TY - JOUR
T1 - Imatinib for melanomas harboring mutationally activated or amplified kit arising on mucosal, acral, and chronically sun-damaged skin
AU - Hodi, F. Stephen
AU - Corless, Christopher L.
AU - Giobbie-Hurder, Anita
AU - Fletcher, Jonathan A.
AU - Zhu, Meijun
AU - Marino-Enriquez, Adrian
AU - Friedlander, Philip
AU - Gonzalez, Rene
AU - Weber, Jeffrey S.
AU - Gajewski, Thomas F.
AU - O'Day, Steven J.
AU - Kim, Kevin B.
AU - Lawrence, Donald
AU - Flaherty, Keith T.
AU - Luke, Jason J.
AU - Collichio, Frances A.
AU - Ernstoff, Marc S.
AU - Heinrich, Michael C.
AU - Beadling, Carol
AU - Zukotynski, Katherine A.
AU - Yap, Jeffrey T.
AU - Van Den Abbeele, Annick D.
AU - Demetri, George D.
AU - Fisher, David E.
PY - 2013/9/10
Y1 - 2013/9/10
N2 - Purpose Amplifications and mutations in the KIT proto-oncogene in subsets of melanomas provide therapeutic opportunities. Patients and Methods We conducted a multicenter phase II trial of imatinib in metastatic mucosal, acral, or chronically sun-damaged (CSD) melanoma with KIT amplifications and/or mutations. Patients received imatinib 400 mg once per day or 400 mg twice per day if there was no initial response. Dose reductions were permitted for treatment-related toxicities. Additional oncogene mutation screening was performed by mass spectroscopy. Results Twenty-five patients were enrolled (24 evaluable). Eight patients (33%) had tumors with KIT mutations, 11 (46%) with KIT amplifications, and five (21%) with both. Median follow-up was 10.6 months (range, 3.7 to 27.1 months). Best overall response rate (BORR) was 29% (21% excluding nonconfirmed responses) with a two-stage 95% CI of 13% to 51%. BORR was significantly greater than the hypothesized null of 5% and statistically significantly different by mutation status (7 of 13 or 54% KIT mutated v 0% KIT amplified only). There were no statistical differences in rates of progression or survival by mutation status or by melanoma site. The overall disease control rate was 50% but varied significantly by KIT mutation status (77% mutated v 18% amplified). Four patients harbored pretreatment NRAS mutations, and one patient acquired increased KIT amplification after treatment. Conclusion Melanomas that arise on mucosal, acral, or CSD skin should be assessed for KIT mutations. Imatinib can be effective when tumors harbor KIT mutations, but not if KIT is amplified only. NRAS mutations and KIT copy number gain may be mechanisms of therapeutic resistance to imatinib.
AB - Purpose Amplifications and mutations in the KIT proto-oncogene in subsets of melanomas provide therapeutic opportunities. Patients and Methods We conducted a multicenter phase II trial of imatinib in metastatic mucosal, acral, or chronically sun-damaged (CSD) melanoma with KIT amplifications and/or mutations. Patients received imatinib 400 mg once per day or 400 mg twice per day if there was no initial response. Dose reductions were permitted for treatment-related toxicities. Additional oncogene mutation screening was performed by mass spectroscopy. Results Twenty-five patients were enrolled (24 evaluable). Eight patients (33%) had tumors with KIT mutations, 11 (46%) with KIT amplifications, and five (21%) with both. Median follow-up was 10.6 months (range, 3.7 to 27.1 months). Best overall response rate (BORR) was 29% (21% excluding nonconfirmed responses) with a two-stage 95% CI of 13% to 51%. BORR was significantly greater than the hypothesized null of 5% and statistically significantly different by mutation status (7 of 13 or 54% KIT mutated v 0% KIT amplified only). There were no statistical differences in rates of progression or survival by mutation status or by melanoma site. The overall disease control rate was 50% but varied significantly by KIT mutation status (77% mutated v 18% amplified). Four patients harbored pretreatment NRAS mutations, and one patient acquired increased KIT amplification after treatment. Conclusion Melanomas that arise on mucosal, acral, or CSD skin should be assessed for KIT mutations. Imatinib can be effective when tumors harbor KIT mutations, but not if KIT is amplified only. NRAS mutations and KIT copy number gain may be mechanisms of therapeutic resistance to imatinib.
UR - http://www.scopus.com/inward/record.url?scp=84881512367&partnerID=8YFLogxK
U2 - 10.1200/JCO.2012.47.7836
DO - 10.1200/JCO.2012.47.7836
M3 - Article
C2 - 23775962
AN - SCOPUS:84881512367
SN - 0732-183X
VL - 31
SP - 3182
EP - 3190
JO - Journal of Clinical Oncology
JF - Journal of Clinical Oncology
IS - 26
ER -