CD317 功能研究进展
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中国博士后基金(2016M602541);广东省省级科技计划项目(2013A022100037);广东省第四批领军人才(粤人才办【2014】1 号);深圳市海外高层次人才创新创业计划团队(1110140040347260);深圳市知识创新计划(JCYJ20140417113430654);深圳市技术创新计划 (JSGG20140701164558078、JSGG20160229202150023)

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Research Progress on CD317 Function
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    摘要:

    CD317(Tetherin,BST-2 或 HM1.24)于 1994 年被发现并命名,是终末分化 B 细胞的特异性表面标志。2008 年首次被鉴定为干扰素诱导型宿主抗病毒因子,此后越来越多的科学家加入到该领域的探索中。经过近十年的研究,目前已经阐述了 CD317 结构、抗病毒及免疫特性等问题,也陆续发现了一些诸如参与肿瘤进展、束缚外泌体释放等新功能,研究热度不减当年。因此,文章对近几年 CD317 功能的研究进展进行一个系统的总结,以期为病毒感染、肿瘤发病以及治疗等方面的理论进步和技术发展提供新 的思路。

    Abstract:

    CD317 (also known as tetherin, BST-2, or HM1.24) was first discovered from a human plasma cell line in 1994 and defined as a novel terminal B-cell-restricted antigen. It was first reported to be a potent interferon-induced host antiviral factor in 2008, and was demonstrated that it inhibited the release of HIV-1 viral particles deficient in the viral membrane protein Vpu. Since that time, numerous reports have been published regarding to the structure, the antiviral activity and immunological properties of this protein. Moreover, some new functions of CD317, such as involvement with tumor development and exosome tetherin, have been found recently. Thus, CD317 function is not just limited to the antiviral field. In this review, the antiviral function, oncobiology and signal transduction of CD317 were summarized, which will enhance the overall knowledge of CD317 function during viral infection and cancer metastasis, possibly leading to unique therapeutic applications for these diseases.

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引文格式
章桂忠,李欣,黄诗然,等. CD317 功能研究进展 [J].集成技术,2017,6(3):15-28

Citing format
ZHANG Guizhong, LI Xin, HUANG Shiran, et al. Research Progress on CD317 Function[J]. Journal of Integration Technology,2017,6(3):15-28

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  • 在线发布日期: 2017-05-22
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