Ⅱ类囊膜病毒膜融合的分子机制
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高等学校全国优秀博士学位论文作者专项资金(200769), 中国农业大学科研启动基金资助项目(2004009).


Molecular Mechanism of Class II Enveloped Viruses Membrane Fusion
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This work was supported by grants from Foundation for the Author of National Excellent Doctoral Dissertation of PR China (FANEDD, 200769) and The Foundation of China Agricultural University (2004009).

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    摘要:

    病毒囊膜与宿主细胞膜的膜融合是囊膜病毒入侵的重要过程,病毒囊膜融合糖蛋白的一系列结构变化引发此过程. 综述了Ⅱ类囊膜病毒、弹状病毒及疱疹病毒融合蛋白结构与功能研究的最新进展,介绍了软件分析并定位融合蛋白功能区域的方法. Ⅱ类病毒与Ⅰ类病毒融合蛋白的融合前结构不同,但融合后结构 (发夹三聚体结构) 相似. 弹状病毒与疱疹病毒的融合蛋白集合了Ⅰ/Ⅱ类融合蛋白的某些特征,但其结构变化及融合过程各不相同,被归为新型融合蛋白. 上述研究为基础设计的以病毒融合过程为靶标的抑制子,可为抗病毒新药的研制提供新思路.

    Abstract:

    Entry of enveloped viruses into host cells requires fusion of the viral envelope with a cellular membrane. This step is mediated by viral glycoproteins that undergo a dramatic conformational change. Recent advances in structure and function of the fusion proteins of the class Ⅱ viruses, Rhabdoviruses and Herpesviruses were described. Proteomics computational analyses to locate the functional domain of fusion protein were introduced. The fusion proteins of class Ⅱ and class Ⅰ viruses differ radically in their initial structures but refold toward similar final conformation (trimer of hairpin). The Rhabdoviruses and Herpesviruses have a novel fold combining features of fusion proteins from class Ⅰ and class Ⅱ. The fusion proteins of these viruses have a different conformation change and mediate a different fusion process, therefore, the proteins belong to a novel class of fusion proteins. The potent inhibitor of virus entry should be new strategies for developing antiviral drugs.

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王晓佳,汪 明.Ⅱ类囊膜病毒膜融合的分子机制[J].生物化学与生物物理进展,2007,34(7):682-686

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  • 收稿日期:2006-10-11
  • 最后修改日期:2007-01-14
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  • 在线发布日期: 2007-04-06
  • 出版日期: 2007-07-20