李斯特菌中复杂的泛酸利用途径。
A complex lipoate utilization pathway in Listeria monocytogenes.
机构信息
Department of Microbiology, University of Illinois, Urbana, Illinois 61801, USA.
出版信息
J Biol Chem. 2011 Sep 9;286(36):31447-56. doi: 10.1074/jbc.M111.273607. Epub 2011 Jul 18.
Abstract
Although a complete pathway of lipoic acid metabolism has been established in Escherichia coli, lipoic acid metabolism in other bacteria is more complex and incompletely understood. Listeria monocytogenes has been shown to utilize two lipoate-protein ligases for lipoic acid scavenging, whereas only one of the ligases can function in utilization of host-derived lipoic acid-modified peptides. We report that lipoic acid scavenging requires not only ligation of lipoic acid but also a lipoyl relay pathway in which an amidotransferase transfers lipoyl groups to the enzyme complexes that require the cofactor for activity. In addition, we provide evidence for a new lipoamidase activity that could allow utilization of lipoyl peptides by lipoate-protein ligase. These data support a model of an expanded, three-enzyme pathway for lipoic acid scavenging that seems widespread in the Firmicutes phylum of bacteria.
摘要
尽管在大肠杆菌中已经建立了完整的硫辛酸代谢途径,但其他细菌的硫辛酸代谢更为复杂,且尚未完全了解。已经表明单核细胞增生李斯特菌利用两种脂酰-蛋白连接酶来摄取硫辛酸,而只有一种连接酶可以用于利用宿主来源的硫辛酸修饰肽。我们报告称,硫辛酸的摄取不仅需要硫辛酸的连接,还需要一个脂酰转移酶将脂酰基团转移到需要辅因子才能发挥活性的酶复合物的脂酰传递途径。此外,我们还提供了证据表明存在一种新的脂酰酶活性,这可能允许脂酰-蛋白连接酶利用脂酰肽。这些数据支持了一个扩展的、三酶途径的模型,用于硫辛酸的摄取,该途径似乎在细菌的厚壁菌门中广泛存在。
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