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The significance of GlgE as a new target for tuberculosis.

机译:GlgE作为结核病新靶标的意义。

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Largely neglected by the industrialized world for decades, tuberculosis (TB), caused by the bacterium Mycobacterium tuberculosis, has made a fulminant return to the public health agenda as a major global health threat. The worsening of the TB pandemic is driven by the rapid emergence of multidrug-resistant and extensively drug-resistant M. tuberculosis strains, which are virtually untreatable with current chemotherapies. The search for new strategies to combat such resistant strains is of paramount importance for control of the TB pandemic. In searching for new vulnerable processes in M. tuberculosis to enable the rational design of more efficient anti-TB chemotherapy, a novel class of antimycobacterial drug targets has recently been discovered; it is represented by GlgE, an essential maltosyltransferase that elongates linear alpha-glucans as part of a synthetic lethal biosynthetic pathway. Inactivation of GlgE causes accumulation of a toxic phosphosugar intermediate, maltose 1-phosphate, which drives the bacilli into a suicidal self-poisoning cycle that elicits a complex stress profile, eventually resulting in DNA damage and death of M. tuberculosis. GlgE combines many favorable properties that make it a highly attractive novel drug target for chemotherapy of TB.
机译:几十年来,工业化世界一直忽略结核病,由结核分枝杆菌引起的结核病已成为重大的全球健康威胁,重返公共卫生议程。结核病大流行的恶化是由耐多药和广泛耐药的结核分枝杆菌菌株的快速出现所驱动的,而这实际上是目前化学疗法无法治愈的。寻找新的策略来抵抗这种耐药菌株对于控制结核病大流行至关重要。在寻找结核分枝杆菌的新的脆弱过程以合理设计更有效的抗结核化疗药物时,最近发现了一类新型的抗分枝杆菌药物靶标。它由GlgE代表,GlgE是一种必需的麦芽糖基转移酶,可延长线性α-葡聚糖,作为合成致死生物合成途径的一部分。 GlgE的失活会导致有毒的磷酸糖中间体1麦芽糖1磷酸的积累,从而将细菌驱动进入自杀性自中毒循环,引发复杂的应激反应,最终导致DNA损伤和结核分枝杆菌的死亡。 GlgE结合了许多有利的特性,使其成为结核病化疗的高度有吸引力的新型药物靶标。

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