Literature DB >> 21615881

Clinical outcome and pathological features associated with NRAS mutation in cutaneous melanoma.

Bianca Devitt1, Wendy Liu, Renato Salemi, Rory Wolfe, John Kelly, Chin-Yuan Tzen, Alexander Dobrovic, Grant McArthur.   

Abstract

The effect of NRAS mutations on the pathological features and clinical outcomes in patients with cutaneous melanoma was compared with that of tumors containing BRAF(V600E) mutations and tumors wild type for both (WT). Clinical outcome data were obtained from a prospective cohort of 249 patients. Mutations involving NRAS and BRAF(V600E) were detected by PCR and were sequence verified. Cox proportional hazards regression was performed to relate NRAS and BRAF mutations to clinical outcome. Seventy-five percentage of NRAS mutations occurred in tumors >1 mm thick (BRAF(V600E) 40%, WT 34%); 75% of NRAS mutations had >1 mitosis/mm(2) (BRAF(V600E) 40%, WT 55%). When compared to WT, multivariate analysis of melanoma-specific survival (MSS) identified NRAS mutations as an adverse prognostic factor [hazard ratio (HR) 2.96; P = 0.04] but not BRAF(V600E) mutations (HR 1.73; P = 0.23). NRAS mutations were associated with thicker tumors and higher rates of mitosis when compared to BRAF(V600E) and WT melanoma and independently of this, with shorter MSS.
© 2011 John Wiley & Sons A/S.

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Year:  2011        PMID: 21615881     DOI: 10.1111/j.1755-148X.2011.00873.x

Source DB:  PubMed          Journal:  Pigment Cell Melanoma Res        ISSN: 1755-1471            Impact factor:   4.693


  92 in total

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Journal:  Cancer       Date:  2011-12-16       Impact factor: 6.860

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Review 3.  Driver mutations in melanoma: lessons learned from bench-to-bedside studies.

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Review 4.  Recent advances in the treatment of melanoma with BRAF and MEK inhibitors.

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Review 5.  Molecular targets in melanoma: time for 'ethnic personalization'.

Authors:  Shane Y Morita; Svetomir N Markovic
Journal:  Expert Rev Anticancer Ther       Date:  2012-05       Impact factor: 4.512

Review 6.  Searching for the Chokehold of NRAS Mutant Melanoma.

Authors:  Christian Posch; Igor Vujic; Babak Monshi; Martina Sanlorenzo; Felix Weihsengruber; Klemens Rappersberger; Susana Ortiz-Urda
Journal:  J Invest Dermatol       Date:  2016-05-07       Impact factor: 8.551

7.  BRAF Inhibitors Amplify the Proapoptotic Activity of MEK Inhibitors by Inducing ER Stress in NRAS-Mutant Melanoma.

Authors:  Heike Niessner; Tobias Sinnberg; Corinna Kosnopfel; Keiran S M Smalley; Daniela Beck; Christian Praetorius; Marion Mai; Stefan Beissert; Dagmar Kulms; Martin Schaller; Claus Garbe; Keith T Flaherty; Dana Westphal; Ines Wanke; Friedegund Meier
Journal:  Clin Cancer Res       Date:  2017-07-19       Impact factor: 12.531

8.  Outcomes after progression of disease with anti-PD-1/PD-L1 therapy for patients with advanced melanoma.

Authors:  James R Patrinely; Laura X Baker; Elizabeth J Davis; Haocan Song; Fei Ye; Douglas B Johnson
Journal:  Cancer       Date:  2020-05-28       Impact factor: 6.860

9.  Inhibition of Wee1, AKT, and CDK4 underlies the efficacy of the HSP90 inhibitor XL888 in an in vivo model of NRAS-mutant melanoma.

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Journal:  Mol Cancer Ther       Date:  2013-03-28       Impact factor: 6.261

Review 10.  NRAS mutant melanoma: biological behavior and future strategies for therapeutic management.

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Journal:  Oncogene       Date:  2012-10-15       Impact factor: 9.867

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