β-Coronaviruses Use Lysosomes for Egress Instead of the Biosynthetic Secretory Pathway
Author(s) -
Sourish Ghosh,
Teegan A. Dellibovi-Ragheb,
Adeline Kerviel,
Eowyn Pak,
Qi Qiu,
M. Patricia Fisher,
Peter M. Takvorian,
Christopher K. E. Bleck,
Victor W. Hsu,
Anthony R. Fehr,
Stanley Perlman,
Sooraj Achar,
Marco R. Straus,
Gary R. Whittaker,
Cornelis A. M. de Haan,
John H. Kehrl,
Grégoire AltanBonnet,
Nihal AltanBonnet
Publication year - 2020
Publication title -
cell
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 26.304
H-Index - 776
eISSN - 1097-4172
pISSN - 0092-8674
DOI - 10.1016/j.cell.2020.10.039
Subject(s) - biology , lytic cycle , coronavirus , microbiology and biotechnology , endosome , lysosome , gtpase , rab , viral replication , virology , secretory pathway , virus , covid-19 , enzyme , biochemistry , medicine , golgi apparatus , disease , pathology , endoplasmic reticulum , infectious disease (medical specialty) , intracellular
β-Coronaviruses are a family of positive-strand enveloped RNA viruses that includes the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). Much is known regarding their cellular entry and replication pathways, but their mode of egress remains uncertain. Using imaging methodologies and virus-specific reporters, we demonstrate that β-coronaviruses utilize lysosomal trafficking for egress rather than the biosynthetic secretory pathway more commonly used by other enveloped viruses. This unconventional egress is regulated by the Arf-like small GTPase Arl8b and can be blocked by the Rab7 GTPase competitive inhibitor CID1067700. Such non-lytic release of β-coronaviruses results in lysosome deacidification, inactivation of lysosomal degradation enzymes, and disruption of antigen presentation pathways. β-Coronavirus-induced exploitation of lysosomal organelles for egress provides insights into the cellular and immunological abnormalities observed in patients and suggests new therapeutic modalities.
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