SHIP1 modulates antimalarial immunity by bridging the crosstalk between type I IFN signaling and autophagy-Reference-Cited by-同舟云学术

SHIP1 modulates antimalarial immunity by bridging the crosstalk between type I IFN signaling and autophagy

Published:2023-06-27 Issue: Volume: Page:
ISSN:2150-7511
Container-title:mBio
language:en
Short-container-title:mBio

Author:

Li Hongyu¹^ORCID,Yang Shuai²,Zeng Ke¹,Guo Jiayin¹,Wu Jian³,Jiang Huaji¹⁴,Xie Yingchao¹,Hu Zhiqiang¹,Lu Jiansen¹⁵,Yang Jianwu¹,Su Xin-zhuan³^ORCID,Cui Jun²,Yu Xiao¹⁶^ORCID

Affiliation:

1. Department of Immunology, School of Basic Medical Sciences, Southern Medical University , Guangzhou, Guangdong, China

2. Guangdong Province Key Laboratory of Pharmaceutical Functional Genes, MOE Key Laboratory of Gene Function and Regulation, School of Life Sciences, Sun Yat-sen University , Guangzhou, Guangdong, China

3. Malaria Functional Genomics Section, Laboratory of Malaria and Vector Research, National Institute of Allergy and Infectious Diseases, National Institutes of Health , Bethesda, Maryland, USA

4. Yue Bei People's Hospital Postdoctoral Innovation Practice Base, Southern Medical University , Guangzhou, Guangdong, China

5. Department of Joint Surgery, the Fifth Affiliated Hospital of Southern Medical University , Guangzhou, Guangdong, China

6. Guangdong Provincial Key Lab of Single Cell Technology and Application, Southern Medical University , Guangzhou, Guangdong, China

Abstract

ABSTRACT Stringent control of the type I interferon (IFN-I) signaling is critical for host immune defense against infectious diseases, yet the molecular mechanisms that regulate this pathway remain elusive. Here, we show that Src homology 2 containing inositol phosphatase 1 (SHIP1) suppresses IFN-I signaling by promoting IRF3 degradation during malaria infection. Genetic ablation of Ship1 in mice leads to high levels of IFN-I and confers resistance to Plasmodium yoelii nigeriensis ( P.y. ) N67 infection. Mechanistically, SHIP1 promotes the selective autophagic degradation of IRF3 by enhancing K63-linked ubiquitination of IRF3 at lysine 313, which serves as a recognition signal for NDP52-mediated selective autophagic degradation. In addition, SHIP1 is downregulated by IFN-I-induced miR-155-5p upon P.y . N67 infection and severs as a feedback loop of the signaling crosstalk. This study reveals a regulatory mechanism between IFN-I signaling and autophagy, and verifies SHIP1 can be a potential target for therapeutic intervention against malaria and other infectious diseases. IMPORTANCE Malaria remains a serious disease affecting millions of people worldwide. Malaria parasite infection triggers tightly controlled type I interferon (IFN-I) signaling that plays a critical role in host innate immunity; however, the molecular mechanisms underlying the immune responses are still elusive. Here, we discover a host gene [Src homology 2-containing inositol phosphatase 1 (SHIP1)] that can regulate IFN-I signaling by modulating NDP52-mediated selective autophagic degradation of IRF3 and significantly affect parasitemia and resistance of Plasmodium -infected mice. This study identifies SHIP1 as a potential target for immunotherapies in malaria and highlights the crosstalk between IFN-I signaling and autophagy in preventing related infectious diseases. SHIP1 functions as a negative regulator during malaria infection by targeting IRF3 for autophagic degradation.

Funder

MOST | National Natural Science Foundation of China

GDSTC | Basic and Applied Basic Research Foundation of Guangdong Province

Guangdong Zhujiang Youth Scholar Funding

Division of Intramural Research, National Institute of Allergy and Infectious Diseases

The Star-up Fund for High-level talents of Southern Medical University

Publisher

American Society for Microbiology

Subject

Virology,Microbiology

Link

https://journals.asm.org/doi/pdf/10.1128/mbio.03512-22