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TRIM21 依赖的细胞内抗体对病毒感染的中和作用。

TRIM21-dependent intracellular antibody neutralization of virus infection.

作者信息

McEwan William A, James Leo C

机构信息

Protein and Nucleic Acid Chemistry Division, Medical Research Council Laboratory of Molecular Biology, Cambridge, United Kingdom.

Protein and Nucleic Acid Chemistry Division, Medical Research Council Laboratory of Molecular Biology, Cambridge, United Kingdom.

出版信息

Prog Mol Biol Transl Sci. 2015;129:167-87. doi: 10.1016/bs.pmbts.2014.10.006. Epub 2014 Dec 12.

DOI:10.1016/bs.pmbts.2014.10.006
PMID:25595804
Abstract

The ability of antibodies to prevent viral infection has long been recognized. In vitro neutralization assays, which take place in the absence of professional immune effector mechanisms, have demonstrated that the process of neutralization can occur by a variety of molecular mechanisms. Most known mechanisms involve the blocking of an event essential for infection, for instance, the steric inhibition of attachment to entry receptors. As such, neutralization is often thought of as a passive process that can occur without the need for host effector machinery. In contrast to this view, it has recently been demonstrated that neutralization can depend on the widely expressed cytosolic Fc binding protein TRIM21. This unique and novel Ig receptor directs the ubiquitin and proteasome-dependent degradation of intracellular antibody-bound viral particles and prevents infection. It has been further demonstrated that detection of cytosolic antibody by TRIM21 activates inflammatory signaling pathways and promotes the production of cytokines and chemokines. Studies in a TRIM21-null mouse demonstrate the importance of these activities: homozygous knockouts suffer fatal viral infection where wild-type mice survive. Though there is much to be learned about the role of TRIM21 in immunity, it is clear that there is a hitherto unappreciated role for antibodies in the intracellular environment.

摘要

抗体预防病毒感染的能力早已得到认可。在缺乏专业免疫效应机制的体外中和试验表明,中和过程可通过多种分子机制发生。大多数已知机制涉及阻断感染所必需的事件,例如,对附着于进入受体的空间位阻抑制。因此,中和作用通常被认为是一个无需宿主效应机制即可发生的被动过程。与这种观点相反,最近有研究表明,中和作用可能依赖于广泛表达的胞质Fc结合蛋白TRIM21。这种独特且新颖的Ig受体会引导泛素和蛋白酶体依赖性的细胞内抗体结合病毒颗粒的降解,并防止感染。进一步的研究表明,TRIM21对胞质抗体的检测会激活炎症信号通路,并促进细胞因子和趋化因子的产生。对TRIM21基因敲除小鼠的研究证明了这些活性的重要性:纯合敲除小鼠会遭受致命的病毒感染,而野生型小鼠则存活下来。尽管关于TRIM21在免疫中的作用仍有许多有待了解之处,但很明显,抗体在细胞内环境中存在迄今未被认识到的作用。

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