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首页> 外文期刊>MBio >A New Family of Capsule Polymerases Generates Teichoic Acid-Like Capsule Polymers in Gram-Negative Pathogens
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A New Family of Capsule Polymerases Generates Teichoic Acid-Like Capsule Polymers in Gram-Negative Pathogens

机译:胶囊聚合酶的新家族在革兰氏阴性病原体中产生类似于硫辛酸的胶囊聚合物

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ABSTRACT Group 2 capsule polymers represent crucial virulence factors of Gram-negative pathogenic bacteria. They are synthesized by enzymes called capsule polymerases. In this report, we describe a new family of polymerases that combine glycosyltransferase and hexose- and polyol-phosphate transferase activity to generate complex poly(oligosaccharide phosphate) and poly(glycosylpolyol phosphate) polymers, the latter of which display similarity to wall teichoic acid (WTA), a cell wall component of Gram-positive bacteria. Using modeling and multiple-sequence alignment, we showed homology between the predicted polymerase domains and WTA type I biosynthesis enzymes, creating a link between Gram-negative and Gram-positive cell wall biosynthesis processes. The polymerases of the new family are highly abundant and found in a variety of capsule-expressing pathogens such as Neisseria meningitidis , Actinobacillus pleuropneumoniae , Haemophilus influenzae , Bibersteinia trehalosi , and Escherichia coli with both human and animal hosts. Five representative candidates were purified, their activities were confirmed using nuclear magnetic resonance (NMR) spectroscopy, and their predicted folds were validated by site-directed mutagenesis. IMPORTANCE Bacterial capsules play an important role in the interaction between a pathogen and the immune system of its host. During the last decade, capsule polymerases have become attractive tools for the production of capsule polymers applied as antigens in glycoconjugate vaccine formulations. Conventional production of glycoconjugate vaccines requires the cultivation of the pathogen and thus the highest biosafety standards, leading to tremendous costs. With regard to animal husbandry, where vaccines could avoid the extensive use of antibiotics, conventional production is not sufficiently cost-effective. In contrast, enzymatic synthesis of capsule polymers is pathogen-free and fast, offers high stereo- and regioselectivity, and works with high efficacy. The new capsule polymerase family described here vastly increases the toolbox of enzymes available for biotechnology purposes. Representatives are abundantly found in human pathogens but also in animal pathogens, paving the way for the exploitation of polymerases for the development of a new generation of vaccines for animal husbandry.
机译:抽象的第2组胶囊聚合物代表了革兰氏阴性致病菌的关键毒力因子。它们由称为胶囊聚合酶的酶合成。在本报告中,我们描述了一个新的聚合酶家族,其结合了糖基转移酶以及己糖和多元醇磷酸酯转移酶的活性以生成复杂的聚(寡糖磷酸酯)和聚(糖基多元醇磷酸酯)聚合物,后者显示出与壁壁chochochoic acid( WTA),即革兰氏阳性细菌的细胞壁成分。使用建模和多序列比对,我们显示了预测的聚合酶结构域和WTA I型生物合成酶之间的同源性,从而在革兰氏阴性和革兰氏阳性细胞壁生物合成过程之间建立了联系。该新家族的聚合酶高度丰富,并在多种表达胶囊的病原体中发现,例如脑膜炎奈瑟氏球菌,胸膜肺炎放线杆菌,流感嗜血杆菌,海生巴比斯坦菌和人和动物宿主的大肠杆菌。纯化了五个代表性候选物,使用核磁共振(NMR)光谱确认了它们的活性,并通过定点诱变验证了它们的预测折叠。重要信息细菌胶囊在病原体与其宿主免疫系统之间的相互作用中起着重要作用。在过去的十年中,胶囊聚合酶已成为用于生产在糖缀合物疫苗制剂中用作抗原的胶囊聚合物的有吸引力的工具。糖缀合物疫苗的常规生产需要病原体的培养,因此需要最高的生物安全标准,从而导致巨大的成本。关于畜牧业,疫苗可以避免广泛使用抗生素,常规生产的成本效益不足。相反,胶囊聚合物的酶促合成是无病原体且快速的,具有高的立体选择性和区域选择性,并且具有很高的功效。这里描述的新型胶囊聚合酶家族极大地增加了可用于生物技术目的的酶的工具箱。在人类病原体和动物病原体中都发现了很多代表,这为开发用于畜牧业的新一代疫苗的聚合酶的开发铺平了道路。

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