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Intracellular antibody-bound pathogens stimulate immune signaling via the Fc receptor TRIM21

机译:细胞内抗体结合病原体通过Fc受体TRIM21刺激免疫信号

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During pathogen infection, antibodies can be carried into the infected cell, where they are detected by the ubiquitously expressed cytosolic antibody receptor TRIM21. Here we found that recognition of intracellular antibodies by TRIM21 activated immune signaling. TRIM21 catalyzed the formation of Lys63 (K63)-linked ubiquitin chains and stimulated the transcription factor pathways of NF-??B, AP-1, IRF3, IRF5 and IRF7. Activation resulted in the production of proinflammatory cytokines, modulation of natural killer stress ligands and induction of an antiviral state. Intracellular antibody signaling was abrogated by genetic deletion of TRIM21 and was restored by ectopic expression of TRIM21. The sensing of antibodies by TRIM21 was stimulated after infection by DNA or RNA nonenveloped viruses or intracellular bacteria. Thus, the antibody-TRIM21 detection system provides potent, comprehensive activation of the innate immune system independently of known pattern-recognition receptors. ? 2013 Nature America, Inc. All rights reserved.
机译:在病原体感染期间,抗体可以被携带到被感染的细胞中,在那里被普遍表达的胞质抗体受体TRIM21检测到。在这里,我们发现TRIM21对细胞内抗体的识别激活了免疫信号传导。 TRIM21催化Lys63(K63)连接的泛素链的形成,并刺激NF-κB,AP-1,IRF3,IRF5和IRF7的转录因子途径。活化导致促炎细胞因子的产生,天然杀伤应激配体的调节和抗病毒状态的诱导。细胞内抗体信号转导被TRIM21的基因缺失所废除,并被TRIM21的异位表达所恢复。 DNA或RNA非包膜病毒或细胞内细菌感染后,刺激了TRIM21对抗体的感应。因此,抗体-TRIM21检测系统可独立于已知的模式识别受体,有效地,全面地激活先天免疫系统。 ? 2013 Nature America,Inc.保留所有权利。

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