Real-World Outcomes in BRAF-Mutant Non-small Cell Lung Cancer: A Multicenter Analysis From the Turkish Oncology Group

Tuğba Akın Telli; Ali Murat Tatlı; Özkan Alan; Gülsema Yıldıran Keskin; Nuri Karadurmuş; Serdar Karakaya; Muhammet Ali Kaplan; Özgür Açıkgöz; Ahmet Bilici; Eda Eylemer Mocan; Ahmet Demirkazık; Seda Kahraman; Mehmet A.N. Şendur; Mutlu Doğan; Meltem Topalgökçeli Selam; Özlem Er; Oktay Ünsal; Ozan Yazıcı; Erkan Özcan; Ayşegül Kargı; Mustafa Gürbüz; Fatih Selçukbiricik; Teoman Şakalar; Pınar Gürsoy; Burak Bilgin; Oğuzhan Selvi; İbrahim Karadağ; Orhan Önder Eren; Ertuğrul Bayram; Ahmet Taner Sümbül; Serkan Keskin; Akın Öztürk; Sevgi Topçu; Miraç Özen; Saadettin Kılıçkap; Perran Fulden Yumuk

doi:10.1016/j.cllc.2025.07.015

Real-World Outcomes in BRAF-Mutant Non-small Cell Lung Cancer: A Multicenter Analysis From the Turkish Oncology Group

Tuğba Akın Telli
, Ali Murat Tatlı
, Özkan Alan
, Gülsema Yıldıran Keskin
, Nuri Karadurmuş
, Serdar Karakaya
, Muhammet Ali Kaplan
, Özgür Açıkgöz
, Ahmet Bilici
, Eda Eylemer Mocan
, Ahmet Demirkazık
, Seda Kahraman
, Mehmet A.N. Şendur
, Mutlu Doğan
, Meltem Topalgökçeli Selam
, Özlem Er
, Oktay Ünsal
, Ozan Yazıcı
, Erkan Özcan
, Ayşegül Kargı

Mustafa Gürbüz, Fatih Selçukbiricik, Teoman Şakalar, Pınar Gürsoy, Burak Bilgin, Oğuzhan Selvi, İbrahim Karadağ, Orhan Önder Eren, Ertuğrul Bayram, Ahmet Taner Sümbül, Serkan Keskin, Akın Öztürk, Sevgi Topçu, Miraç Özen, Saadettin Kılıçkap, Perran Fulden Yumuk

Istanbul Bilim University
Akdeniz University
Istanbul University - Cerrahpaşa
Gülhane Military Medical Academy
Department of Neurosurgery
Dicle University
Istanbul Medipol University
Ankara University
Yildirim Beyazit Universitesi
Ankara Oncology Education and Research Hospital
Liv Hospital Ulus
Acibadem Mehmet Ali Aydinlar Universitesi
Gazi University
Trakya University
Medstar Hospital
Baskent University
Koc University
Kahramanmaraş Necip Fazıl City Hospital
Ege University
Konya City Hospital
University of Health Sciences
Hitit University
Selcuk University
Cukurova University
Medical Park Hospital
Memorial Şişli Hospital
Süreyyapaşa Chest Diseases and Thoracic Surgery Training and Research Hospital
Osmaniye State Hospital
Sakarya University
Istinye University

Araştırma sonucu: Dergiye katkı › Makale › bilirkişi

2 Alıntılar (Scopus)

Özet

Background Real-world data on BRAF-mutant non-small cell lung cancer (NSCLC) remain limited, particularly regarding outcomes with dabrafenib plus trametinib ( D + T ). Methods This multicenter retrospective study included 88 patients with advanced BRAF-mutant NSCLC treated across 30 centers. Clinicopathologic characteristics, treatment outcomes, and safety data were collected and analyzed. Patients received either chemotherapy or dabrafenib plus trametinib in the first-line or subsequent settings. Progression-free survival (PFS), overall survival (OS), and objective response rates (ORR) were compared across treatment groups. Results Among 88 patients (78 V600E, 10 non-V600E), median age was 64 years. Co-mutations were more frequent in non-V600E cases (40% vs. 10%). Brain metastases were more frequent in non-V600E cases (60% vs. 15%, p = .001). First-line D + T was associated with superior ORR (67% vs. 39%, p = .02), DCR (81% vs. 51%, p = .009), and PFS (median 13.1 vs. 6.1 months, p = .007) compared to chemotherapy, while OS was similar between groups. Among chemotherapy regimens, platinum-pemetrexed outperformed platinum-taxane in terms of ORR (77% vs. 33%, p = .006) and PFS (median 14.7 vs. 3.2 months, p = .002). No significant differences in efficacy were observed between first-line and later-line use of D + T . Co-mutations were associated with shorter OS (median 8.7 vs. 20.2 months, p = .009). PD-L1 status and BRAF subtype did not impact OS. Median treatment duration with D + T was 10.6 months, with treatment-related adverse events occurring in 61% of patients, most commonly fatigue and pyrexia. Conclusions In this real-world cohort, dabrafenib plus trametinib was associated with superior response rates and PFS compared to chemotherapy in the first-line setting. Presence of co-mutations was associated with poorer outcomes.

Orijinal dil	İngilizce
Sayfa (başlangıç-bitiş)	e649-e659
Dergi	Clinical Lung Cancer
Hacim	26
Basın numarası	8
DOI'lar	https://doi.org/10.1016/j.cllc.2025.07.015
Yayın durumu	Yayınlandı - Ara 2025
Harici olarak yayınlandı	Evet

BM SKH

Bu sonuç, aşağıdaki Sürdürülebilir Kalkınma Hedefine/Hedeflerine katkıda bulunur

SKH 3 Sağlık ve Kaliteli Yaşam

Belgeye Erişim

10.1016/j.cllc.2025.07.015

Diger dosyalar ve linkler

Link to publication in Scopus

Bundan alıntı yap

Telli, T. A., Tatlı, A. M., Alan, Ö., Keskin, G. Y., Karadurmuş, N., Karakaya, S., Kaplan, M. A., Açıkgöz, Ö., Bilici, A., Mocan, E. E., Demirkazık, A., Kahraman, S., Şendur, M. A. N., Doğan, M., Selam, M. T., Er, Ö., Ünsal, O., Yazıcı, O., Özcan, E., ... Yumuk, P. F. (2025). Real-World Outcomes in BRAF-Mutant Non-small Cell Lung Cancer: A Multicenter Analysis From the Turkish Oncology Group. Clinical Lung Cancer, 26(8), e649-e659. https://doi.org/10.1016/j.cllc.2025.07.015

@article{38bcc9e66c6b43ee9eb62f53be1761d5,

title = "Real-World Outcomes in BRAF-Mutant Non-small Cell Lung Cancer: A Multicenter Analysis From the Turkish Oncology Group",

abstract = "Background Real-world data on BRAF-mutant non-small cell lung cancer (NSCLC) remain limited, particularly regarding outcomes with dabrafenib plus trametinib ( D + T ). Methods This multicenter retrospective study included 88 patients with advanced BRAF-mutant NSCLC treated across 30 centers. Clinicopathologic characteristics, treatment outcomes, and safety data were collected and analyzed. Patients received either chemotherapy or dabrafenib plus trametinib in the first-line or subsequent settings. Progression-free survival (PFS), overall survival (OS), and objective response rates (ORR) were compared across treatment groups. Results Among 88 patients (78 V600E, 10 non-V600E), median age was 64 years. Co-mutations were more frequent in non-V600E cases (40\% vs. 10\%). Brain metastases were more frequent in non-V600E cases (60\% vs. 15\%, p = .001). First-line D + T was associated with superior ORR (67\% vs. 39\%, p = .02), DCR (81\% vs. 51\%, p = .009), and PFS (median 13.1 vs. 6.1 months, p = .007) compared to chemotherapy, while OS was similar between groups. Among chemotherapy regimens, platinum-pemetrexed outperformed platinum-taxane in terms of ORR (77\% vs. 33\%, p = .006) and PFS (median 14.7 vs. 3.2 months, p = .002). No significant differences in efficacy were observed between first-line and later-line use of D + T . Co-mutations were associated with shorter OS (median 8.7 vs. 20.2 months, p = .009). PD-L1 status and BRAF subtype did not impact OS. Median treatment duration with D + T was 10.6 months, with treatment-related adverse events occurring in 61\% of patients, most commonly fatigue and pyrexia. Conclusions In this real-world cohort, dabrafenib plus trametinib was associated with superior response rates and PFS compared to chemotherapy in the first-line setting. Presence of co-mutations was associated with poorer outcomes.",

keywords = "BRAF mutation, BRAFV600E, Dabrafenib, Real-life, Trametinib",

author = "Telli, \{Tuğba Akın\} and Tatlı, \{Ali Murat\} and {\"O}zkan Alan and Keskin, \{G{\"u}lsema Yıldıran\} and Nuri Karadurmu{\c s} and Serdar Karakaya and Kaplan, \{Muhammet Ali\} and {\"O}zg{\"u}r A{\c c}ıkg{\"o}z and Ahmet Bilici and Mocan, \{Eda Eylemer\} and Ahmet Demirkazık and Seda Kahraman and {\c S}endur, \{Mehmet A.N.\} and Mutlu Doğan and Selam, \{Meltem Topalg{\"o}k{\c c}eli\} and {\"O}zlem Er and Oktay {\"U}nsal and Ozan Yazıcı and Erkan {\"O}zcan and Ay{\c s}eg{\"u}l Kargı and Mustafa G{\"u}rb{\"u}z and Fatih Sel{\c c}ukbiricik and Teoman {\c S}akalar and Pınar G{\"u}rsoy and Burak Bilgin and Oğuzhan Selvi and İbrahim Karadağ and Eren, \{Orhan {\"O}nder\} and Ertuğrul Bayram and S{\"u}mb{\"u}l, \{Ahmet Taner\} and Serkan Keskin and Akın {\"O}zt{\"u}rk and Sevgi Top{\c c}u and Mira{\c c} {\"O}zen and Saadettin Kılı{\c c}kap and Yumuk, \{Perran Fulden\}",

note = "Publisher Copyright: {\textcopyright} 2025 Elsevier Inc.",

year = "2025",

month = dec,

doi = "10.1016/j.cllc.2025.07.015",

language = "English",

volume = "26",

pages = "e649--e659",

journal = "Clinical Lung Cancer",

issn = "1525-7304",

publisher = "Elsevier Inc.",

number = "8",

}

Telli, TA, Tatlı, AM, Alan, Ö, Keskin, GY, Karadurmuş, N, Karakaya, S, Kaplan, MA, Açıkgöz, Ö, Bilici, A, Mocan, EE, Demirkazık, A, Kahraman, S, Şendur, MAN, Doğan, M, Selam, MT, Er, Ö, Ünsal, O, Yazıcı, O, Özcan, E, Kargı, A, Gürbüz, M, Selçukbiricik, F, Şakalar, T, Gürsoy, P, Bilgin, B, Selvi, O, Karadağ, İ, Eren, OÖ, Bayram, E, Sümbül, AT, Keskin, S, Öztürk, A, Topçu, S, Özen, M, Kılıçkap, S & Yumuk, PF 2025, 'Real-World Outcomes in BRAF-Mutant Non-small Cell Lung Cancer: A Multicenter Analysis From the Turkish Oncology Group', Clinical Lung Cancer, hac. 26, no. 8, pp. e649-e659. https://doi.org/10.1016/j.cllc.2025.07.015

TY - JOUR

T1 - Real-World Outcomes in BRAF-Mutant Non-small Cell Lung Cancer

T2 - A Multicenter Analysis From the Turkish Oncology Group

AU - Telli, Tuğba Akın

AU - Tatlı, Ali Murat

AU - Alan, Özkan

AU - Keskin, Gülsema Yıldıran

AU - Karadurmuş, Nuri

AU - Karakaya, Serdar

AU - Kaplan, Muhammet Ali

AU - Açıkgöz, Özgür

AU - Bilici, Ahmet

AU - Mocan, Eda Eylemer

AU - Demirkazık, Ahmet

AU - Kahraman, Seda

AU - Şendur, Mehmet A.N.

AU - Doğan, Mutlu

AU - Selam, Meltem Topalgökçeli

AU - Er, Özlem

AU - Ünsal, Oktay

AU - Yazıcı, Ozan

AU - Özcan, Erkan

AU - Kargı, Ayşegül

AU - Gürbüz, Mustafa

AU - Selçukbiricik, Fatih

AU - Şakalar, Teoman

AU - Gürsoy, Pınar

AU - Bilgin, Burak

AU - Selvi, Oğuzhan

AU - Karadağ, İbrahim

AU - Eren, Orhan Önder

AU - Bayram, Ertuğrul

AU - Sümbül, Ahmet Taner

AU - Keskin, Serkan

AU - Öztürk, Akın

AU - Topçu, Sevgi

AU - Özen, Miraç

AU - Kılıçkap, Saadettin

AU - Yumuk, Perran Fulden

PY - 2025/12

Y1 - 2025/12

N2 - Background Real-world data on BRAF-mutant non-small cell lung cancer (NSCLC) remain limited, particularly regarding outcomes with dabrafenib plus trametinib ( D + T ). Methods This multicenter retrospective study included 88 patients with advanced BRAF-mutant NSCLC treated across 30 centers. Clinicopathologic characteristics, treatment outcomes, and safety data were collected and analyzed. Patients received either chemotherapy or dabrafenib plus trametinib in the first-line or subsequent settings. Progression-free survival (PFS), overall survival (OS), and objective response rates (ORR) were compared across treatment groups. Results Among 88 patients (78 V600E, 10 non-V600E), median age was 64 years. Co-mutations were more frequent in non-V600E cases (40% vs. 10%). Brain metastases were more frequent in non-V600E cases (60% vs. 15%, p = .001). First-line D + T was associated with superior ORR (67% vs. 39%, p = .02), DCR (81% vs. 51%, p = .009), and PFS (median 13.1 vs. 6.1 months, p = .007) compared to chemotherapy, while OS was similar between groups. Among chemotherapy regimens, platinum-pemetrexed outperformed platinum-taxane in terms of ORR (77% vs. 33%, p = .006) and PFS (median 14.7 vs. 3.2 months, p = .002). No significant differences in efficacy were observed between first-line and later-line use of D + T . Co-mutations were associated with shorter OS (median 8.7 vs. 20.2 months, p = .009). PD-L1 status and BRAF subtype did not impact OS. Median treatment duration with D + T was 10.6 months, with treatment-related adverse events occurring in 61% of patients, most commonly fatigue and pyrexia. Conclusions In this real-world cohort, dabrafenib plus trametinib was associated with superior response rates and PFS compared to chemotherapy in the first-line setting. Presence of co-mutations was associated with poorer outcomes.

AB - Background Real-world data on BRAF-mutant non-small cell lung cancer (NSCLC) remain limited, particularly regarding outcomes with dabrafenib plus trametinib ( D + T ). Methods This multicenter retrospective study included 88 patients with advanced BRAF-mutant NSCLC treated across 30 centers. Clinicopathologic characteristics, treatment outcomes, and safety data were collected and analyzed. Patients received either chemotherapy or dabrafenib plus trametinib in the first-line or subsequent settings. Progression-free survival (PFS), overall survival (OS), and objective response rates (ORR) were compared across treatment groups. Results Among 88 patients (78 V600E, 10 non-V600E), median age was 64 years. Co-mutations were more frequent in non-V600E cases (40% vs. 10%). Brain metastases were more frequent in non-V600E cases (60% vs. 15%, p = .001). First-line D + T was associated with superior ORR (67% vs. 39%, p = .02), DCR (81% vs. 51%, p = .009), and PFS (median 13.1 vs. 6.1 months, p = .007) compared to chemotherapy, while OS was similar between groups. Among chemotherapy regimens, platinum-pemetrexed outperformed platinum-taxane in terms of ORR (77% vs. 33%, p = .006) and PFS (median 14.7 vs. 3.2 months, p = .002). No significant differences in efficacy were observed between first-line and later-line use of D + T . Co-mutations were associated with shorter OS (median 8.7 vs. 20.2 months, p = .009). PD-L1 status and BRAF subtype did not impact OS. Median treatment duration with D + T was 10.6 months, with treatment-related adverse events occurring in 61% of patients, most commonly fatigue and pyrexia. Conclusions In this real-world cohort, dabrafenib plus trametinib was associated with superior response rates and PFS compared to chemotherapy in the first-line setting. Presence of co-mutations was associated with poorer outcomes.

KW - BRAF mutation

KW - BRAFV600E

KW - Dabrafenib

KW - Real-life

KW - Trametinib

UR - https://www.scopus.com/pages/publications/105013151370

U2 - 10.1016/j.cllc.2025.07.015

DO - 10.1016/j.cllc.2025.07.015

M3 - Article

C2 - 40813186

AN - SCOPUS:105013151370

SN - 1525-7304

VL - 26

SP - e649-e659

JO - Clinical Lung Cancer

JF - Clinical Lung Cancer

IS - 8

ER -

Real-World Outcomes in BRAF-Mutant Non-small Cell Lung Cancer: A Multicenter Analysis From the Turkish Oncology Group

Özet

BM SKH

Belgeye Erişim

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