Neonatal Fc receptor is a functional receptor for classical human astrovirus

Author:

Haga Kei1,Tokui Takashi1,Miyamoto Kana1,Takai‐Todaka Reiko1,Kudo Shiori1,Ishikawa Azusa1,Ishiyama Ryoka1,Kato Akiko2,Yokoyama Masaru3,Katayama Kazuhiko1ORCID,Nakanishi Akira24

Affiliation:

1. Laboratory of Viral Infection Control, Department of Infection Control and Immunology, Ōmura Satoshi Memorial Institute & Graduate School of Infection Control Sciences Kitasato University Tokyo Japan

2. National Center for Geriatrics and Gerontology, Department of Aging Intervention Laboratory of Gene Therapy, and Laboratory for Radiation safety Aichi Japan

3. Pathogen Genomics Center, National Institute of Infectious Diseases Tokyo Japan

4. Department of Biology‐Oriented Science and Technology Kindai University Wakayama Japan

Abstract

AbstractHuman astrovirus (HAstV) is a global cause of gastroenteritis in infants, the elderly, and the immunocompromised. However, the molecular mechanisms that control its susceptibility are not fully understood, as the functional receptor used by the virus has yet to be identified. Here, a genome‐wide CRISPR‐Cas9 library screen in Caco2 cells revealed that the neonatal Fc receptor (FcRn) can function as a receptor for classical HAstV (Mamastrovirus genotype 1). Deletion of FCGRT or B2M, which encode subunits of FcRn, rendered Caco2 cells and intestinal organoid cells resistant to HAstV infection. We also showed that human FcRn expression renders non‐susceptible cells permissive to viral infection and that FcRn binds directly to the HAstV spike protein. Therefore, our findings provide insight into the entry mechanism of HAstV into susceptible cells. We anticipate that this information can be used to develop new therapies targeting human astroviruses, providing new strategies to treat this global health issue.

Funder

Japan Agency for Medical Research and Development

Japan Society for the Promotion of Science

Publisher

Wiley

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