Park Bo R, Zielke Ryszard A, Wierzbicki Igor H, Mitchell Kristie C, Withey Jeffrey H, Sikora Aleksandra E
Department of Pharmaceutical Sciences, College of Pharmacy, Oregon State University, Corvallis, Oregon, USA.
Department of Immunology and Microbiology, Wayne State University School of Medicine, Detroit, Michigan, USA.
J Bacteriol. 2015 Mar;197(6):1051-64. doi: 10.1128/JB.02329-14. Epub 2015 Jan 5.
Vibrio cholerae is autochthonous to various aquatic niches and is the etiological agent of the life-threatening diarrheal disease cholera. The persistence of V. cholerae in natural habitats is a crucial factor in the epidemiology of cholera. In contrast to the well-studied V. cholerae-chitin connection, scarce information is available about the factors employed by the bacteria for the interaction with collagens. Collagens might serve as biologically relevant substrates, because they are the most abundant protein constituents of metazoan tissues and V. cholerae has been identified in association with invertebrate and vertebrate marine animals, as well as in a benthic zone of the ocean where organic matter, including collagens, accumulates. Here, we describe the characterization of the V. cholerae putative collagenase, VchC, encoded by open reading frame VC1650 and belonging to the subfamily M9A peptidases. Our studies demonstrate that VchC is an extracellular collagenase degrading native type I collagen of fish and mammalian origin. Alteration of the predicted catalytic residues coordinating zinc ions completely abolished the protein enzymatic activity but did not affect the translocation of the protease by the type II secretion pathway into the extracellular milieu. We also show that the protease undergoes a maturation process with the aid of a secreted factor(s). Finally, we propose that V. cholerae is a collagenovorous bacterium, as it is able to utilize collagen as a sole nutrient source. This study initiates new lines of investigations aiming to uncover the structural and functional components of the V. cholerae collagen utilization program.
霍乱弧菌是多种水生生态位中的本地菌种,是危及生命的腹泻病霍乱的病原体。霍乱弧菌在自然栖息地中的持久性是霍乱流行病学中的一个关键因素。与已被充分研究的霍乱弧菌 - 几丁质联系不同,关于该细菌与胶原蛋白相互作用所利用的因素的信息却很少。胶原蛋白可能作为具有生物学相关性的底物,因为它们是后生动物组织中最丰富的蛋白质成分,并且霍乱弧菌已被发现与无脊椎动物和脊椎动物海洋动物有关,以及在包括胶原蛋白在内的有机物积累的海洋底栖区域中存在。在此,我们描述了由开放阅读框VC1650编码且属于M9A肽酶亚家族的霍乱弧菌假定胶原酶VchC的特性。我们的研究表明,VchC是一种细胞外胶原酶,可降解鱼类和哺乳动物来源的天然I型胶原蛋白。协调锌离子的预测催化残基的改变完全消除了该蛋白质的酶活性,但不影响蛋白酶通过II型分泌途径转运到细胞外环境中。我们还表明,该蛋白酶在一种分泌因子的帮助下经历成熟过程。最后,我们提出霍乱弧菌是一种噬胶原细菌,因为它能够将胶原蛋白作为唯一的营养来源。这项研究开启了旨在揭示霍乱弧菌胶原利用程序的结构和功能成分的新研究方向。