BRAF, NRAS and C-KIT Advanced Melanoma: Clinico-pathological Features, Targeted-Therapy Strategies and Survival

被引:48
作者
Ponti, Giovanni [1 ]
Manfredini, Marco [1 ]
Greco, Stefano [2 ]
Pellacani, Giovanni [1 ]
Depenni, Roberta [2 ]
Tomasi, Aldo [3 ]
Maccaferri, Monia [1 ]
Cascinu, Stefano [2 ]
机构
[1] Univ Modena & Reggio Emilia, Dept Surg Med Dent & Morphol Sci Interest Transpl, Modena, Italy
[2] Univ Modena & Reggio Emilia, Dept Oncol, Modena, Italy
[3] Univ Modena & Reggio Emilia, Dept Diagnost & Clin Med & Publ Hlth, Modena, Italy
关键词
Advanced melanoma; targeted therapies; survival; BRAF; NRAS and C-KIT;
D O I
10.21873/anticanres.12175
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Background/Aim: The mutational status of stage III and IV melanomas should be recognized in order to allow for targeted therapies. The aim of our study was the characterization of BRAF, NRAS and C-KIT melanoma patients, in order to define their optimal management. Patients and Methods: Between 1991 and 2015, 63 mutated melanoma patients were treated and monitored during their diagnostic and therapeutic management at a single institution. Results: BRAF-mutated melanoma patients were the most common, representing 70% of the study population, while NRAS-and C-KIT-mutated melanoma represented 19% and 11% respectively. BRAF-mutated melanomas were mostly located at sites of intermittent sun exposure, and were associated with higher Breslow thickness and an increased number of mitosis. NRAS mutated melanoma were mainly observed in chronic sun-damaged areas and had a negative prognostic value, with shorter time to progression and a high incidence of central nervous system involvement. C-KIT mutated melanoma were located at acral and mucosal sites. Overall survival observed in the three groups of patients revealed wide differences. Conclusion: BRAF, NRAS and C-KIT melanomas constitute distinct clinico-pathological entities. BRAF-mutated melanoma benefit from both anti-BRAF and anti-MEK targeted therapies while triple-negative melanomas could benefit from novel anti-CTLA-4 and anti-PD-L1 immunotherapeutic approaches.
引用
收藏
页码:7043 / 7048
页数:6
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