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Nucleic acids and endosomal pattern recognition: how to tell friend from foe?

机译:核酸和内体模式识别:如何对付敌人?

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摘要

The innate immune system has evolved endosomal and cytoplasmic receptors for the detection of viral nucleic acids as sensors for virus infection. Some of these pattern recognition receptors (PRR) detect features of viral nucleic acids that are not found in the host such as long stretches of double-stranded RNA (dsRNA) and uncapped single-stranded RNA (ssRNA) in case of Toll-like receptor (TLR) 3 and RIG-I, respectively. In contrast, TLR7/8 and TLR9 are unable to distinguish between viral and self-nucleic acids on the grounds of distinct molecular patterns. The ability of these endosomal TLR to act as PRR for viral nucleic acids seems to rely solely on the mode of access to the endolysosomal compartment in which recognition takes place. The current dogma states that self-nucleic acids do not enter the TLR-sensing compartment under normal physiological conditions. However, it is still poorly understood how dendritic cells (DC) evade activation by self-nucleic acids, in particular with regard to specific DC subsets, which are specialized in taking up material from dying cells for cross-presentation of cell-associated antigens. In this review we discuss the current understanding of how the immune system distinguishes between foreign and self-nucleic acids and point out some of the key aspects that still require further research and clarification.
机译:先天免疫系统已经进化出内体和细胞质受体,用于检测病毒核酸作为病毒感染的传感器。这些模式识别受体(PRR)中的一些可检测宿主中未发现的病毒核酸特征,例如在Toll样受体的情况下长链的双链RNA(dsRNA)和无盖的单链RNA(ssRNA) (TLR)3和RIG-I。相反,TLR7 / 8和TLR9不能基于不同的分子模式来区分病毒核酸和自身核酸。这些内体TLR充当病毒核酸的PRR的能力似乎仅取决于进入发生识别的内体体区室的方式。当前的教条指出,在正常的生理条件下,自核酸不会进入TLR感应腔。然而,人们仍然很少了解树突状细胞(DC)如何通过自身核酸逃避活化,特别是关于特定的DC亚群,其专门用于从垂死的细胞中摄取物质以交叉呈递与细胞相关的抗原。在这篇综述中,我们讨论了目前对免疫系统如何区分外来核酸和自身核酸的理解,并指出了一些仍需进一步研究和阐明的关键方面。

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