Author
Listed:
- Rohit K. Jangra
(Albert Einstein College of Medicine)
- Andrew S. Herbert
(United States Army Medical Research Institute of Infectious Diseases)
- Rong Li
(Utah State University)
- Lucas T. Jae
(The Netherlands Cancer Institute
Ludwig-Maximilians-Universität München)
- Lara M. Kleinfelter
(Albert Einstein College of Medicine)
- Megan M. Slough
(Albert Einstein College of Medicine)
- Sarah L. Barker
(University of Toronto)
- Pablo Guardado-Calvo
(Structural Virology Unit and CNRS UMR3569)
- Gleyder Román-Sosa
(Structural Virology Unit and CNRS UMR3569)
- M. Eugenia Dieterle
(Albert Einstein College of Medicine)
- Ana I. Kuehne
(United States Army Medical Research Institute of Infectious Diseases)
- Nicolás A. Muena
(Laboratorio de Virología Molecular)
- Ariel S. Wirchnianski
(United States Army Medical Research Institute of Infectious Diseases
Albert Einstein College of Medicine)
- Elisabeth K. Nyakatura
(Albert Einstein College of Medicine)
- J. Maximilian Fels
(Albert Einstein College of Medicine)
- Melinda Ng
(Albert Einstein College of Medicine)
- Eva Mittler
(Albert Einstein College of Medicine)
- James Pan
(University of Toronto)
- Sushma Bharrhan
(Albert Einstein College of Medicine)
- Anna Z. Wec
(Albert Einstein College of Medicine
Adimab LLC)
- Jonathan R. Lai
(Albert Einstein College of Medicine)
- Sachdev S. Sidhu
(University of Toronto)
- Nicole D. Tischler
(Laboratorio de Virología Molecular)
- Félix A. Rey
(Structural Virology Unit and CNRS UMR3569)
- Jason Moffat
(University of Toronto
Canadian Institute for Advanced Research)
- Thijn R. Brummelkamp
(The Netherlands Cancer Institute
CeMM Research Center for Molecular Medicine of the Austrian Academy of Sciences
Cancer GenomiCs.nl (CGC.nl))
- Zhongde Wang
(Utah State University)
- John M. Dye
(United States Army Medical Research Institute of Infectious Diseases)
- Kartik Chandran
(Albert Einstein College of Medicine)
Abstract
The zoonotic transmission of hantaviruses from their rodent hosts to humans in North and South America is associated with a severe and frequently fatal respiratory disease, hantavirus pulmonary syndrome (HPS)1,2. No specific antiviral treatments for HPS are available, and no molecular determinants of in vivo susceptibility to hantavirus infection and HPS are known. Here we identify the human asthma-associated gene protocadherin-1 (PCDH1)3–6 as an essential determinant of entry and infection in pulmonary endothelial cells by two hantaviruses that cause HPS, Andes virus (ANDV) and Sin Nombre virus (SNV). In vitro, we show that the surface glycoproteins of ANDV and SNV directly recognize the outermost extracellular repeat domain of PCDH1—a member of the cadherin superfamily7,8—to exploit PCDH1 for entry. In vivo, genetic ablation of PCDH1 renders Syrian golden hamsters highly resistant to a usually lethal ANDV challenge. Targeting PCDH1 could provide strategies to reduce infection and disease caused by New World hantaviruses.
Suggested Citation
Rohit K. Jangra & Andrew S. Herbert & Rong Li & Lucas T. Jae & Lara M. Kleinfelter & Megan M. Slough & Sarah L. Barker & Pablo Guardado-Calvo & Gleyder Román-Sosa & M. Eugenia Dieterle & Ana I. Kuehne, 2018.
"Protocadherin-1 is essential for cell entry by New World hantaviruses,"
Nature, Nature, vol. 563(7732), pages 559-563, November.
Handle:
RePEc:nat:nature:v:563:y:2018:i:7732:d:10.1038_s41586-018-0702-1
DOI: 10.1038/s41586-018-0702-1
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