RAS mutations in cutaneous squamous-cell carcinomas in patients treated with BRAF inhibitors

Fei Su; Amaya Viros; Carla Milagre; Kerstin Trunzer; Gideon Bollag; Olivia Spleiss; Jorge S. Reis-Filho; Xiangju Kong; Richard C. Koya; Keith T. Flaherty; Paul B. Chapman; Min Jung Kim; Robert Hayward; Matthew Martin; Hong Yang; Qiongqing Wang; Holly Hilton; Julie S. Hang; Johannes Noe; Maryou Lambros; Felipe Geyer; Nathalie Dhomen; Ion Niculescu-Duvaz; Alfonso Zambon; Dan Niculescu-Duvaz; Natasha Preece; Lídia Robert; Nicholas J. Otte; Stephen Mok; Damien Kee; Yan Ma; Chao Zhang; Gaston Habets; Elizabeth A. Burton; Bernice Wong; Hoa Nguyen; Mark Kockx; Luc Andries; Brian Lestini; Keith B. Nolop; Richard J. Lee; Andrew K. Joe; James L. Troy; Rene Gonzalez; Thomas E. Hutson; Igor Puzanov; Bartosz Chmielowski; Caroline J. Springer; Grant A. McArthur; Jeffrey A. Sosman; Roger S. Lo; Antoni Ribas; Richard Marais

doi:10.1056/NEJMoa1105358

RAS mutations in cutaneous squamous-cell carcinomas in patients treated with BRAF inhibitors

Fei Su
, Amaya Viros
, Carla Milagre
, Kerstin Trunzer
, Gideon Bollag
, Olivia Spleiss
, Jorge S. Reis-Filho
, Xiangju Kong
, Richard C. Koya
, Keith T. Flaherty
, Paul B. Chapman
, Min Jung Kim
, Robert Hayward
, Matthew Martin
, Hong Yang
, Qiongqing Wang
, Holly Hilton
, Julie S. Hang
, Johannes Noe
, Maryou Lambros

Felipe Geyer, Nathalie Dhomen, Ion Niculescu-Duvaz, Alfonso Zambon, Dan Niculescu-Duvaz, Natasha Preece, Lídia Robert, Nicholas J. Otte, Stephen Mok, Damien Kee, Yan Ma, Chao Zhang, Gaston Habets, Elizabeth A. Burton, Bernice Wong, Hoa Nguyen, Mark Kockx, Luc Andries, Brian Lestini, Keith B. Nolop, Richard J. Lee, Andrew K. Joe, James L. Troy, Rene Gonzalez, Thomas E. Hutson, Igor Puzanov, Bartosz Chmielowski, Caroline J. Springer, Grant A. McArthur, Jeffrey A. Sosman, Roger S. Lo, Antoni Ribas, Richard Marais

Medicine

University at Buffalo

Hoffmann-La Roche, Inc.
The Institute of Cancer Research
Autonomous University of Barcelona
F. Hoffmann-La Roche AG
Plexxikon, Inc.
University of California at Los Angeles
Massachusetts General Hospital
Memorial Sloan-Kettering Cancer Center
Peter Maccallum Cancer Centre
HistoGeneX NV
Medical College of Wisconsin
University of Colorado Anschutz Medical Campus
Baylor Health Care System
Vanderbilt University

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

973 Scopus citations

Abstract

BACKGROUND: Cutaneous squamous-cell carcinomas and keratoacanthomas are common findings in patients treated with BRAF inhibitors. METHODS: We performed a molecular analysis to identify oncogenic mutations (HRAS, KRAS, NRAS, CDKN2A, and TP53) in the lesions from patients treated with the BRAF inhibitor vemurafenib. An analysis of an independent validation set and functional studies with BRAF inhibitors in the presence of the prevalent RAS mutation was also performed. RESULTS: Among 21 tumor samples, 13 had RAS mutations (12 in HRAS). In a validation set of 14 samples, 8 had RAS mutations (4 in HRAS). Thus, 60% (21 of 35) of the specimens harbored RAS mutations, the most prevalent being HRAS Q61L. Increased proliferation of HRAS Q61L-mutant cell lines exposed to vemurafenib was associated with mitogen-activated protein kinase (MAPK)-pathway signaling and activation of ERK-mediated transcription. In a mouse model of HRAS Q61L-mediated skin carcinogenesis, the vemurafenib analogue PLX4720 was not an initiator or a promoter of carcinogenesis but accelerated growth of the lesions harboring HRAS mutations, and this growth was blocked by concomitant treatment with a MEK inhibitor. CONCLUSIONS: Mutations in RAS, particularly HRAS, are frequent in cutaneous squamous-cell carcinomas and keratoacanthomas that develop in patients treated with vemurafenib. The molecular mechanism is consistent with the paradoxical activation of MAPK signaling and leads to accelerated growth of these lesions. (Funded by Hoffmann-La Roche and others; ClinicalTrials.gov numbers, NCT00405587, NCT00949702, NCT01001299, and NCT01006980.)

Original language	English
Pages (from-to)	207-215
Number of pages	9
Journal	New England Journal of Medicine
Volume	366
Issue number	3
DOIs	https://doi.org/10.1056/NEJMoa1105358
State	Published - Jan 19 2012

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Su, F., Viros, A., Milagre, C., Trunzer, K., Bollag, G., Spleiss, O., Reis-Filho, J. S., Kong, X., Koya, R. C., Flaherty, K. T., Chapman, P. B., Kim, M. J., Hayward, R., Martin, M., Yang, H., Wang, Q., Hilton, H., Hang, J. S., Noe, J., ... Marais, R. (2012). RAS mutations in cutaneous squamous-cell carcinomas in patients treated with BRAF inhibitors. New England Journal of Medicine, 366(3), 207-215. https://doi.org/10.1056/NEJMoa1105358

@article{c35d5089d42a4462a2f63f8a7f147233,

title = "RAS mutations in cutaneous squamous-cell carcinomas in patients treated with BRAF inhibitors",

abstract = "BACKGROUND: Cutaneous squamous-cell carcinomas and keratoacanthomas are common findings in patients treated with BRAF inhibitors. METHODS: We performed a molecular analysis to identify oncogenic mutations (HRAS, KRAS, NRAS, CDKN2A, and TP53) in the lesions from patients treated with the BRAF inhibitor vemurafenib. An analysis of an independent validation set and functional studies with BRAF inhibitors in the presence of the prevalent RAS mutation was also performed. RESULTS: Among 21 tumor samples, 13 had RAS mutations (12 in HRAS). In a validation set of 14 samples, 8 had RAS mutations (4 in HRAS). Thus, 60\% (21 of 35) of the specimens harbored RAS mutations, the most prevalent being HRAS Q61L. Increased proliferation of HRAS Q61L-mutant cell lines exposed to vemurafenib was associated with mitogen-activated protein kinase (MAPK)-pathway signaling and activation of ERK-mediated transcription. In a mouse model of HRAS Q61L-mediated skin carcinogenesis, the vemurafenib analogue PLX4720 was not an initiator or a promoter of carcinogenesis but accelerated growth of the lesions harboring HRAS mutations, and this growth was blocked by concomitant treatment with a MEK inhibitor. CONCLUSIONS: Mutations in RAS, particularly HRAS, are frequent in cutaneous squamous-cell carcinomas and keratoacanthomas that develop in patients treated with vemurafenib. The molecular mechanism is consistent with the paradoxical activation of MAPK signaling and leads to accelerated growth of these lesions. (Funded by Hoffmann-La Roche and others; ClinicalTrials.gov numbers, NCT00405587, NCT00949702, NCT01001299, and NCT01006980.)",

author = "Fei Su and Amaya Viros and Carla Milagre and Kerstin Trunzer and Gideon Bollag and Olivia Spleiss and Reis-Filho, \{Jorge S.\} and Xiangju Kong and Koya, \{Richard C.\} and Flaherty, \{Keith T.\} and Chapman, \{Paul B.\} and Kim, \{Min Jung\} and Robert Hayward and Matthew Martin and Hong Yang and Qiongqing Wang and Holly Hilton and Hang, \{Julie S.\} and Johannes Noe and Maryou Lambros and Felipe Geyer and Nathalie Dhomen and Ion Niculescu-Duvaz and Alfonso Zambon and Dan Niculescu-Duvaz and Natasha Preece and L{\'i}dia Robert and Otte, \{Nicholas J.\} and Stephen Mok and Damien Kee and Yan Ma and Chao Zhang and Gaston Habets and Burton, \{Elizabeth A.\} and Bernice Wong and Hoa Nguyen and Mark Kockx and Luc Andries and Brian Lestini and Nolop, \{Keith B.\} and Lee, \{Richard J.\} and Joe, \{Andrew K.\} and Troy, \{James L.\} and Rene Gonzalez and Hutson, \{Thomas E.\} and Igor Puzanov and Bartosz Chmielowski and Springer, \{Caroline J.\} and McArthur, \{Grant A.\} and Sosman, \{Jeffrey A.\} and Lo, \{Roger S.\} and Antoni Ribas and Richard Marais",

year = "2012",

month = jan,

day = "19",

doi = "10.1056/NEJMoa1105358",

language = "English",

volume = "366",

pages = "207--215",

journal = "New England Journal of Medicine",

issn = "0028-4793",

publisher = "Massachussetts Medical Society",

number = "3",

}

Su, F, Viros, A, Milagre, C, Trunzer, K, Bollag, G, Spleiss, O, Reis-Filho, JS, Kong, X, Koya, RC, Flaherty, KT, Chapman, PB, Kim, MJ, Hayward, R, Martin, M, Yang, H, Wang, Q, Hilton, H, Hang, JS, Noe, J, Lambros, M, Geyer, F, Dhomen, N, Niculescu-Duvaz, I, Zambon, A, Niculescu-Duvaz, D, Preece, N, Robert, L, Otte, NJ, Mok, S, Kee, D, Ma, Y, Zhang, C, Habets, G, Burton, EA, Wong, B, Nguyen, H, Kockx, M, Andries, L, Lestini, B, Nolop, KB, Lee, RJ, Joe, AK, Troy, JL, Gonzalez, R, Hutson, TE, Puzanov, I, Chmielowski, B, Springer, CJ, McArthur, GA, Sosman, JA, Lo, RS, Ribas, A & Marais, R 2012, 'RAS mutations in cutaneous squamous-cell carcinomas in patients treated with BRAF inhibitors', New England Journal of Medicine, vol. 366, no. 3, pp. 207-215. https://doi.org/10.1056/NEJMoa1105358

TY - JOUR

T1 - RAS mutations in cutaneous squamous-cell carcinomas in patients treated with BRAF inhibitors

AU - Su, Fei

AU - Viros, Amaya

AU - Milagre, Carla

AU - Trunzer, Kerstin

AU - Bollag, Gideon

AU - Spleiss, Olivia

AU - Reis-Filho, Jorge S.

AU - Kong, Xiangju

AU - Koya, Richard C.

AU - Flaherty, Keith T.

AU - Chapman, Paul B.

AU - Kim, Min Jung

AU - Hayward, Robert

AU - Martin, Matthew

AU - Yang, Hong

AU - Wang, Qiongqing

AU - Hilton, Holly

AU - Hang, Julie S.

AU - Noe, Johannes

AU - Lambros, Maryou

AU - Geyer, Felipe

AU - Dhomen, Nathalie

AU - Niculescu-Duvaz, Ion

AU - Zambon, Alfonso

AU - Niculescu-Duvaz, Dan

AU - Preece, Natasha

AU - Robert, Lídia

AU - Otte, Nicholas J.

AU - Mok, Stephen

AU - Kee, Damien

AU - Ma, Yan

AU - Zhang, Chao

AU - Habets, Gaston

AU - Burton, Elizabeth A.

AU - Wong, Bernice

AU - Nguyen, Hoa

AU - Kockx, Mark

AU - Andries, Luc

AU - Lestini, Brian

AU - Nolop, Keith B.

AU - Lee, Richard J.

AU - Joe, Andrew K.

AU - Troy, James L.

AU - Gonzalez, Rene

AU - Hutson, Thomas E.

AU - Puzanov, Igor

AU - Chmielowski, Bartosz

AU - Springer, Caroline J.

AU - McArthur, Grant A.

AU - Sosman, Jeffrey A.

AU - Lo, Roger S.

AU - Ribas, Antoni

AU - Marais, Richard

PY - 2012/1/19

Y1 - 2012/1/19

N2 - BACKGROUND: Cutaneous squamous-cell carcinomas and keratoacanthomas are common findings in patients treated with BRAF inhibitors. METHODS: We performed a molecular analysis to identify oncogenic mutations (HRAS, KRAS, NRAS, CDKN2A, and TP53) in the lesions from patients treated with the BRAF inhibitor vemurafenib. An analysis of an independent validation set and functional studies with BRAF inhibitors in the presence of the prevalent RAS mutation was also performed. RESULTS: Among 21 tumor samples, 13 had RAS mutations (12 in HRAS). In a validation set of 14 samples, 8 had RAS mutations (4 in HRAS). Thus, 60% (21 of 35) of the specimens harbored RAS mutations, the most prevalent being HRAS Q61L. Increased proliferation of HRAS Q61L-mutant cell lines exposed to vemurafenib was associated with mitogen-activated protein kinase (MAPK)-pathway signaling and activation of ERK-mediated transcription. In a mouse model of HRAS Q61L-mediated skin carcinogenesis, the vemurafenib analogue PLX4720 was not an initiator or a promoter of carcinogenesis but accelerated growth of the lesions harboring HRAS mutations, and this growth was blocked by concomitant treatment with a MEK inhibitor. CONCLUSIONS: Mutations in RAS, particularly HRAS, are frequent in cutaneous squamous-cell carcinomas and keratoacanthomas that develop in patients treated with vemurafenib. The molecular mechanism is consistent with the paradoxical activation of MAPK signaling and leads to accelerated growth of these lesions. (Funded by Hoffmann-La Roche and others; ClinicalTrials.gov numbers, NCT00405587, NCT00949702, NCT01001299, and NCT01006980.)

AB - BACKGROUND: Cutaneous squamous-cell carcinomas and keratoacanthomas are common findings in patients treated with BRAF inhibitors. METHODS: We performed a molecular analysis to identify oncogenic mutations (HRAS, KRAS, NRAS, CDKN2A, and TP53) in the lesions from patients treated with the BRAF inhibitor vemurafenib. An analysis of an independent validation set and functional studies with BRAF inhibitors in the presence of the prevalent RAS mutation was also performed. RESULTS: Among 21 tumor samples, 13 had RAS mutations (12 in HRAS). In a validation set of 14 samples, 8 had RAS mutations (4 in HRAS). Thus, 60% (21 of 35) of the specimens harbored RAS mutations, the most prevalent being HRAS Q61L. Increased proliferation of HRAS Q61L-mutant cell lines exposed to vemurafenib was associated with mitogen-activated protein kinase (MAPK)-pathway signaling and activation of ERK-mediated transcription. In a mouse model of HRAS Q61L-mediated skin carcinogenesis, the vemurafenib analogue PLX4720 was not an initiator or a promoter of carcinogenesis but accelerated growth of the lesions harboring HRAS mutations, and this growth was blocked by concomitant treatment with a MEK inhibitor. CONCLUSIONS: Mutations in RAS, particularly HRAS, are frequent in cutaneous squamous-cell carcinomas and keratoacanthomas that develop in patients treated with vemurafenib. The molecular mechanism is consistent with the paradoxical activation of MAPK signaling and leads to accelerated growth of these lesions. (Funded by Hoffmann-La Roche and others; ClinicalTrials.gov numbers, NCT00405587, NCT00949702, NCT01001299, and NCT01006980.)

UR - https://www.scopus.com/pages/publications/84862908097

U2 - 10.1056/NEJMoa1105358

DO - 10.1056/NEJMoa1105358

M3 - Article

SN - 0028-4793

VL - 366

SP - 207

EP - 215

JO - New England Journal of Medicine

JF - New England Journal of Medicine

IS - 3

ER -

RAS mutations in cutaneous squamous-cell carcinomas in patients treated with BRAF inhibitors

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