Opposing effect of EGFRWT on EGFRvIII-mediated NF-κB activation with RIP1 as a cell death switch

Vineshkumar Thidil Puliyappadamba; Sharmistha Chakraborty; SandiliS Chauncey; Li Li; Kimmo J. Hatanpaa; Bruce Mickey; Shayan Noorani; Hui Kuo G Shu; Sandeep Burma; David A. Boothman; Amyn A. Habib

doi:10.1016/j.celrep.2013.07.025

Opposing effect of EGFRWT on EGFRvIII-mediated NF-κB activation with RIP1 as a cell death switch

Vineshkumar Thidil Puliyappadamba, Sharmistha Chakraborty, SandiliS Chauncey, Li Li, Kimmo J. Hatanpaa, Bruce Mickey, Shayan Noorani, Hui Kuo G Shu, Sandeep Burma, David A. Boothman, Amyn A. Habib

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

36 Scopus citations

Abstract

RIP1 is a central mediator of cell death in response tocell stress but can also mediate cell survival by activating NF-κB. Here, we show that RIP1 acts as a switch in EGFR signaling. EGFRvIII is an oncogenic mutant that does not bind ligand and is coexpressed with EGFRWT in glioblastoma multiforme (GBM). EGFRvIII recruits ubiquitin ligases to RIP1, resultingin K63-linked ubiquitination of RIP1. RIP1 binds toTAK1 and NEMO, forming an EGFRvIII-RIP1 signalosome that activates NF-κB. RIP1 is essential for EGFRvIII-mediated oncogenicity and correlates with NF-κB activation in GBM. Surprisingly, activation of EGFRWT with EGF results in a negative regulation of EGFRvIII, with dissociation of the EGFRvIII-RIP1 signalosome, loss of RIP1 ubiquitination and NF-κB activation, and association of RIP1 with FADD and caspase-8. If EGFRWT is overexpressed with EGFRvIII, the addition of EGF leads to a RIP1 kinase-dependent cell death. The EGFRWT-EGFRvIII-RIP1 interplay may regulate oncogenicity and vulnerability to targeted treatment in GBM

Original language	English (US)
Pages (from-to)	764-775
Number of pages	12
Journal	Cell Reports
Volume	4
Issue number	4
DOIs	https://doi.org/10.1016/j.celrep.2013.07.025
State	Published - Aug 29 2013

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology

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10.1016/j.celrep.2013.07.025

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@article{fdb0668f469e40489eb7f1fe93f812ba,

title = "Opposing effect of EGFRWT on EGFRvIII-mediated NF-κB activation with RIP1 as a cell death switch",

abstract = "RIP1 is a central mediator of cell death in response tocell stress but can also mediate cell survival by activating NF-κB. Here, we show that RIP1 acts as a switch in EGFR signaling. EGFRvIII is an oncogenic mutant that does not bind ligand and is coexpressed with EGFRWT in glioblastoma multiforme (GBM). EGFRvIII recruits ubiquitin ligases to RIP1, resultingin K63-linked ubiquitination of RIP1. RIP1 binds toTAK1 and NEMO, forming an EGFRvIII-RIP1 signalosome that activates NF-κB. RIP1 is essential for EGFRvIII-mediated oncogenicity and correlates with NF-κB activation in GBM. Surprisingly, activation of EGFRWT with EGF results in a negative regulation of EGFRvIII, with dissociation of the EGFRvIII-RIP1 signalosome, loss of RIP1 ubiquitination and NF-κB activation, and association of RIP1 with FADD and caspase-8. If EGFRWT is overexpressed with EGFRvIII, the addition of EGF leads to a RIP1 kinase-dependent cell death. The EGFRWT-EGFRvIII-RIP1 interplay may regulate oncogenicity and vulnerability to targeted treatment in GBM",

author = "Puliyappadamba, {Vineshkumar Thidil} and Sharmistha Chakraborty and SandiliS Chauncey and Li Li and Hatanpaa, {Kimmo J.} and Bruce Mickey and Shayan Noorani and Shu, {Hui Kuo G} and Sandeep Burma and Boothman, {David A.} and Habib, {Amyn A.}",

note = "Funding Information: We thank Dr. Mien-Chie Hung (MD Anderson Cancer Center) for the EGFRWT-Myc plasmid and Dr. James Van Brocklyn (Ohio State University) for GBM9-NS cells. This work was supported in part by NIH grants RO1 NS062080 to A.A.H., RO1 grants CA139217 and CA102792 to D.A.B., and RO1 CA149461 to S.B., and by grants from the National Aeronautics and Space Administration (NNX13AI13G) and the Cancer Prevention and Research Institute of Texas (RP100644) to S.B. ",

year = "2013",

month = aug,

day = "29",

doi = "10.1016/j.celrep.2013.07.025",

language = "English (US)",

volume = "4",

pages = "764--775",

journal = "Cell Reports",

issn = "2211-1247",

publisher = "Cell Press",

number = "4",

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TY - JOUR

T1 - Opposing effect of EGFRWT on EGFRvIII-mediated NF-κB activation with RIP1 as a cell death switch

AU - Puliyappadamba, Vineshkumar Thidil

AU - Chakraborty, Sharmistha

AU - Chauncey, SandiliS

AU - Li, Li

AU - Hatanpaa, Kimmo J.

AU - Mickey, Bruce

AU - Noorani, Shayan

AU - Shu, Hui Kuo G

AU - Burma, Sandeep

AU - Boothman, David A.

AU - Habib, Amyn A.

N1 - Funding Information: We thank Dr. Mien-Chie Hung (MD Anderson Cancer Center) for the EGFRWT-Myc plasmid and Dr. James Van Brocklyn (Ohio State University) for GBM9-NS cells. This work was supported in part by NIH grants RO1 NS062080 to A.A.H., RO1 grants CA139217 and CA102792 to D.A.B., and RO1 CA149461 to S.B., and by grants from the National Aeronautics and Space Administration (NNX13AI13G) and the Cancer Prevention and Research Institute of Texas (RP100644) to S.B.

PY - 2013/8/29

Y1 - 2013/8/29

N2 - RIP1 is a central mediator of cell death in response tocell stress but can also mediate cell survival by activating NF-κB. Here, we show that RIP1 acts as a switch in EGFR signaling. EGFRvIII is an oncogenic mutant that does not bind ligand and is coexpressed with EGFRWT in glioblastoma multiforme (GBM). EGFRvIII recruits ubiquitin ligases to RIP1, resultingin K63-linked ubiquitination of RIP1. RIP1 binds toTAK1 and NEMO, forming an EGFRvIII-RIP1 signalosome that activates NF-κB. RIP1 is essential for EGFRvIII-mediated oncogenicity and correlates with NF-κB activation in GBM. Surprisingly, activation of EGFRWT with EGF results in a negative regulation of EGFRvIII, with dissociation of the EGFRvIII-RIP1 signalosome, loss of RIP1 ubiquitination and NF-κB activation, and association of RIP1 with FADD and caspase-8. If EGFRWT is overexpressed with EGFRvIII, the addition of EGF leads to a RIP1 kinase-dependent cell death. The EGFRWT-EGFRvIII-RIP1 interplay may regulate oncogenicity and vulnerability to targeted treatment in GBM

AB - RIP1 is a central mediator of cell death in response tocell stress but can also mediate cell survival by activating NF-κB. Here, we show that RIP1 acts as a switch in EGFR signaling. EGFRvIII is an oncogenic mutant that does not bind ligand and is coexpressed with EGFRWT in glioblastoma multiforme (GBM). EGFRvIII recruits ubiquitin ligases to RIP1, resultingin K63-linked ubiquitination of RIP1. RIP1 binds toTAK1 and NEMO, forming an EGFRvIII-RIP1 signalosome that activates NF-κB. RIP1 is essential for EGFRvIII-mediated oncogenicity and correlates with NF-κB activation in GBM. Surprisingly, activation of EGFRWT with EGF results in a negative regulation of EGFRvIII, with dissociation of the EGFRvIII-RIP1 signalosome, loss of RIP1 ubiquitination and NF-κB activation, and association of RIP1 with FADD and caspase-8. If EGFRWT is overexpressed with EGFRvIII, the addition of EGF leads to a RIP1 kinase-dependent cell death. The EGFRWT-EGFRvIII-RIP1 interplay may regulate oncogenicity and vulnerability to targeted treatment in GBM

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SN - 2211-1247

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SP - 764

EP - 775

JO - Cell Reports

JF - Cell Reports

IS - 4

ER -

Opposing effect of EGFRWT on EGFRvIII-mediated NF-κB activation with RIP1 as a cell death switch

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