeutic development.

Subspecies of the African trypanosome, Trypanosoma brucei, which cause human African trypanosomiasis, are transmitted by the tsetse fly, with transmission-essential lifecycle stages occurring in both the insect vector and human host. During infection of the human host, the parasite is limited to using glycolysis of host sugar for ATP production. This dependence on glucose breakdown presents a series of targets for potential therapeutic development, many of which have been explored and validated as therapeutic targets experimentally. These include enzymes directly involved in glucose metabolism (e.g., the trypanosome hexokinases), as well as cellular components required for development and maintenance of the essential subcellular compartments that house the major part of the pathway, the glycosomes.

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