Amivantamab plus lazertinib versus osimertinib in first-line EGFR-mutant advanced non-small-cell lung cancer with biomarkers of high-risk disease: a secondary analysis from MARIPOSA

被引：16

作者：

Felip, E. ^{[1
]}

Cho, B. C. ^{[2
]}

Gutierrez, V ^{[3
]}

Alip, A. ^{[4
]}

Besse, B. ^{[5
]}

Lu, S. ^{[6
]}

Spira, A. I. ^{[7
]}

Girard, N. ^{[8
,9
]}

Califano, R. ^{[10
,11
]}

Gadgeel, S. M. ^{[12
]}

Yang, J. C-H. ^{[13
,14
]}

Yamamoto, S. ^{[15
]}

Azuma, K. ^{[16
]}

Kim, Y. J. ^{[17
]}

Lee, K. -H. ^{[18
]}

Danchaivijitr, P. ^{[19
]}

Ferreira, C. G. ^{[20
]}

Cheng, Y. ^{[21
]}

Sendur, M. A. N. ^{[22
,23
]}

Chang, G. -C. ^{[24
,25
,26
]}

Wang, C. -C. ^{[27
]}

Prabhash, K. ^{[28
]}

Shinno, Y. ^{[29
]}

Stroyakovskiy, D. ^{[30
]}

Paz-Ares, L. ^{[31
,32
]}

Rodriguez-Cid, J. R. ^{[33
]}

Martin, C. ^{[34
,35
]}

Campelo, M. R. G. ^{[36
]}

Hayashi, H. ^{[37
]}

Nguyen, D. ^{[38
]}

Tomasini, P. ^{[39
]}

Gottfried, M. ^{[40
]}

Dooms, C. ^{[41
]}

Passaro, A. ^{[42
]}

Schuler, M. ^{[43
]}

Gelatti, A. C. Z. ^{[44
]}

Owen, S. ^{[45
]}

Perdrizet, K. ^{[46
]}

Ou, S. -H. I. ^{[47
]}

Curtin, J. C. ^{[48
]}

Zhang, J. ^{[48
]}

Gormley, M. ^{[48
]}

Sun, T. ^{[49
]}

Panchal, A. ^{[50
]}

Ennis, M. ^{[48
]}

Fennema, E. ^{[51
]}

Bauml, J. M. ^{[48
]}

Daksh, M. ^{[49
]}

Sethi, S. ^{[48
]}

Lee, S. -H. ^{[52
]}

机构：

[1] Univ Autonoma Barcelona, Vall dHebron Barcelona Hosp Campus, Vall dHebron Inst Oncol VHIO, Med Oncol Serv, Barcelona, Spain

[2] Yonsei Univ, Coll Med, Yonsei Canc Ctr, Div Med Oncol, Seoul, South Korea

[3] Hosp Reg Univ Malaga y Virgen Victoria, Med Oncol Dept, IBIMA, Malaga, Spain

[4] Univ Malaya, Fac Med, Clin Oncol Unit, Kuala Lumpur, Malaysia

[5] Paris Saclay Univ, Gustave Roussy, Villejuif, France

[6] Shanghai Jiao Tong Univ, Shanghai Chest Hosp, Shanghai Lung Canc Ctr, Sch Med, Shanghai, Peoples R China

[7] Virginia Canc Specialists, Fairfax, VA USA

[8] Inst Thorax Curie Montsouris, Paris, France

[9] Univ Versailles St Quentin En Yvelines, Paris Saclay Univ, Versailles, France

[10] Christie NHS Fdn Trust, Dept Med Oncol, Manchester, England

[11] Univ Manchester, Div Canc Sci, Manchester, England

[12] Henry Ford Canc Inst, Dept Internal Med, Detroit, MI USA

[13] Natl Taiwan Univ, Canc Ctr, Taipei, Taiwan

[14] Natl Taiwan Univ Hosp, Taipei, Taiwan

[15] Ehime Univ Hosp, Toon, Ehime, Japan

[16] Kurume Univ, Sch Med, Kurume, Japan

[17] Seoul Natl Univ, Bundang Hosp, Coll Med, Seongnam, South Korea

[18] Chungbuk Natl Univ Hosp, Med Dept, Cheongju, South Korea

[19] Mahidol Univ, Siriraj Hosp, Fac Med, Dept Med, Bangkok, Thailand

[20] Oncoclin & CO MedSir, Rio De Janeiro, Brazil

[21] Jilin Canc Hosp, Changchun, Peoples R China

[22] Ankara Bilkent City Hosp, Dept Med Oncol, Ankara, Turkiye

[23] Ankara Yildirim Beyazit Univ, Ankara, Turkiye

[24] Chung Shan Med Univ, Sch Med, Taichung, Taiwan

[25] Chung Shan Med Univ, Inst Med, Taichung, Taiwan

[26] Chung Shan Med Univ Hosp, Dept Internal Med, Div Pulm Med, Taichung, Taiwan

[27] Kaohsiung Chang Gung Mem Hosp, Div Pulm & Crit Care Med, Kaohsiung, Taichung, Taiwan

[28] HBNI, Tata Mem Ctr, Dept Med Oncol, Mumbai, India

[29] Natl Canc Ctr, Dept Thorac Oncol, Tokyo, Japan

[30] Moscow City Oncol Hosp 62, Healthcare Dept, Moscow, Russia

[31] Univ Complutense Madrid, Univ Hosp 12 Octubre, CNIO Lung Canc Unit H120, Madrid, Spain

[32] CIBERONC, Madrid, Spain

[33] Med Sur, Mexico City, Mexico

[34] Alexander Fleming Canc Inst, Thorac Oncol Unit, Buenos Aires, Argentina

[35] Alexander Fleming Canc Inst, Dept Med Oncol, Clin Res Unit, Buenos Aires, Argentina

[36] Hosp Univ A Coruna, Med Oncol, La Coruna, Spain

[37] Kindai Univ, Fac Med, Dept Med Oncol, Osaka, Japan

[38] City Hope Natl Med Ctr, Duarte, CA USA

[39] Aix Marseille Univ, Hop Timone, Multidisciplinary Oncol & Therapeut Innovat Dept, APHM,INSERM,NCRS,CRCM, Marseille, France

[40] Meir Med Ctr, Kefar Sava, Israel

[41] Univ Hosp Leuven, Resp Oncol Unit, Leuven, Belgium

[42] European Inst Oncol IRCCS, Div Thorac Oncol, Milan, Italy

[43] Univ Hosp Essen, West German Canc Ctr, Dept Med Oncol, Essen, Germany

[44] Uniao Brasileira Educ & Assistencia Hosp Sao Lucas, Porto Alegre, RS, Brazil

[45] McGill Univ, Dept Oncol, Montreal, PQ, Canada

[46] William Osler Hlth Syst, Brampton, ON, Canada

[47] Univ Calif Irvine, Chao Family Comprehens Canc Ctr, Sch Med, Orange, CA USA

[48] Janssen Res & Dev, Chao Family Comprehens Canc Ctr, Sch Med, Spring House, PA USA

[49] Janssen Res & Dev, Raritan, NJ USA

[50] Janssen Res & Dev, High Wycombe, England

来源：

ANNALS OF ONCOLOGY | 2024年 / 35卷 / 09期

关键词：

amivantamab; lazertinib; NSCLC; biomarkers; ctDNA; TP53; LIVER METASTASIS; MUTATIONS; CLEARANCE; PROGNOSIS; THERAPY; NSCLC;

D O I：

10.1016/j.annonc.2024.05.541

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

Background: Amivantamab-lazertinib significantly prolonged progression-free survival (PFS) versus osimertinib in patients with epidermal growth factor receptor (EGFR)-mutant advanced non-small-cell lung cancer [NSCLC; hazard ratio (HR) 0.70; P < 0.001], including those with a history of brain metastases (HR 0.69). Patients with TP53 co-mutations, detectable circulating tumor DNA (ctDNA), baseline liver metastases, and those without ctDNA clearance on treatment have poor prognoses. We evaluated outcomes in these high-risk subgroups. Patients and methods: This analysis included patients with treatment-naive, EGFR-mutant advanced NSCLC randomized to amivantamab-lazertinib (n = 429) or osimertinib (n = 429) in MARIPOSA. Pathogenic alterations were identified by next-generation sequencing (NGS) of baseline blood ctDNA with Guardant360 CDx. Ex19del and L858R ctDNA in blood was analyzed at baseline and cycle 3 day 1 (C3D1) with Biodesix droplet digital polymerase chain reaction (ddPCR). Results: Baseline ctDNA for NGS of pathogenic alterations was available for 636 patients (amivantamab-lazertinib, n = 320; osimertinib, n = 316). Amivantamab-lazertinib improved median PFS (mPFS) versus osimertinib for patients with TP53 co-mutations {18.2 versus 12.9 months; HR 0.65 [95% confidence interval (CI) 0.48-0.87]; P = 0.003} and for patients with wild-type TP53 [22.1 versus 19.9 months; HR 0.75 (95% CI 0.52-1.07)]. In patients with EGFR-mutant, ddPCR-detectable baseline ctDNA, amivantamab-lazertinib significantly prolonged mPFS versus osimertinib [20.3 versus 14.8 months; HR 0.68 (95% CI 0.53-0.86); P = 0.002]. Amivantamab-lazertinib significantly improved mPFS versus osimertinib in patients without ctDNA clearance at C3D1 [16.5 versus 9.1 months; HR 0.49 (95% CI 0.27-0.87); P = 0.015] and with clearance [24.0 versus 16.5 months; HR 0.64 (95% CI 0.48-0.87); P = 0.004]. Amivantamab-lazertinib significantly prolonged mPFS versus osimertinib among randomized patients with [18.2 versus 11.0 months; HR 0.58 (95% CI 0.37-0.91); P = 0.017] and without baseline liver metastases [24.0 versus 18.3 months; HR 0.74 (95% CI 0.60-0.91); P = 0.004]. Conclusions: Amivantamab-lazertinib effectively overcomes the effect of high-risk features and represents a promising new standard of care for patients with EGFR-mutant advanced NSCLC.

引用

页码：805 / 816

页数：12

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