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2
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Identification of a carbohydrate recognition domain in filamentous hemagglutinin from Bordetella pertussis.百日咳博德特氏菌丝状血凝素中碳水化合物识别结构域的鉴定
Infect Immun. 1993 Jul;61(7):2780-5. doi: 10.1128/iai.61.7.2780-2785.1993.
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Molecular characterization of an operon required for pertussis toxin secretion.百日咳毒素分泌所需操纵子的分子特征分析。
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Inhibition of Bordetella pertussis filamentous hemagglutinin-mediated cell adherence with monoclonal antibodies.用单克隆抗体抑制百日咳博德特氏菌丝状血凝素介导的细胞黏附
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The filamentous haemagglutinin, a multifaceted adhesion produced by virulent Bordetella spp.丝状血凝素,一种由致病性博德特氏菌属产生的多面黏附素
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Mutational analysis of the Bordetella pertussis fim/fha gene cluster: identification of a gene with sequence similarities to haemolysin accessory genes involved in export of FHA.百日咳博德特氏菌fim/fha基因簇的突变分析:鉴定出一个与参与丝状血凝素(FHA)输出的溶血素辅助基因具有序列相似性的基因。
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Heparin-inhibitable lectin activity of the filamentous hemagglutinin adhesin of Bordetella pertussis.百日咳博德特氏菌丝状血凝素黏附素的肝素抑制性凝集素活性
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The complete general secretory pathway in gram-negative bacteria.革兰氏阴性菌中的完整通用分泌途径。
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Individual chaperones required for Yop secretion by Yersinia.耶尔森氏菌分泌Yop所需的单个分子伴侣。
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百日咳博德特氏菌丝状血凝素生物合成中N端和C端前体结构域的不同作用

Distinct roles of the N-terminal and C-terminal precursor domains in the biogenesis of the Bordetella pertussis filamentous hemagglutinin.

作者信息

Renauld-Mongénie G, Cornette J, Mielcarek N, Menozzi F D, Locht C

机构信息

Centre d'Immunologie et de Biologie Parasitaire, INSERM 167, Institut Pasteur, Lille, France.

出版信息

J Bacteriol. 1996 Feb;178(4):1053-60. doi: 10.1128/jb.178.4.1053-1060.1996.

DOI:10.1128/jb.178.4.1053-1060.1996
PMID:8576038
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC177765/
Abstract

The 220-kDa Bordetella pertussis filamentous hemagglutinin (FHA) is the major exported protein found in culture supernatants. The structural gene of FHA has a coding potential for a 367-kDa protein, and the mature form constitutes the N-terminal 60% of the 367-kDa precursor. The C-terminal domain of the precursor was found to be important for the high-level secretion of full-length FHA but not of truncated analogs (80 kDa or less). The secretion of full-length and truncated FHA polypeptides requires the presence of the approximately 100-amino-acid N-terminal domain and the outer membrane protein FhaC, homologous to the N-terminal domains of the Serratia marcescens and Proteus mirabilis hemolysins and their accessory proteins, respectively. By analogy to these hemolysins, it is likely that the N-terminal domain of the FHA precursor interacts, directly or indirectly, with the accessory protein during FHA biogenesis. However, immunogenicity and antigenicity studies suggest that the N-terminal domain of FHA is masked by its C-terminal domain and therefore should not be available for its interactions with FhaC. These observations suggest a model in which the C-terminal domain of the FHA precursor may play a role as an intramolecular chaperone to prevent premature folding of the protein. Both heparin binding and hemagglutination are expressed by the N-terminal half of FHA, indicating that this domain contains important functional regions of the molecule.

摘要

220 kDa的百日咳博德特氏菌丝状血凝素(FHA)是培养上清液中发现的主要分泌蛋白。FHA的结构基因编码一种367 kDa的蛋白,成熟形式占367 kDa前体N端的60%。发现前体的C端结构域对于全长FHA的高水平分泌很重要,但对于截短类似物(80 kDa或更小)则不重要。全长和截短的FHA多肽的分泌需要存在大约100个氨基酸的N端结构域和外膜蛋白FhaC,它们分别与粘质沙雷氏菌和奇异变形杆菌溶血素及其辅助蛋白的N端结构域同源。类似于这些溶血素,在FHA生物合成过程中,FHA前体的N端结构域可能直接或间接与辅助蛋白相互作用。然而,免疫原性和抗原性研究表明,FHA的N端结构域被其C端结构域掩盖,因此不应可用于与FhaC的相互作用。这些观察结果提示了一种模型,其中FHA前体的C端结构域可能作为分子内伴侣发挥作用,以防止蛋白质过早折叠。肝素结合和血凝作用均由FHA的N端一半表现出来,表明该结构域包含分子的重要功能区。