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自我与非自我核糖核酸的辨别

Discrimination of Self and Non-Self Ribonucleic Acids.

作者信息

Gebhardt Anna, Laudenbach Beatrice T, Pichlmair Andreas

机构信息

Innate Immunity Laboratory, Max-Planck Institute of Biochemistry , Munich, Germany .

出版信息

J Interferon Cytokine Res. 2017 May;37(5):184-197. doi: 10.1089/jir.2016.0092.

Abstract

Most virus infections are controlled through the innate and adaptive immune system. A surprisingly limited number of so-called pattern recognition receptors (PRRs) have the ability to sense a large variety of virus infections. The reason for the broad activity of PRRs lies in the ability to recognize viral nucleic acids. These nucleic acids lack signatures that are present in cytoplasmic cellular nucleic acids and thereby marking them as pathogen-derived. Accumulating evidence suggests that these signatures, which are predominantly sensed by a class of PRRs called retinoic acid-inducible gene I (RIG-I)-like receptors and other proteins, are not unique to viruses but rather resemble immature forms of cellular ribonucleic acids generated by cellular polymerases. RIG-I-like receptors, and other cellular antiviral proteins, may therefore have mainly evolved to sense nonprocessed nucleic acids typically generated by primitive organisms and pathogens. This capability has not only implications on induction of antiviral immunity but also on the function of cellular proteins to handle self-derived RNA with stimulatory potential.

摘要

大多数病毒感染是通过先天免疫系统和适应性免疫系统来控制的。数量惊人有限的所谓模式识别受体(PRR)能够感知多种病毒感染。PRR具有广泛活性的原因在于其识别病毒核酸的能力。这些核酸缺乏细胞质细胞核酸中存在的特征,从而将它们标记为病原体来源。越来越多的证据表明,这些主要由一类称为视黄酸诱导基因I(RIG-I)样受体和其他蛋白质感知的特征并非病毒所特有,而是类似于细胞聚合酶产生的细胞核糖核酸的不成熟形式。因此,RIG-I样受体和其他细胞抗病毒蛋白可能主要进化为感知通常由原始生物和病原体产生的未加工核酸。这种能力不仅对抗病毒免疫的诱导有影响,而且对处理具有刺激潜力的自身来源RNA的细胞蛋白功能也有影响。

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Discrimination of Self and Non-Self Ribonucleic Acids.自我与非自我核糖核酸的辨别
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