The viral nucleocapsid protein of transmissible gastroenteritis coronavirus (TGEV) is cleaved by caspase-6 and -7 during TGEV-induced apoptosis

J F Eléouët; E A Slee; F Saurini; N Castagné; D Poncet; C Garrido; E Solary; S J Martin

doi:10.1128/jvi.74.9.3975-3983.2000

The viral nucleocapsid protein of transmissible gastroenteritis coronavirus (TGEV) is cleaved by caspase-6 and -7 during TGEV-induced apoptosis

J Virol. 2000 May;74(9):3975-83. doi: 10.1128/jvi.74.9.3975-3983.2000.

Authors

J F Eléouët¹, E A Slee, F Saurini, N Castagné, D Poncet, C Garrido, E Solary, S J Martin

Affiliation

¹ Unité de Virologie et Immunologie Moléculaires, Institut National de la Recherche Agronomique, 78350 Jouy-en-Josas, France. [email protected]

Abstract

The transmissible gastroenteritis coronavirus (TGEV), like many other viruses, exerts much of its cytopathic effect through the induction of apoptosis of its host cell. Apoptosis is coordinated by a family of cysteine proteases, called caspases, that are activated during apoptosis and participate in dismantling the cell by cleaving key structural and regulatory proteins. We have explored the caspase activation events that are initiated upon infection of the human rectal tumor cell line HRT18 with TGEV. We show that TGEV infection results in the activation of caspase-3, -6, -7, -8, and -9 and cleavage of the caspase substrates eIF4GI, gelsolin, and alpha-fodrin. Surprisingly, the TGEV nucleoprotein (N) underwent proteolysis in parallel with the activation of caspases within the host cell. Cleavage of the N protein was inhibited by cell-permeative caspase inhibitors, suggesting that this viral structural protein is a target for host cell caspases. We show that the TGEV nucleoprotein is a substrate for both caspase-6 and -7, and using site-directed mutagenesis, we have mapped the cleavage site to VVPD(359) downward arrow. These data demonstrate that viral proteins can be targeted for destruction by the host cell death machinery.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Amino Acid Chloromethyl Ketones / pharmacology
Animals
Apoptosis* / drug effects
CD13 Antigens / genetics
CD13 Antigens / metabolism
Caspase 3
Caspase 6
Caspase 7
Caspase 8
Caspase 9
Caspases / metabolism*
Cell Extracts
Coronavirus Nucleocapsid Proteins
Cysteine Proteinase Inhibitors / pharmacology
Cytochrome c Group / metabolism
Cytosol / metabolism
Enzyme Activation
Humans
Mitochondria / metabolism
Nucleocapsid / genetics
Nucleocapsid / metabolism*
Nucleocapsid Proteins*
Oligopeptides / pharmacology
Receptors, Virus / genetics
Receptors, Virus / metabolism
Transmissible gastroenteritis virus / metabolism*
Transmissible gastroenteritis virus / physiology
Tumor Cells, Cultured

Substances

Amino Acid Chloromethyl Ketones
Cell Extracts
Coronavirus Nucleocapsid Proteins
Cysteine Proteinase Inhibitors
Cytochrome c Group
Nucleocapsid Proteins
Oligopeptides
Receptors, Virus
benzyloxycarbonyl-isoleucyl-glutamyl-threonyl-aspartic acid fluoromethyl ketone
benzyloxycarbonylvalyl-alanyl-aspartyl fluoromethyl ketone
CD13 Antigens
CASP3 protein, human
CASP6 protein, human
CASP7 protein, human
CASP8 protein, human
CASP9 protein, human
Caspase 3
Caspase 6
Caspase 7
Caspase 8
Caspase 9
Caspases

Grants and funding

Wellcome Trust/United Kingdom