结核分枝杆菌的糖基因组学

A. Gupta, Amit Singh, Sarman Singh
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引用次数: 8

摘要

糖原是几乎所有生物体的重要能量储存。它是一种由数千个葡萄糖单位组成的α键聚合物。在细菌中,它通常是在生长培养基中碳离子过量时合成的,它的合成有助于细菌在这种营养条件下的生存。结核分枝杆菌(M. tuberculosis)在活性氧和氮中间体、低pH、营养物质和其他重要元素饥饿等不利条件下,在宿主体内积累糖原以维持其生存。糖原在结核分枝杆菌的发病过程中也起着非常重要的作用。糖原的生物合成是由糖基转移酶介导的,糖基转移酶可分为两科;糖原转移酶(GT) 3和糖基转移酶GT 5。细菌糖原代谢的调控机制复杂,涉及多种合成酶,如糖原合成酶a (glgA)、糖原分支酶(glgB)和催化酶(glgC)。另一种酶称为糖原磷酸化酶(glgP),从糖原分子的非还原端去除额外的葡萄糖单位。近年来,一些研究人员已经认识到糖原在分枝杆菌发病中的作用。存在于细胞壁的海藻糖-二mycolate (TDM)和海藻糖-单omycolate (TMM)确实是分枝杆菌mycolic酸的前体,在其侵袭和发病中起重要作用。本文综述了结核分枝杆菌糖原合成的各种循环和机制及其在发病机制中的作用。
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Glycogenomics of Mycobacterium tuberculosis
Glycogen is an important energy store of almost all living organisms. It is an alpha linked polymer comprised of thousands of glucose units. In bacteria it is usually synthesized when carbon ions are in excess in the growth medium and its synthesis helps for the survival of the bacteria under such nutritional conditions. Mycobacterium tuberculosis (M. tuberculosis), accumulates glycogen during the adverse condition such as reactive oxygen and nitrogen intermediates, low pH, nutrients and other vital element starvation for their survival in the host. Glycogen also plays a very important role in the pathogenesis of M. tuberculosis. The biosynthesis of glycogens is mediated by glycosyltransferases enzyme which can be divided into two families; glycogen transferase (GT) 3 and glycosyltransferases GT 5. Regulation of glycogen metabolism in bacteria involves a complex mechanism, involving several synthase enzymes such as glycogen synthase A (glgA), glycogen branching enzyme (glgB), and catalytic enzyme (glgC). Another enzyme known as glycogen phosphorylase (glgP), removes extra units of glucose from the non- reducing ends of the glycogen molecule. Several workers have recognized role of glycogen in Mycobacterial pathogenesis, in the recent years. Trehalose-dimycolate (TDM) and trehalose-monomycolate (TMM) present in the cell wall are indeed a precursor of mycolic acid of Mycobacteria, which plays an important role in its invasion and pathogenesis. This review focuses on various cycles and mechanisms involved in the glycogen synthesis in M. tuberculosis and its role in pathogenesis.
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