Pembrolizumab in combination with gemcitabine for patients with HER2‑negative advanced breast cancer: GEICAM/2015–04 (PANGEA‑Breast) study

Background: We evaluated a new chemoimmunotherapy combination based on the anti-PD1 monoclonal antibody pembrolizumab and the pyrimidine antimetabolite gemcitabine in HER2- advanced breast cancer (ABC) patients previously treated in the advanced setting, in order to explore a potential synergism tha...

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Autores: Cruz-Merino, L. (Luis) de la|||/items/a02a8c32-08e2-4305-ad2d-c3ea0a24aea1, Gion, M. (M.)|||/items/31cb0702-1ccd-49c3-a509-a2b165de9abd, Cruz, J. (J.)|||/items/f5089a5a-b361-4b5a-8be9-27dfe5bca517, Alonso‑Romero, J.L. (J. L.)|||/items/2eca489b-07c9-41af-acc8-f94efd7c3a4d, Quiroga, V. (V.)|||/items/7b3b23d4-1ad6-43c7-b723-c6094ff16e5d, Moreno, F. (Fernando)|||/items/158b8d5c-7596-427a-8a24-078f07412bac, Andrés, R. (R.)|||/items/04bed57c-d702-4f58-bffd-04c0fb13629e, Santisteban-Eslava, M. (Marta)|||/items/563d2cef-8a22-4110-97f4-8e16eac15419, Ramos, M. (Marina)|||/items/51caaadd-2834-4bd4-861d-8669782d4e40, Holgado, E. (E.)|||/items/bd39955d-b7fd-4ac5-a26a-8a885f68d35d, Cortes, J. (Javier)|||/items/1337e19a-ac62-43e4-a2e7-8ba44b48cd40, López‑Miranda, E. (E.)|||/items/ae4c5cdc-454b-48ba-a1f7-875fdf9ec1f8, Cortés, A. (A.)|||/items/09693989-3de8-4edc-a449-4d382728c14c, Henao, F. (F.)|||/items/e82d2583-87c8-47be-afa8-3134cde28325, Palazón‑Carrión, N. (N.)|||/items/69a57460-602b-478c-afd5-9b3923d84ff3, Rodríguez, L.M. (L. M.)|||/items/8e3cb71e-7a79-43f2-90c4-e24dc2a219b8, Ceballos, I.(I.)|||/items/c1b80c2a-5a53-4a33-b0c5-e46aed55c715, Soto, A. (A.)|||/items/760cab98-e2b3-41dd-aaba-5343151a65f9, Puertes, A. (A.)|||/items/1761a214-195f-4bd7-a750-bd5149a495c0, Casas, M. (M.)|||/items/68065b8a-89ac-42f8-8ff2-6bc2f56989e6, Benito, S. (S.)|||/items/e7749e66-a31d-4298-bdec-f920fbf2d3b9, Chiesa, M. (M.)|||/items/dda47907-7607-4f1f-a819-f47737ab4d38, Bezares, S. (S.)|||/items/a2afe26b-3b53-456d-9fe6-ab435ab97ddf, Caballero, R. (R.)|||/items/1d23a2b8-cfd5-430c-8c3c-fbdcb6e360a3, Jiménez‑Cortegana, C. (C.)|||/items/ad8d8616-18ca-4931-9099-a5df5a94bfb3, Sánchez-Margalet, V. (V.)|||/items/6b483dd3-6474-4e2e-924e-d9e34498c4d1, Rojo-Todo, F. (Federico)|||/items/705623da-f57f-4f92-a471-a3b53c6171c5
Tipo de recurso: artículo
Fecha de publicación:2022
País:España
Institución:Universidad de Navarra
Repositorio:Dadun. Depósito Académico Digital de la Universidad de Navarra
Idioma:inglés
OAI Identifier:oai:dadun.unav.edu:10171/68682
Acceso en línea:https://hdl.handle.net/10171/68682
Access Level:acceso abierto
Palabra clave:Advanced breast cancer
Chemotherapy
HER2-negative
MDSCs
PD-L1
Pembrolizumab
TILs
Descripción
Sumario:Background: We evaluated a new chemoimmunotherapy combination based on the anti-PD1 monoclonal antibody pembrolizumab and the pyrimidine antimetabolite gemcitabine in HER2- advanced breast cancer (ABC) patients previously treated in the advanced setting, in order to explore a potential synergism that could eventually obtain long term benefit in these patients. Methods: HER2-negative ABC patients received 21-day cycles of pembrolizumab 200 mg (day 1) and gemcitabine (days 1 and 8). A run-in-phase (6 + 6 design) was planned with two dose levels (DL) of gemcitabine (1,250 mg/m2 [DL0]; 1,000 mg/m2 [DL1]) to determine the recommended phase II dose (RP2D). The primary objective was objective response rate (ORR). Tumor infiltrating lymphocytes (TILs) density and PD-L1 expression in tumors and myeloid-derived suppressor cells (MDSCs) levels in peripheral blood were analyzed. Results: Fourteen patients were treated with DL0, resulting in RP2D. Thirty-six patients were evaluated during the first stage of Simon's design. Recruitment was stopped as statistical assumptions were not met. The median age was 52; 21 (58%) patients had triple-negative disease, 28 (78%) visceral involvement, and 27 (75%) ≥ 2 metastatic locations. Progression disease was observed in 29 patients. ORR was 15% (95% CI, 5-32). Eight patients were treated ≥ 6 months before progression. Fourteen patients reported grade ≥ 3 treatment-related adverse events. Due to the small sample size, we did not find any clear association between immune tumor biomarkers and treatment efficacy that could identify a subgroup with higher probability of response or better survival. However, patients that experienced a clinical benefit showed decreased MDSCs levels in peripheral blood along the treatment. Conclusion: Pembrolizumab 200 mg and gemcitabine 1,250 mg/m2 were considered as RP2D. The objective of ORR was not met; however, 22% patients were on treatment for ≥ 6 months. ABC patients that could benefit of chemoimmunotherapy strategies must be carefully selected by robust and validated biomarkers. In our heavily pretreated population, TILs, PD-L1 expression and MDSCs levels could not identify a subgroup of patients for whom the combination of gemcitabine and pembrolizumab would induce long term benefit. Trial registration: ClinicalTrials.gov and EudraCT (NCT03025880 and 2016-001,779-54, respectively). Registration dates: 20/01/2017 and 18/11/2016, respectively.