Surgery and Oncology

Хирургия и онкология

2949-5857

Publishing House ABV Press

241

10.17650/2220-3478-2018-8-1-34-41

ORIGINAL REPORTS

ОРИГИНАЛЬНЫЕ ИССЛЕДОВАНИЯ

Efficacy of first-line oxaliplatin-based chemotherapy regimens depending on the KRAS mutation status

Эффективность оксалиплатинсодержащих режимов химиотерапии 1-й линии в зависимости от мутационного статуса гена KRAS

https://orcid.org/0000-0001-5615-7806

Fedyanin

M. Yu.

Федянин

М. Ю.

Russian Federation

fedianinmu@mail.ru

El’snukaeva

Kh. Kh.-M.

Эльснукаева

Х. Х.-М.

Russian Federation

https://orcid.org/0000-0001-9864-3837

Pokataev

I. A.

Покатаев

И. А.

Russian Federation

https://orcid.org/0000-0003-2245-214X

Tryakin

A. A.

Трякин

А. А.

Russian Federation

Bulanov

A. A.

Буланов

А. А.

Russian Federation

Sekhina

O. V.

Сехина

О. В.

Russian Federation

Chekini

D. A.

Чекини

Д. А.

Russian Federation

Ignatova

E. O.

Игнатова

Е. О.

Russian Federation

https://orcid.org/0000-0002-9303-8379

Gordeev

S. S.

Гордеев

С. С.

Russian Federation

Budurova

M. D.

Будурова

М. Д.

Russian Federation

Mamedli

Мамедли

З.

Russian Federation

Podluzhnyy

D. V.

Подлужный

Д. В.

Russian Federation

Kozlov

N. A.

Козлов

Н. А.

Russian Federation

https://orcid.org/0000-0001-9807-2229

Tyulyandin

S. A.

Тюляндин

С. А.

Russian Federation

N.N. Blokhin National Medical Research Center of Oncology, Ministry of Health of RussiaФГБУ «Национальный медицинский исследовательский центр онкологии им. Н.Н. Блохина» Минздрава России

29052018

34412905201829052018

Copyright ©; 2018, Fedyanin M.Y., El’snukaeva K.K., Pokataev I.A., Tryakin A.A., Bulanov A.A., Sekhina O.V., Chekini D.A., Ignatova E.O., Gordeev S.S., Budurova M.D., Mamedli Z., Podluzhnyy D.V., Kozlov N.A., Tyulyandin S.A.

Copyright ©; 2018, Федянин М.Ю., Эльснукаева Х.Х., Покатаев И.А., Трякин А.А., Буланов А.А., Сехина О.В., Чекини Д.А., Игнатова Е.О., Гордеев С.С., Будурова М.Д., Мамедли З., Подлужный Д.В., Козлов Н.А., Тюляндин С.А.

2018

Fedyanin M.Y., El’snukaeva K.K., Pokataev I.A., Tryakin A.A., Bulanov A.A., Sekhina O.V., Chekini D.A., Ignatova E.O., Gordeev S.S., Budurova M.D., Mamedli Z., Podluzhnyy D.V., Kozlov N.A., Tyulyandin S.A.

Федянин М.Ю., Эльснукаева Х.Х., Покатаев И.А., Трякин А.А., Буланов А.А., Сехина О.В., Чекини Д.А., Игнатова Е.О., Гордеев С.С., Будурова М.Д., Мамедли З., Подлужный Д.В., Козлов Н.А., Тюляндин С.А.

https://creativecommons.org/licenses/by/4.0

https://onco-surgery.info/jour/article/view/241

Objective: to determine the efficacy of 2 oxaliplatin-based chemotherapy regimens (FOLFOX and XELOX) for metastatic colorectal cancer (CRC) depending on the KRAS mutation status and primary tumor location. Materials and methods. We performed retrospective analysis of the data on patients with metastatic CRC taken from a prospective database. We included patients with known KRAS mutation status that received either FOLFOX or XELOX without targeted drugs. Progression-free survival (PFS) was used as a main criterion in estimating treatment efficacy. Results. The inclusion criteria were met by 157 patients. The FOLFOX regimen was more effective in patients with wild-type KRAS CRC: median PFS was 10 months versus 8 months in the XELOX group (hazard ratio (HR) = 0.7; 95 % confidence interval (CI) 0.4–1.2; р = 0.1). However, we observed no significant differences in median life expectancy between these groups: it was 37 and 38 months respectively (HR = 1.1; 95 % CI 0.6–2.1; p = 0.6). Similar trends were observed in patients bearing KRAS mutations: median PFS in the FOLFOX group was 9 months vs 5 months in the XELOX group (HR = 0.6; 95 % CI 0.3–1.2; р = 0.1; p value by Breslow – Day test = 0.04). No differences in median life expectancy between these groups were observed: 33 and 23 months respectively (HR = 0.8; 95 % CI 0.4–1.6; p = 0.5). Conclusion. We failed to find an association between the KRAS mutation status and response to a particular chemotherapy regimen. We found that patients with metastatic CRC receiving the FOLFOX regimen were more likely to achieve objective responses and demonstrated higher median PFS than patients on the XELOX regimen.

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