Afatinib beyond progression in patients with non-small-cell lung cancer following chemotherapy, erlotinib/gefitinib and afatinib: Phase III randomized LUX-Lung 5 trial

Martin Schuler; J. C.H. Yang; K. Park; J. H. Kim; J. Bennouna; Y. M. Chen; C. Chouaid; F. De Marinis; J. F. Feng; Francesco Grossi; D. W. Kim; X. Liu; S. Lu; J. Strausz; Y. Vinnyk; R. Wiewrodt; Caicun Zhou; B. Wang; V. K. Chand; D. Planchard; Claudia Bagnes; Claudio Marcelo Martin; Gonzalo Recondo; Juan Jose Zarba; Cesar Blajman; Martín Richardet; Sue Anne McLachlan; Phillip Parente; Craig Underhill; Catherine Crombie; Paul Mainwaring; Richard Greil; Yves Humblet; Frédérique Bustin; Luciano Carestia; Danny Galdermans; Marc Lambrechts; Laetitia Delval; Piet Vercauter; Jin Wang; Cheng Huang; Xiaoyan Lin; Yilong Wu; Xiaoqing Liu; Ying Cheng; Shukui Qin; Jifeng Feng; Jianjin Huang; Yiping Zhang; Shun Lu; Manuela Zereu; Bernardo Garicochea; Cyntia Albuquerque Zadra; Henrik Riska; Tuomo Alanko; Jacques Cadranel; Christos Chouaid; Gérard Zalcman; Denis Moro Sibilot; Maurice Perol; Jaafar Bennouna; Pierre Fournel; Radj Gervais; Maciej Rotarski; Bruno Coudert; Michael Thomas; Thomas Wehler; Martin Faehling; Ulrich Keilholz; Eckart Laack; Joachim Von Pawel; Rudolf Huber; Nicolas Dickgreber; Rainer Wiewrodt; Zsuzsanna Mark; Sandor Tehenes; Janos Strausz; Veronika Sarosi; Kumar Prabhash; Minish Jain; Srinivasan Venkatesan; Lalit Sharma; Hemant Dadhich; Rajnish Vasant Nagarkar; Amir Onn; Maya Gottfried; Solomon Stemmer; Maria Rita Migliorino; Paolo Bidoli; Alessandra Bearz; Cesare Gridelli; Carlo Milandri; Marco Platania; Giovanni Luca Ceresoli; Giorgio Cruciani; Francisco Gutierrez Delgado; José Luis Gonzalez Perez; Gabriela Alvarado Luna; Othon Padilla Baca; Joachim Aerts; Jos Stigt; Anne Marie Dingemans; Gerarda Herder; Steven Gans; Jorge Fernando Salas Sánchez; Renzo Luzgardo Alvarez Barreda; Wilbert Rodriguez Pantigoso; Osbert Luis Mejia Palomino; Piotr Jaskiewicz; Andrzej Kazarnowicz; Piotr Serwatowski; Aleksandra Szczesna; Jacek Jassem; Vladimir Lubennikov; Nina Karaseva; Sergey Orlov; Yuri Ragulin; Pilar Garrido; José Luis González Larriba; Carlos Camps; Rosario García Campelo; Pilar Lianes; Manuel Cobo; Enriqueta Felip; Dong Wan Kim; Sang We Kim; Keunchil Park; Joo Hang Kim; Ji Youn Han; Young Chul Kim; Chih Hsin Yang; Te Chun Hsia; Yuh Min Chen; Ying Huang Tsai; Gee Chen Chang; Thomas Chang Yao Tsao; Wu Chou Su; Ming Shyan Huang; Ching Liang Ho; Ruey Kuen Hsieh; Yuriy Vinnyk; Oleksandr Popovych; Olga Ponomarova; Igor Bondarenko; Iryna Polishchuk; Riyaz Shah; Sanka Mitra; Sanjaykumar Popat; James Spicer; Elizabeth Toy; Toby Talbot; Emma Brown; Sunil Upadhyay; Yvonne Summers; Jayne Gurtler; Luis Meza; John Thropay

Journal ArticleOPEN ACCESS

Afatinib beyond progression in patients with non-small-cell lung cancer following chemotherapy, erlotinib/gefitinib and afatinib: Phase III randomized LUX-Lung 5 trial

Annals of Oncology (2016) 27(3) 417-423

DOI: 10.1093/annonc/mdv597

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Abstract

Background: Afatinib has demonstrated clinical benefit in patients with non-small-cell lung cancer progressing after treatment with erlotinib/gefitinib. This phase III trial prospectively assessed whether continued irreversible ErbB-family blockade with afatinib plus paclitaxel has superior outcomes versus switching to chemotherapy alone in patients acquiring resistance to erlotinib/gefitinib and afatinib monotherapy. Patients and methods: Patients with relapsed/refractory disease following ≥ 1 line of chemotherapy, and whose tumors had progressed following initial disease control (≥ 12 weeks) with erlotinib/gefitinib and thereafter afatinib (50 mg/day), were randomized 2:1 to receive afatinib plus paclitaxel (40 mg/day; 80 mg/m2/week) or investigator's choice of single-agent chemotherapy. The primary end point was progression-free survival (PFS). Other end points included objective response rate (ORR), overall survival (OS), safety and patient-reported outcomes. Results: Two hundred and two patients with progressive disease following clinical benefit from afatinib were randomized to afatinib plus paclitaxel (n ≥ 134) or single-agent chemotherapy (n ≥ 68). PFS (median 5.6 versus 2.8 months, hazard ratio 0.60, P ≥ 0.003) and ORR (32.1% versus 13.2%, P ≥ 0.005) significantly improved with afatinib plus paclitaxel. There was no difference in OS. Global health status/quality of life was maintained with afatinib plus paclitaxel over the entire treatment period. The median treatment duration was 133 and 51 days with afatinib plus paclitaxel and single-agent chemotherapy, respectively; 48.5% of patients receiving afatinib plus paclitaxel and 30.0% of patients receiving single-agent chemotherapy experienced drug-related grade 3/4 adverse events. Treatment-related adverse events were consistent with those previously reported with each agent. Conclusion: Afatinib plus paclitaxel improved PFS and ORR compared with single-agent chemotherapy in patients who acquired resistance to erlotinib/gefitinib and progressed on afatinib after initial benefit. LUX-Lung 5 is the first prospective trial to demonstrate the benefit of continued ErbB targeting post-progression, versus switching to single-agent chemotherapy. Trial registration number: NCT01085136 (clinicaltrials.gov).

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Schuler, M., Yang, J. C. H., Park, K., Kim, J. H., Bennouna, J., Chen, Y. M., … Thropay, J. (2016). Afatinib beyond progression in patients with non-small-cell lung cancer following chemotherapy, erlotinib/gefitinib and afatinib: Phase III randomized LUX-Lung 5 trial. Annals of Oncology, 27(3), 417–423. https://doi.org/10.1093/annonc/mdv597

Afatinib beyond progression in patients with non-small-cell lung cancer following chemotherapy, erlotinib/gefitinib and afatinib: Phase III randomized LUX-Lung 5 trial

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