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睡眠嗜血杆菌 IbpA Fic 细胞毒素在牛、羊和野牛的疾病株和大多数携带株中保守。

Histophilus somni IbpA Fic cytotoxin is conserved in disease strains and most carrier strains from cattle, sheep and bison.

机构信息

Department of Pathology, University of California, San Diego, CA 92103, USA.

出版信息

Vet Microbiol. 2011 Apr 21;149(1-2):177-85. doi: 10.1016/j.vetmic.2010.10.012. Epub 2010 Nov 4.

DOI:10.1016/j.vetmic.2010.10.012
PMID:21112704
Abstract

Histophilus somni causes bovine pneumonia, septicemia, myocarditis, thrombotic meningoencephalitis and arthritis, as well as a genital or upper respiratory carrier state in normal animals. However, differences in virulence factors among strains are not well studied. The surface and secreted immunoglobulin binding protein A (IbpA) Fic motif of H. somni causes bovine alveolar type 2 (BAT2) cells to retract, allowing virulent bacteria to cross the alveolar monolayer. Because H. somni IbpA is an important virulence factor, its presence was evaluated in different strains from cattle, sheep and bison to define whether there are syndrome specific markers and whether antigenic/molecular/functional conservation occurs. A few preputial carrier strains lacked IbpA by Western blotting but all other tested disease or carrier strains were IbpA positive. These positive strains had either both IbpA DR1/Fic and IbpA DR2/Fic or only IbpA DR2/Fic by PCR. IbpA Fic mediated cytotoxicity for BAT2 cells and sequence analysis of IbpA DR2/Fic from selected strains revealed conservation of sequence and function in disease and IbpA positive carrier strains. Passive protection of mice against H. somni septicemia with antibody to IbpA DR2/Fic, along with previous data, indicates that the IbpA DR1/Fic and/or DR2/Fic domains are candidate vaccine antigens for protection against many strains of H. somni. Since IbpA DR2/Fic is conserved in most carrier strains, they may be virulent if introduced to susceptible animals at susceptible sites. Conservation of the protective IbpA antigen in all disease isolates tested is encouraging for development of protective vaccines and diagnostic assays.

摘要

唾液支原体引起牛肺炎、败血症、心肌炎、血栓性脑膜脑炎和关节炎,以及正常动物的生殖道或上呼吸道携带状态。然而,不同菌株的毒力因子差异尚未得到充分研究。唾液支原体的表面和分泌免疫球蛋白结合蛋白 A(IbpA)Fic 基序导致牛肺泡 II 型(BAT2)细胞回缩,使毒力细菌能够穿过肺泡单层。由于 H. somni IbpA 是一种重要的毒力因子,因此评估了来自牛、绵羊和野牛的不同菌株中 IbpA 的存在情况,以确定是否存在特定综合征的标志物,以及是否存在抗原/分子/功能保守性。一些包皮携带株通过 Western blot 检测缺乏 IbpA,但所有其他测试的疾病或携带株均为 IbpA 阳性。这些阳性株通过 PCR 要么同时具有 IbpA DR1/Fic 和 IbpA DR2/Fic,要么只有 IbpA DR2/Fic。IbpA Fic 介导的 BAT2 细胞细胞毒性和从选定菌株中 IbpA DR2/Fic 的序列分析表明,在疾病和 IbpA 阳性携带株中,序列和功能具有保守性。用针对 IbpA DR2/Fic 的抗体对小鼠进行 H. somni 败血症的被动保护,以及以前的数据表明,IbpA DR1/Fic 和/或 DR2/Fic 结构域是针对许多 H. somni 菌株的保护性疫苗抗原的候选物。由于 IbpA DR2/Fic 在大多数携带株中保守,因此如果将其引入易感动物的易感部位,它们可能具有毒力。在所有测试的疾病分离株中都保守的保护性 IbpA 抗原令人鼓舞地为保护性疫苗和诊断检测的开发提供了支持。

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