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结核病的新方法——基于与巨噬细胞中Toll样受体相关药物靶点的新型药物。

New approaches to tuberculosis--novel drugs based on drug targets related to toll-like receptors in macrophages.

作者信息

Tomioka Haruaki

机构信息

Department of Microbiology and Immunology, Shimane University School of Medicine, Izumo, Shimane 693-8501, Japan.

出版信息

Curr Pharm Des. 2014;20(27):4404-17. doi: 10.2174/1381612819666131118163331.

Abstract

Tuberculosis (TB) is one of the most important health concerns in the world, causing serious levels of morbidity and mortality, particularly in many developing countries. Unfortunately, the development of new anti-TB drugs with superior chemotherapeutic and prophylactic activity has been very slow. Thus, it is urgently necessary to develop novel kinds of antituberculosis drugs that exert their anti-Mycobacterium tuberculosis (MTB) activity through unique drug targets expressed by MTB organisms. At present, the drug targets of most current anti-TB drugs are primarily bacterial metabolic reactions and cell components that are indispensable to the growth and survival of MTB organisms in extracellular milieus, particularly in culture media. To develop novel and unique anti-TB drugs in the future, it is desirable to highlight the drug targets related to the bacterial ability to survive and replicate in host macrophages by escaping from a macrophage's bacterial killing mechanism during infection inside such phagocytes. For this purpose, it is reasonable to focus our research efforts on mycobacterial virulence factors that cross-talk and interfere with signaling pathways of host macrophages, because such virulence factors will provide intracellular milieus favorable to intramacrophage survival and growth of MTB. In this chapter, based on such a viewpoint and strategy, the present status of worldwide research on novel potential drug targets related to Toll-like receptor in the MTB pathogen will be described.

摘要

结核病是全球最重要的健康问题之一,会导致严重的发病率和死亡率,在许多发展中国家尤为如此。不幸的是,具有卓越化疗和预防活性的新型抗结核药物的研发进展非常缓慢。因此,迫切需要开发新型抗结核药物,这些药物通过结核分枝杆菌(MTB)表达的独特药物靶点发挥其抗MTB活性。目前,大多数现有抗结核药物的药物靶点主要是细菌代谢反应和细胞成分,这些对于MTB在细胞外环境(特别是在培养基中)的生长和存活是不可或缺的。为了在未来开发新颖独特的抗结核药物,有必要突出与细菌在宿主巨噬细胞中存活和复制能力相关的药物靶点,即细菌在吞噬细胞内感染期间逃避巨噬细胞杀菌机制的能力。为此,将研究重点集中在与宿主巨噬细胞信号通路相互作用和干扰的分枝杆菌毒力因子上是合理的,因为这些毒力因子将为MTB在巨噬细胞内的存活和生长提供有利的细胞内环境。在本章中,基于这样的观点和策略,将描述全球范围内与MTB病原体中Toll样受体相关的新型潜在药物靶点的研究现状。

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