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Autophagy receptor CCDC50 tunes the STING-mediated interferon response in viral infections and autoimmune diseases

机译:自噬受体CCDC50在病毒感染和自身免疫疾病中调整刺痛介导的干扰素反应

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摘要

DNA sensing and timely activation of interferon(IFN)-mediated innate immunity are crucial for the defense against DNA virus infections and the clearance of abnormal cells.However,overactivation of immune responses may lead to tissue damage and autoimmune diseases;therefore,these processes must be intricately regulated.STING is the key adaptor protein,which is activated by cyclic GMP-AMP,the second messenger derived from cGAS-mediated DNA sensing.Here,we report that CCDC50,a newly identified autophagy receptor,tunes STING-directed type I IFN signaling activity by delivering K63-polyubiquitinated STING to autolysosomes for degradation.Knockout of CCDC50 significantly increases herpes simplex virus 1(HSV-1)-or DNA ligand-induced production of type I IFN and proinflammatory cytokines.Ccdc50-deficient mice show increased production of IFN,decreased viral replication,reduced cell infiltration,and improved survival rates compared with their wild-type littermates when challenged with HSV-1.Remarkably,the expression of CCDC50 is downregulated in systemic lupus erythematosus(SLE),a chronic autoimmune disease.CCDC50 levels are negatively correlated with IFN signaling pathway activation and disease severity in human SLE patients.CCDC50 deficiency potentiates the cGAS-STING-mediated immune response triggered by SLE serum.Thus,our findings reveal the critical role of CCDC50 in the immune regulation of viral infections and autoimmune diseases and provide insights into the therapeutic implications of CCDC50 manipulation.

著录项

  • 来源
    《细胞与分子免疫学:英文版》 |2021年第10期|P.2358-2371|共14页
  • 作者单位

    MOE Key Laboratory of Tropical Disease Control Centre for Infection and Immunity Study(CIIS) School of Medicine Sun Yat-sen University Shenzhen China;

    MOE Key Laboratory of Tropical Disease Control Centre for Infection and Immunity Study(CIIS) School of Medicine Sun Yat-sen University Shenzhen China;

    MOE Key Laboratory of Tropical Disease Control Centre for Infection and Immunity Study(CIIS) School of Medicine Sun Yat-sen University Shenzhen China;

    MOE Key Laboratory of Tropical Disease Control Centre for Infection and Immunity Study(CIIS) School of Medicine Sun Yat-sen University Shenzhen China;

    MOE Key Laboratory of Tropical Disease Control Centre for Infection and Immunity Study(CIIS) School of Medicine Sun Yat-sen University Shenzhen China;

    The Center for Applied Genomics Abramson Research Center The Children''s Hospital of Philadelphia Philadelphia PA USA;

    MOE Key Laboratory of Tropical Disease Control Centre for Infection and Immunity Study(CIIS) School of Medicine Sun Yat-sen University Shenzhen China;

    Division of Rheumatology Third Affiliated Hospital of Sun Yat-sen University Guangzhou China;

    MOE Key Laboratory of Tropical Disease Control Centre for Infection and Immunity Study(CIIS) School of Medicine Sun Yat-sen University Shenzhen China;

    MOE Key Laboratory of Tropical Disease Control Centre for Infection and Immunity Study(CIIS) School of Medicine Sun Yat-sen University Shenzhen China;

    MOE Key Laboratory of Tropical Disease Control Centre for Infection and Immunity Study(CIIS) School of Medicine Sun Yat-sen University Shenzhen China;

    Division of Rheumatology Third Affiliated Hospital of Sun Yat-sen University Guangzhou China;

    MOE Key Laboratory of Tropical Disease Control Centre for Infection and Immunity Study(CIIS) School of Medicine Sun Yat-sen University Shenzhen China;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 chi
  • 中图分类 全身性疾病;
  • 关键词

    CCDC50; STING; Type I IFN; HSV-1; Autophagy; Autoimmune diseases;

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