Immune-related adverse events associated with immune-checkpoint inhibitors therapy in Mexican patients: Experience at a single center.

I.r.r Gonzalez Espinoza ,José Carlos Arroyo Kuribreña,Feliciano De Jesús Vizcarra Ramos,Mariana Chiquillo-Domínguez,Carmen Aguilar,Giovanni Tobón Helú,Mónica Sabaté Fernández ,Julio Cesar Garibay Diaz ,Sergio Sánchez Sosa ,Gabriela Juárez Salazar ,Juan Carlos García Reyna ,Enrique Miguel Cruz ,M.d.j González Blanco ,E Acosta Ponce De León ,Alfredo Domínguez Peregrina ,A Gozalishvili Boncheva ,R Ibarra Fernández ,Carlos Cordero Vargas ,José Manuel Aguilar Priego ,N Cortés Escobar

doi:10.1200/jco.2021.39.15_suppl.e14580

I.r.r Gonzalez Espinoza , José Carlos Arroyo Kuribreña + Show 18 more

https://doi.org/10.1200/jco.2021.39.15_suppl.e14580

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Abstract

e14580 Background: The use of immune-checkpoint inhibitors (ICIs) for solid malignancies is rapidly rising, and many new agents and treatment combinations are in development. However, ICIs have a unique side-effect profile of immune-related adverse events (irAEs) compared with chemotherapeutic agents or targeted therapies. The aim of this work was to describe the irAEs in diverse types of malignant tumors using real-world data. Methods: This is a retrospective and descriptive study of patients with diverse types of advanced malignancies treated with immunotherapy at Centro Oncológico Integral of the Hospital Ángeles in Puebla, México; during the period 2016-2020. Data about the primary neoplasm, ICIs, irAEs, organ system affected, grade and treatment was collected. Clinical and laboratory parameters were obtained by reviewing medical records. Results: A total of 117 patients were included, median age of 65 years, of which 63.2% were male and 36.8% were female. The most frequent neoplasms treated with ICIs were: lung (27.4%), kidney (16.2%), melanoma (12.8%), hepatocellular (9.4%), breast (8.5%), non-melanoma skin cancer (6.0%), mesothelioma (4.3%) and other tumors (15.3%). 39.3% of the patients had no metastases, 41.9% had metastases to at least 1 or 2 sites, and 18.8% to 3 or more sites. The types of ICIs were: nivolumab (35.0%), pembrolizumab (28.2%), atezolizumab (23.9%), ipilimumab + nivolumab (12.0%) and durvalumab (0.9%). The most frequent irAEs were: gastrointestinal (61.5%), neurologic (46.2%), pulmonary (38.5%), metabolic (32.5%) and hematologic (29.1%). 39.3% of the irAEs were reported as grade 1, 31.6% as grade 2, 14.5% as grade 3 and 2.6% as grade 4. Conclusions: Our work shows the incidence of irAEs in a poorly studied population and provides new data that complement that reported by other works, however, further prospective studies are necessary.[Table: see text]

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