Czech Experience with Crizotinib in the Personalized Treatment of NSCLC

Kolek, Vitezslav; Pesek, Milos; Skřičková,  Jana; Grygarkova, Ivona; Roubec, Jaromir; Koubkova, Leona; Cernovska, Marketa; Hejduk,  Karel

Czech Experience with Crizotinib in the Personalized Treatment of NSCLC

Autoři	KOLEK Vitezslav PESEK Milos SKŘIČKOVÁ Jana GRYGARKOVA Ivona ROUBEC Jaromir KOUBKOVA Leona CERNOVSKA Marketa HEJDUK Karel
Rok publikování	2015
Druh	Konferenční abstrakty
Fakulta / Pracoviště MU	Lékařská fakulta
Citace
Popis	Background: Crizotinib is a highly selective drug used in the treatment of anaplastic lymphoma kinase (ALK) gene re-arrangement positive non-small cell lung cancer (NSCLC). In the Czech Republic it was used in frame of compassionate cases program and now is reimbursed in pretreated tumors with EML 4/ALK gen translocation verified by FISH and/or IHC testing. The recommended dose is 250 mg bid/ day. Crizotinib is used since 2011, data are evaluated according to the National Reference Centre Registry. Methods: Present study evaluates 26 patients (pts), 14 males,12 females with mean age 60 (31- 75) years. Out of them 11 (42.3%) were non-smokers, 8 (30.8%) ex-smokers and 7 (26.9 %) smokers. All of them had NSCLC with EML4/ALK gene translocation, 23 had adenocarcinoma, two NOS and one patient had adenosquamous cancer. Stage in the time of treatment was IIIB in 3 and IV in 23 pts. Crizotinib was applied in 2nd line in 17 pts, 3rd line in 5 pts, 4th line in 3 pts, 5th in one patient. PS was 0 in 3 pts, 1 in 20 pts and 2 in 3 pts. Results: On the date of evaluation, 14 pts continued the treatment, 6 died and 6 stopped treatment due to progression. Crizotinib effectiveness was assessed in 15 pts: CR in 3 (20%) pts, PR in 3 (20%) pts, SD in 5 (33.3 %) pts, DP in 4 (26.7 %) pts. CR was associated with long response duration (10.7, 31.8, 34.1 months). Grade 3 adverse events (gastrointenstinal discomfort and liver disease) were observed in two (7.7 %) pts, grade 2 problems with visus appeared in two patients. Dose of crizotinib was reduced in 3 pts. Median of progression free survival was 15 months, median of overall survival was not reached. Conclusion: Interim analysis of present series shows, that crizotinib has very good tolerability and promising effectiveness even in heavily pretreated patients with EML4/ALK gene translocation. Long term survival analysis is running.