The HSV-1 Us3 protein kinase is sufficient to block apoptosis induced by overexpression of a variety of Bcl-2 family members

Paul D. Ogg; Peter J. McDonell; Brent J. Ryckman; C. Michael Knudson; Richard J. Roller

doi:10.1016/j.virol.2003.10.019

The HSV-1 Us3 protein kinase is sufficient to block apoptosis induced by overexpression of a variety of Bcl-2 family members

Paul D. Ogg
, Peter J. McDonell
, Brent J. Ryckman
, C. Michael Knudson
, Richard J. Roller

University of Iowa

Research output: Contribution to journal › Article › peer-review

103 Scopus citations

Abstract

The Us3 protein kinase encoded by herpes simplex virus type-1 (HSV-1) suppresses apoptosis in infected cells and is sufficient to block apoptosis induced by overexpression of Bad [Proc. Natl. Acad. Sci. 98 (2001) 10410]. While Us3 can induce phosphorylation of Bad, phosphorylation of Bad is dispensable for Us3 anti-apoptotic function [J. Virol. 77 (2003) 6567]. We extend the findings with Bad to demonstrate that Us3 blocks apoptosis induced by overexpression of Bid, a factor parallel to Bad in the apoptotic pathway, and Bax, a factor downstream of Bad in the apoptotic pathway. A previous report suggested that Us3 exerts its effects at a premitochondrial stage [J. Virol. 75 (2001) 5491], but our results suggest that Us3 exerts anti-apoptotic effects downstream of the mitochondria. We show that the kinase activity of Us3 is necessary for Us3 anti-apoptotic effects, because a catalytically inactive form of Us3 was unable to block apoptosis. A second function of Us3, primary envelopment during viral egress, is conserved in the Us3 homologue of Pseudorabies virus (PRV) [J. Gen. Virol. 82 (2001) 2363]. Experiments published here demonstrate that PRV Us3 can also block apoptosis induced by Bax, suggesting that the anti-apoptotic activity of Us3 is conserved across α-herpesviruses.

Original language	English
Pages (from-to)	212-224
Number of pages	13
Journal	Virology
Volume	319
Issue number	2
DOIs	https://doi.org/10.1016/j.virol.2003.10.019
State	Published - Feb 20 2004

Funding

We thank the Central Microscopy Facility at the University of Iowa (especially Katherine Walters) for their assistance with fluorescence microscopy and the Olympus BX-51 camera, Dr. Bernard Roizman (University of Chicago) for the generous gift of Us3 antibody, and Dr. Wendy Maury (University of Iowa) for critical reading of the manuscript. This work was supported by the University of Iowa and Public Health Service Awards AI 41478.

Funder number
R01AI041478

Keywords

Apoptosis
Herpes simplex virus type-1, HSV-1
Kinase
Mitochondria
Programmed cell death
Protein
Pseudorabies virus, PRV
Us3

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10.1016/j.virol.2003.10.019

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title = "The HSV-1 Us3 protein kinase is sufficient to block apoptosis induced by overexpression of a variety of Bcl-2 family members",

abstract = "The Us3 protein kinase encoded by herpes simplex virus type-1 (HSV-1) suppresses apoptosis in infected cells and is sufficient to block apoptosis induced by overexpression of Bad [Proc. Natl. Acad. Sci. 98 (2001) 10410]. While Us3 can induce phosphorylation of Bad, phosphorylation of Bad is dispensable for Us3 anti-apoptotic function [J. Virol. 77 (2003) 6567]. We extend the findings with Bad to demonstrate that Us3 blocks apoptosis induced by overexpression of Bid, a factor parallel to Bad in the apoptotic pathway, and Bax, a factor downstream of Bad in the apoptotic pathway. A previous report suggested that Us3 exerts its effects at a premitochondrial stage [J. Virol. 75 (2001) 5491], but our results suggest that Us3 exerts anti-apoptotic effects downstream of the mitochondria. We show that the kinase activity of Us3 is necessary for Us3 anti-apoptotic effects, because a catalytically inactive form of Us3 was unable to block apoptosis. A second function of Us3, primary envelopment during viral egress, is conserved in the Us3 homologue of Pseudorabies virus (PRV) [J. Gen. Virol. 82 (2001) 2363]. Experiments published here demonstrate that PRV Us3 can also block apoptosis induced by Bax, suggesting that the anti-apoptotic activity of Us3 is conserved across α-herpesviruses.",

keywords = "Apoptosis, Herpes simplex virus type-1, HSV-1, Kinase, Mitochondria, Programmed cell death, Protein, Pseudorabies virus, PRV, Us3",

author = "Ogg, \{Paul D.\} and McDonell, \{Peter J.\} and Ryckman, \{Brent J.\} and Knudson, \{C. Michael\} and Roller, \{Richard J.\}",

note = "Funding Information: We thank the Central Microscopy Facility at the University of Iowa (especially Katherine Walters) for their assistance with fluorescence microscopy and the Olympus BX-51 camera, Dr. Bernard Roizman (University of Chicago) for the generous gift of Us3 antibody, and Dr. Wendy Maury (University of Iowa) for critical reading of the manuscript. This work was supported by the University of Iowa and Public Health Service Awards AI 41478.",

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doi = "10.1016/j.virol.2003.10.019",

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AU - Ogg, Paul D.

AU - McDonell, Peter J.

AU - Ryckman, Brent J.

AU - Knudson, C. Michael

AU - Roller, Richard J.

N1 - Funding Information: We thank the Central Microscopy Facility at the University of Iowa (especially Katherine Walters) for their assistance with fluorescence microscopy and the Olympus BX-51 camera, Dr. Bernard Roizman (University of Chicago) for the generous gift of Us3 antibody, and Dr. Wendy Maury (University of Iowa) for critical reading of the manuscript. This work was supported by the University of Iowa and Public Health Service Awards AI 41478.

PY - 2004/2/20

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N2 - The Us3 protein kinase encoded by herpes simplex virus type-1 (HSV-1) suppresses apoptosis in infected cells and is sufficient to block apoptosis induced by overexpression of Bad [Proc. Natl. Acad. Sci. 98 (2001) 10410]. While Us3 can induce phosphorylation of Bad, phosphorylation of Bad is dispensable for Us3 anti-apoptotic function [J. Virol. 77 (2003) 6567]. We extend the findings with Bad to demonstrate that Us3 blocks apoptosis induced by overexpression of Bid, a factor parallel to Bad in the apoptotic pathway, and Bax, a factor downstream of Bad in the apoptotic pathway. A previous report suggested that Us3 exerts its effects at a premitochondrial stage [J. Virol. 75 (2001) 5491], but our results suggest that Us3 exerts anti-apoptotic effects downstream of the mitochondria. We show that the kinase activity of Us3 is necessary for Us3 anti-apoptotic effects, because a catalytically inactive form of Us3 was unable to block apoptosis. A second function of Us3, primary envelopment during viral egress, is conserved in the Us3 homologue of Pseudorabies virus (PRV) [J. Gen. Virol. 82 (2001) 2363]. Experiments published here demonstrate that PRV Us3 can also block apoptosis induced by Bax, suggesting that the anti-apoptotic activity of Us3 is conserved across α-herpesviruses.

AB - The Us3 protein kinase encoded by herpes simplex virus type-1 (HSV-1) suppresses apoptosis in infected cells and is sufficient to block apoptosis induced by overexpression of Bad [Proc. Natl. Acad. Sci. 98 (2001) 10410]. While Us3 can induce phosphorylation of Bad, phosphorylation of Bad is dispensable for Us3 anti-apoptotic function [J. Virol. 77 (2003) 6567]. We extend the findings with Bad to demonstrate that Us3 blocks apoptosis induced by overexpression of Bid, a factor parallel to Bad in the apoptotic pathway, and Bax, a factor downstream of Bad in the apoptotic pathway. A previous report suggested that Us3 exerts its effects at a premitochondrial stage [J. Virol. 75 (2001) 5491], but our results suggest that Us3 exerts anti-apoptotic effects downstream of the mitochondria. We show that the kinase activity of Us3 is necessary for Us3 anti-apoptotic effects, because a catalytically inactive form of Us3 was unable to block apoptosis. A second function of Us3, primary envelopment during viral egress, is conserved in the Us3 homologue of Pseudorabies virus (PRV) [J. Gen. Virol. 82 (2001) 2363]. Experiments published here demonstrate that PRV Us3 can also block apoptosis induced by Bax, suggesting that the anti-apoptotic activity of Us3 is conserved across α-herpesviruses.

KW - Apoptosis

KW - Herpes simplex virus type-1, HSV-1

KW - Kinase

KW - Mitochondria

KW - Programmed cell death

KW - Protein

KW - Pseudorabies virus, PRV

KW - Us3

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DO - 10.1016/j.virol.2003.10.019

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AN - SCOPUS:1342279571

SN - 0042-6822

VL - 319

SP - 212

EP - 224

JO - Virology

JF - Virology

IS - 2

ER -

The HSV-1 Us3 protein kinase is sufficient to block apoptosis induced by overexpression of a variety of Bcl-2 family members

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