Author
Listed:
- Yao Dai
(Shanghai Jiao Tong University)
- Manja Idorn
(Aarhus University
Center for Immunology of Viral Infections)
- Manutea C. Serrero
(Aarhus University
Center for Immunology of Viral Infections)
- Xiaoyong Pan
(Shanghai Jiao Tong University)
- Emil A. Thomsen
(Aarhus University
Center for Immunology of Viral Infections)
- Ryo Narita
(Aarhus University
Center for Immunology of Viral Infections)
- Muyesier Maimaitili
(Aarhus University
Center for Immunology of Viral Infections)
- Xiaoqing Qian
(Shanghai Jiao Tong University)
- Marie B. Iversen
(Aarhus University
Center for Immunology of Viral Infections)
- Line S. Reinert
(Aarhus University
Center for Immunology of Viral Infections)
- Rasmus K. Flygaard
(Aarhus University)
- Muwan Chen
(Aarhus University
Center for Immunology of Viral Infections
Aarhus University)
- Xiangning Ding
(Aarhus University
Center for Immunology of Viral Infections)
- Bao-cun Zhang
(Aarhus University
Center for Immunology of Viral Infections)
- Madalina E. Carter-Timofte
(Aarhus University
Center for Immunology of Viral Infections)
- Qing Lu
(Shanghai Jiao Tong University)
- Zhuofan Jiang
(Shanghai Jiao Tong University)
- Yiye Zhong
(Shanghai Jiao Tong University)
- Shuhui Zhang
(Shanghai Jiao Tong University)
- Lintai Da
(Shanghai Jiao Tong University)
- Jinwei Zhu
(Shanghai Jiao Tong University)
- Mark Denham
(Aarhus University
Aarhus University)
- Poul Nissen
(Aarhus University
Aarhus University)
- Trine H. Mogensen
(Aarhus University
Center for Immunology of Viral Infections
Aarhus University Hospital)
- Jacob Giehm Mikkelsen
(Aarhus University
Center for Immunology of Viral Infections)
- Shen-Ying Zhang
(Imagine Institute
The Rockefeller University)
- Jean-Laurent Casanova
(Imagine Institute
The Rockefeller University
Necker Hospital for Sick Children
Howard Hughes Medical Institute)
- Yujia Cai
(Shanghai Jiao Tong University
Aarhus University)
- Søren R. Paludan
(Aarhus University
Center for Immunology of Viral Infections
University of Gothenburg)
Abstract
The brain is highly sensitive to damage caused by infection and inflammation1,2. Herpes simplex virus 1 (HSV-1) is a neurotropic virus and the cause of herpes simplex encephalitis3. It is unknown whether neuron-specific antiviral factors control virus replication to prevent infection and excessive inflammatory responses, hence protecting the brain. Here we identify TMEFF1 as an HSV-1 restriction factor using genome-wide CRISPR screening. TMEFF1 is expressed specifically in neurons of the central nervous system and is not regulated by type I interferon, the best-known innate antiviral system controlling virus infections. Depletion of TMEFF1 in stem-cell-derived human neurons led to elevated viral replication and neuronal death following HSV-1 infection. TMEFF1 blocked the HSV-1 replication cycle at the level of viral entry through interactions with nectin-1 and non-muscle myosin heavy chains IIA and IIB, which are core proteins in virus–cell binding and virus–cell fusion, respectively4–6. Notably, Tmeff1−/− mice exhibited increased susceptibility to HSV-1 infection in the brain but not in the periphery. Within the brain, elevated viral load was observed specifically in neurons. Our study identifies TMEFF1 as a neuron-specific restriction factor essential for prevention of HSV-1 replication in the central nervous system.
Suggested Citation
Yao Dai & Manja Idorn & Manutea C. Serrero & Xiaoyong Pan & Emil A. Thomsen & Ryo Narita & Muyesier Maimaitili & Xiaoqing Qian & Marie B. Iversen & Line S. Reinert & Rasmus K. Flygaard & Muwan Chen & , 2024.
"TMEFF1 is a neuron-specific restriction factor for herpes simplex virus,"
Nature, Nature, vol. 632(8024), pages 383-389, August.
Handle:
RePEc:nat:nature:v:632:y:2024:i:8024:d:10.1038_s41586-024-07670-z
DOI: 10.1038/s41586-024-07670-z
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