Human MARCH1, 2, and 8 block Ebola virus envelope glycoprotein cleavage via targeting furin P domain

Author:

Yu Changqing1ORCID,Bai Yuanzhe2,Tan Wenbo3,Bai Yu4,Li Xuemei1,Zhou Yulong5,Zhai Jingbo6,Xue Mengzhou7,Tang Yan‐Dong2,Zheng Chunfu89ORCID,Liu Qiang10

Affiliation:

1. Engineering Center of Agricultural Biosafety Assessment and Biotechnology School of Advanced Agricultural Sciences, Yibin Vocational and Technical College Yibin People's Republic of China

2. State Key Laboratory for Animal Disease Control and Prevention Harbin Veterinary Research Institute, Chinese Academy of Agricultural Sciences Harbin People's Republic of China

3. College of Advanced Agriculture and Ecological Environment Heilongjiang University Harbin People's Republic of China

4. College of Animal Science Wenzhou Vocational College of Science and Technology Wenzhou People's Republic of China

5. College of Animal Science and Technology Heilongjiang Bayi Agricultural University Daqing People's Republic of China

6. Key Laboratory of Zoonose Prevention and Control at Universities of Inner Mongolia Autonomous Region, Medical College Inner Mongolia Minzu University Tongliao People's Republic of China

7. Department of Cerebrovascular Diseases The Second Affiliated Hospital of Zhengzhou University Zhengzhou People's Republic of China

8. Institute of Animal Health Guangdong Academy of Agricultural Sciences, Key Laboratory of Livestock Disease Prevention of Guangdong Province, Scientific Observation and Experiment Station of Veterinary Drugs and Diagnostic Techniques of Guangdong Province, Ministry of Agriculture and Rural Affairs Guangzhou People's Republic of China

9. Department of Microbiology, Immunology & Infection Diseases University of Calgary Calgary Alberta Canada

10. Nanchong Key Laboratory of Disease Prevention Control and Detection in Livestock and Poultry, Nanchong Vocational and Technical College Nanchong People's Republic of China

Abstract

AbstractMembrane‐associated RING‐CH (MARCH) family proteins were recently reported to inhibit viral replication through multiple modes. Previous work showed that human MARCH8 blocked Ebola virus (EBOV) glycoprotein (GP) maturation. Our study here demonstrates that human MARCH1 and MARCH2 share a similar pattern to MARCH8 in restricting EBOV GP‐pseudotyped viral infection. Human MARCH1 and MARCH2 retain EBOV GP at the trans‐Golgi network, reduce its cell surface display, and impair EBOV GP‐pseudotyped virions infectivity. Furthermore, we uncover that the host proprotein convertase furin could interact with human MARCH1/2 and EBOV GP intracellularly. Importantly, the furin P domain is verified to be recognized by MARCH1/2/8, which is critical for their blocking activities. Besides, bovine MARCH2 and murine MARCH1 also impair EBOV GP proteolytic processing. Altogether, our findings confirm that MARCH1/2 proteins of different mammalian origins showed a relatively conserved feature in blocking EBOV GP cleavage, which could provide clues for subsequent MARCHs antiviral studies and may facilitate the development of novel strategies to antagonize enveloped virus infection.

Publisher

Wiley

Subject

Infectious Diseases,Virology

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