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Genetic and antigenic characterization of sigma C protein from avian reovirus

机译:禽呼肠孤病毒sigma C蛋白的遗传和抗原表征

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摘要

Avian reovirus (ARV) causes viral arthritis, tenosynovitis, liver infection and immunosuppression in birds. Live-attenuated and inactivated vaccines for ARV are available, but do not efficiently protect against recent variants. Sigma C, which mediates virus attachment to target cells, is the most variable protein in ARV. Antibodies to this protein neutralize viral infection. The purpose of the present study was to characterize sigma C in isolates of ARV from infected birds, as compared with the vaccine strain. Amino acids 27 to 293 of sigma C from 28 Israeli isolates were compared, classified and analysed using bioinformatics tools. Large variations were found among the isolates, and the vaccine strain was shown to differ from most of the studied strains, which could explain the failure of commonly used vaccinations in protecting birds against ARV infection. Based on sigma C protein sequences from all over the world, ARV can be divided into four groups. Isolates from all groups were found in the field simultaneously, possibly explaining the insufficient protection achieved by the vaccine strain, which is represented in one of the groups. The results point out the need and the difficulty in producing a wide-ranging vaccine. Several conserved regions among all reported ARV sigma C proteins were identified. These peptides were further studied for structural and functional properties, and for antigenic characterization. The results of this study shed light on peptide selection for a broad and efficient vaccine.
机译:禽呼肠孤病毒(ARV)会导致禽类中的病毒性关节炎,腱鞘炎,肝感染和免疫抑制。目前已有用于ARV的减毒活疫苗和灭活疫苗,但不能有效防止新近变异。介导病毒附着于靶细胞的Sigma C是ARV中变化最大的蛋白质。该蛋白质的抗体可中和病毒感染。与疫苗株相比,本研究的目的是鉴定被感染禽类ARV分离物中的sigmaC。使用生物信息学工具对来自28个以色列分离株的Sigma C氨基酸27至293进行了比较,分类和分析。在分离株之间发现了很大的差异,并且该疫苗株被证明与大多数研究的株不同,这可以解释常用疫苗在保护禽类抗ARV感染方面的失败。基于来自世界各地的sigma C蛋白序列,ARV可以分为四类。在现场同时发现了所有组的分离株,这可能解释了其中一种疫苗株对疫苗的保护作用不足。结果指出了生产广泛疫苗的需求和困难。在所有报告的ARV sigma C蛋白中鉴定了几个保守区。进一步研究了这些肽的结构和功能特性以及抗原特性。这项研究的结果为广泛而有效的疫苗的肽选择提供了启示。

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  • 来源
    《Avian Pathology》 |2010年第3期|p.189-199|共11页
  • 作者

    Dana Goldenberg;

  • 作者单位

    Migal—Galilee Technology Center, P.O. Box 831, Kiryat Shmona, 11016, Israel;

    Department of Biotechnology, Tel-Hai Academic College, Israel;

    Bioinformatics Unit, G.S.W. Faculty of Life Sciences, Tel-Aviv University, Tel Aviv, 69978, Israel;

    Northern P;

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