Annals of oncology : official journal of the European Society for Medical Oncology | 2019
Renal toxicity from platinum/pemetrexed and pembrolizumab in the era of combination therapy.
Abstract
textabstractBackground: Recently, the phase 3 keynote-189 trial showed that in previously untreated \npatients with advanced non-squamous NSCLC without targetable mutations, the \nprogression-free and overall survival were significantly longer with addition of pembrolizumab to chemotherapy than with chemotherapy alone. Both chemotherapy and pembrolizumab can give renal toxicity, which can be a major challenge in the clinical setting. \nMethods: In a prospective multicenter observational real-life cohort study [Visser Eur \nRespir J 2018], we evaluated the incidence of acute/chronic kidney disease (AKD/ \nCKD), its related treatment discontinuation frequency and associated clinical variables \nwith AKD in patients with stage IIIB/IV NSCLC treated with platinum/pemetrexed. In \naddition, the Keynote 189 toxicity data was used for the combination treatment. We \nthereafter reviewed literature to generate an algorithm for diagnosis and treatment in \nincreased creatinine levels. \nResults: 149 patients received pemetrexed platinum, of whom 44 patients (30%) continued \nmaintenance. During induction therapy 48 patients (50%) treated with cisplatinum/pemetrexed developed AKD and 15 patients (29%) treated with carboplatin/pemetrexed. During \nmaintenance 13 patients (30%) developed AKD, leading to CKD and treatment discontinuation in eight patients (62%). In the Keynote 189 trial combining pembrolizumab with chemotherapy, nephritis has been reported in 1,7% of patients in any grade (1,5% grade 3-4). \nHowever, when looking at an increased blood creatinine in the group that was treated with \ncarboplatin, a total of 12,2% of patients showed any increase (0,7% grade 3-4). \nConclusions: Increased blood creatinine levels from pemetrexed and pembrolizumab \nis a common entity, probably more common in a real-life setting. This elevation is clinically challenging in a population that receives three agents that can cause a creatinine \nincrease. Currently, there are no markers to distinguish between renal failure due to \nchemotherapy of immunotherapy. We will present an algorithm based on current \nknowledge for clinicians as guidance for renal dysfunction in patients treated with chemotherapy and pd-(l)1 checkpoint inhibitors.