@article{21566, author = {Kanetsky P. and Dwyer T and Orlow I. and Luo L. and Kricker A. and Armstrong B. and Anton-Culver H. and Gruber S. and Marrett L. and Gallagher R. and Zanetti R. and Rosso S. and From L. and Busam K. and Cust A. and Ollila D. and Begg C. and Berwick M. and Thomas N. and Edmiston S. and Alexander A. and Groben P. and Parrish E. and Hao H. and Reiner A. and Paine S. and Frank J. and Bramson J. and Conway K.}, title = {Association Between and Mutational Status and Melanoma-Specific Survival Among Patients With Higher Risk Primary Melanoma}, abstract = {

IMPORTANCE: NRAS and BRAF mutations in melanoma inform current treatment paradigms but their role in survival from primary melanoma has not been established. Identification of patients at high risk of melanoma-related death based on their primary melanoma characteristics before evidence of recurrence could inform recommendations for patient follow-up and eligibility for adjuvant trials. OBJECTIVE: To determine tumor characteristics and survival from primary melanoma by somatic NRAS and BRAF status. DESIGN SETTING AND PARTICIPANTS: A population-based study with median follow-up of 7.6 years for 912 patients with first primary cutaneous melanoma analyzed for NRAS and BRAF mutations diagnosed in the year 2000 from the United States and Australia in the Genes, Environment and Melanoma Study and followed through 2007. MAIN OUTCOMES AND MEASURES: Tumor characteristics and melanoma-specific survival of primary melanoma by NRAS and BRAF mutational status. RESULTS: The melanomas were 13% NRAS+, 30% BRAF+, and 57% with neither NRAS nor BRAF mutation (wildtype). In a multivariable model including clinicopathologic characteristics, NRAS+ melanoma was associated (P<.05) with mitoses, lower tumor infiltrating lymphocyte (TIL) grade, and anatomic site other than scalp/neck and BRAF+ melanoma was associated with younger age, superficial spreading subtype, and mitoses, relative to wildtype melanoma. There was no significant difference in melanoma-specific survival for melanoma harboring mutations in NRAS (HR 1.7, 95% CI, 0.8-3.4) or BRAF (HR, 1.5, 95% CI, 0.8-2.9) compared to wildtype melanoma adjusted for age, sex, site, AJCC tumor stage, TIL grade, and study center. However, melanoma-specific survival was significantly poorer for higher risk (T2b or higher stage) tumors with NRAS (HR 2.9; 95% CI 1.1-7.7) or BRAF (HR 3.1; 95% CI 1.2-8.5) mutations but not for lower risk (T2a or lower) tumors (P=.65) adjusted for age, sex, site, AJCC tumor stage, TIL grade, and study center. CONCLUSIONS AND RELEVANCE: Lower TIL grade for NRAS+ melanoma suggests it has a more immunosuppressed microenvironment, which may impact its response to immunotherapies. Further, the approximately three-fold increased death rate for higher risk tumors harboring NRAS or BRAF mutations compared to wildtype melanomas after adjusting for other prognostic factors indicates that the prognostic implication of NRAS and BRAF mutations deserves further investigation, particularly in higher AJCC stage primary melanomas.

}, year = {2015}, journal = {JAMA Oncology}, volume = {1}, edition = {2015/07/07}, number = {3}, pages = {359-368}, isbn = {2374-2437 (Print)}, note = {Thomas, Nancy E
Edmiston, Sharon N
Alexander, Audrey
Groben, Pamela A
Parrish, Eloise
Kricker, Anne
Armstrong, Bruce K
Anton-Culver, Hoda
Gruber, Stephen B
From, Lynn
Busam, Klaus J
Hao, Honglin
Orlow, Irene
Kanetsky, Peter A
Luo, Li
Reiner, Anne S
Paine, Susan
Frank, Jill S
Bramson, Jennifer I
Marrett, Lorraine D
Gallagher, Richard P
Zanetti, Roberto
Rosso, Stefano
Dwyer, Terence
Cust, Anne E
Ollila, David W
Begg, Colin B
Berwick, Marianne
Conway, Kathleen
P30 CA016086/CA/NCI NIH HHS/United States
R01 CA112243/CA/NCI NIH HHS/United States
R33 CA160138/CA/NCI NIH HHS/United States
JAMA Oncol. 2015 Jun;1(3):359-368.}, language = {Eng}, }