Oncogenic NRAS signaling differentially regulates survival and proliferation in melanoma

Lawrence N. Kwong; James C. Costello; Huiyun Liu; Shan Jiang; Timothy L. Helms; Aliete E. Langsdorf; David Jakubosky; Giannicola Genovese; Florian L. Muller; Joseph H. Jeong; Ryan P. Bender; Gerald C. Chu; Keith T. Flaherty; Jennifer A. Wargo; James J. Collins; Lynda Chin

doi:10.1038/nm.2941

Oncogenic NRAS signaling differentially regulates survival and proliferation in melanoma

Lawrence N. Kwong, James C. Costello, Huiyun Liu, Shan Jiang, Timothy L. Helms, Aliete E. Langsdorf, David Jakubosky, Giannicola Genovese, Florian L. Muller, Joseph H. Jeong, Ryan P. Bender, Gerald C. Chu, Keith T. Flaherty, Jennifer A. Wargo, James J. Collins, Lynda Chin

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293 Scopus citations

Abstract

The discovery of potent inhibitors of the BRAF proto-oncogene has revolutionized therapy for melanoma harboring mutations in BRAF, yet NRAS-mutant melanoma remains without an effective therapy. Because direct pharmacological inhibition of the RAS proto-oncogene has thus far been unsuccessful, we explored systems biology approaches to identify synergistic drug combination(s) that can mimic RAS inhibition. Here, leveraging an inducible mouse model of NRAS-mutant melanoma, we show that pharmacological inhibition of mitogen-activated protein kinase kinase (MEK) activates apoptosis but not cell-cycle arrest, which is in contrast to complete genetic neuroblastoma RAS homolog (NRAS) extinction, which triggers both of these effects. Network modeling pinpointed cyclin-dependent kinase 4 (CDK4) as a key driver of this differential phenotype. Accordingly, combined pharmacological inhibition of MEK and CDK4 in vivo led to substantial synergy in therapeutic efficacy. We suggest a gradient model of oncogenic NRAS signaling in which the output is gated, resulting in the decoupling of discrete downstream biological phenotypes as a result of incomplete inhibition. Such a gated signaling model offers a new framework to identify nonobvious coextinction target(s) for combined pharmacological inhibition in NRAS-mutant melanomas.

Original language	English (US)
Pages (from-to)	1503-1510
Number of pages	8
Journal	Nature medicine
Volume	18
Issue number	10
DOIs	https://doi.org/10.1038/nm.2941
State	Published - Oct 2012

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology

MD Anderson CCSG core facilities

Functional Proteomics Reverse Phase Protein Array Core

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10.1038/nm.2941

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Kwong, L. N., Costello, J. C., Liu, H., Jiang, S., Helms, T. L., Langsdorf, A. E., Jakubosky, D., Genovese, G., Muller, F. L., Jeong, J. H., Bender, R. P., Chu, G. C., Flaherty, K. T., Wargo, J. A., Collins, J. J., & Chin, L. (2012). Oncogenic NRAS signaling differentially regulates survival and proliferation in melanoma. Nature medicine, 18(10), 1503-1510. https://doi.org/10.1038/nm.2941

@article{979628dc78874be58c6bf5d9d3c4367e,

title = "Oncogenic NRAS signaling differentially regulates survival and proliferation in melanoma",

abstract = "The discovery of potent inhibitors of the BRAF proto-oncogene has revolutionized therapy for melanoma harboring mutations in BRAF, yet NRAS-mutant melanoma remains without an effective therapy. Because direct pharmacological inhibition of the RAS proto-oncogene has thus far been unsuccessful, we explored systems biology approaches to identify synergistic drug combination(s) that can mimic RAS inhibition. Here, leveraging an inducible mouse model of NRAS-mutant melanoma, we show that pharmacological inhibition of mitogen-activated protein kinase kinase (MEK) activates apoptosis but not cell-cycle arrest, which is in contrast to complete genetic neuroblastoma RAS homolog (NRAS) extinction, which triggers both of these effects. Network modeling pinpointed cyclin-dependent kinase 4 (CDK4) as a key driver of this differential phenotype. Accordingly, combined pharmacological inhibition of MEK and CDK4 in vivo led to substantial synergy in therapeutic efficacy. We suggest a gradient model of oncogenic NRAS signaling in which the output is gated, resulting in the decoupling of discrete downstream biological phenotypes as a result of incomplete inhibition. Such a gated signaling model offers a new framework to identify nonobvious coextinction target(s) for combined pharmacological inhibition in NRAS-mutant melanomas.",

author = "Kwong, {Lawrence N.} and Costello, {James C.} and Huiyun Liu and Shan Jiang and Helms, {Timothy L.} and Langsdorf, {Aliete E.} and David Jakubosky and Giannicola Genovese and Muller, {Florian L.} and Jeong, {Joseph H.} and Bender, {Ryan P.} and Chu, {Gerald C.} and Flaherty, {Keith T.} and Wargo, {Jennifer A.} and Collins, {James J.} and Lynda Chin",

note = "Funding Information: for insightful discussions; R. Kwong for manuscript proofreading; D. Camacho for helping develop the TRAP algorithm; and M. Bar-Eli (University of Texas MD Anderson Cancer Center, Houston, Texas) for the SB-2 cell line. L.N.K. is supported by the Postdoctoral Fellowship (117842-PF-09-261-01-TBG) from the American Cancer Society. J.J.C. is supported by the US National Institutes of Health Director{\textquoteright}s Pioneer Award Program and the Howard Hughes Medical Institute. This work was supported by funding from the US National Institutes of Health to L.C. (U01 CA141508). L.C. is a recipient of the Abby S. and Howard P. Milstein 2009 Innovation Award for Melanoma and Skin Cancer Research and a CPRIT (Cancer Prevention Research Institute of Texas) Scholar in Cancer Research.",

year = "2012",

month = oct,

doi = "10.1038/nm.2941",

language = "English (US)",

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T1 - Oncogenic NRAS signaling differentially regulates survival and proliferation in melanoma

AU - Kwong, Lawrence N.

AU - Costello, James C.

AU - Liu, Huiyun

AU - Jiang, Shan

AU - Helms, Timothy L.

AU - Langsdorf, Aliete E.

AU - Jakubosky, David

AU - Genovese, Giannicola

AU - Muller, Florian L.

AU - Jeong, Joseph H.

AU - Bender, Ryan P.

AU - Chu, Gerald C.

AU - Flaherty, Keith T.

AU - Wargo, Jennifer A.

AU - Collins, James J.

AU - Chin, Lynda

N1 - Funding Information: for insightful discussions; R. Kwong for manuscript proofreading; D. Camacho for helping develop the TRAP algorithm; and M. Bar-Eli (University of Texas MD Anderson Cancer Center, Houston, Texas) for the SB-2 cell line. L.N.K. is supported by the Postdoctoral Fellowship (117842-PF-09-261-01-TBG) from the American Cancer Society. J.J.C. is supported by the US National Institutes of Health Director’s Pioneer Award Program and the Howard Hughes Medical Institute. This work was supported by funding from the US National Institutes of Health to L.C. (U01 CA141508). L.C. is a recipient of the Abby S. and Howard P. Milstein 2009 Innovation Award for Melanoma and Skin Cancer Research and a CPRIT (Cancer Prevention Research Institute of Texas) Scholar in Cancer Research.

PY - 2012/10

Y1 - 2012/10

N2 - The discovery of potent inhibitors of the BRAF proto-oncogene has revolutionized therapy for melanoma harboring mutations in BRAF, yet NRAS-mutant melanoma remains without an effective therapy. Because direct pharmacological inhibition of the RAS proto-oncogene has thus far been unsuccessful, we explored systems biology approaches to identify synergistic drug combination(s) that can mimic RAS inhibition. Here, leveraging an inducible mouse model of NRAS-mutant melanoma, we show that pharmacological inhibition of mitogen-activated protein kinase kinase (MEK) activates apoptosis but not cell-cycle arrest, which is in contrast to complete genetic neuroblastoma RAS homolog (NRAS) extinction, which triggers both of these effects. Network modeling pinpointed cyclin-dependent kinase 4 (CDK4) as a key driver of this differential phenotype. Accordingly, combined pharmacological inhibition of MEK and CDK4 in vivo led to substantial synergy in therapeutic efficacy. We suggest a gradient model of oncogenic NRAS signaling in which the output is gated, resulting in the decoupling of discrete downstream biological phenotypes as a result of incomplete inhibition. Such a gated signaling model offers a new framework to identify nonobvious coextinction target(s) for combined pharmacological inhibition in NRAS-mutant melanomas.

AB - The discovery of potent inhibitors of the BRAF proto-oncogene has revolutionized therapy for melanoma harboring mutations in BRAF, yet NRAS-mutant melanoma remains without an effective therapy. Because direct pharmacological inhibition of the RAS proto-oncogene has thus far been unsuccessful, we explored systems biology approaches to identify synergistic drug combination(s) that can mimic RAS inhibition. Here, leveraging an inducible mouse model of NRAS-mutant melanoma, we show that pharmacological inhibition of mitogen-activated protein kinase kinase (MEK) activates apoptosis but not cell-cycle arrest, which is in contrast to complete genetic neuroblastoma RAS homolog (NRAS) extinction, which triggers both of these effects. Network modeling pinpointed cyclin-dependent kinase 4 (CDK4) as a key driver of this differential phenotype. Accordingly, combined pharmacological inhibition of MEK and CDK4 in vivo led to substantial synergy in therapeutic efficacy. We suggest a gradient model of oncogenic NRAS signaling in which the output is gated, resulting in the decoupling of discrete downstream biological phenotypes as a result of incomplete inhibition. Such a gated signaling model offers a new framework to identify nonobvious coextinction target(s) for combined pharmacological inhibition in NRAS-mutant melanomas.

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ER -

Oncogenic NRAS signaling differentially regulates survival and proliferation in melanoma

Abstract

ASJC Scopus subject areas

MD Anderson CCSG core facilities

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