| Literature DB >> 30617039 |
Claudio Vernieri1, Diego Signorelli2, Giulia Galli2, Monica Ganzinelli2, Massimo Moro3, Alessandra Fabbri4, Elena Tamborini4, Mirko Marabese5, Elisa Caiola5, Massimo Broggini5, Lital Hollander6, Rosaria Gallucci2, Giulia Vandoni7, Cecilia Gavazzi7, Tiziana Triulzi8, Mario Paolo Colombo9, Angela Maria Rizzo10, Paola Antonia Corsetto10, Giancarlo Pruneri11, Filippo de Braud12, Gabriella Sozzi3, Valter Torri6, Marina Chiara Garassino13.
Abstract
Advanced lung adenocarcinoma with inactive liver kinase B1 (LKB1) tumor suppressor protein is associated with poor response to immune checkpoint inhibitors and molecularly targeted agents, and with dismal patient prognosis. LKB1 is a central orchestrator of cancer cell metabolism, and halts tumor growth/proliferation during metabolic stress. Recent preclinical evidence suggests that LKB1-inactive lung adenocarcinoma is highly sensitive to metformin, a safe and low-cost antidiabetic compound that inhibits mitochondrial oxidative phosphorylation. The effects of metformin can be enhanced by nutrient deprivation (ie, glucose, amino acids), which reduces intracellular levels of ATP and anabolic precursors and can be achieved by the fasting mimicking diet (FMD). Noticeably, metformin also prevents resistance to cisplatin in preclinical in vitro and in vivo models of LKB1-inactive lung adenocarcinoma. Based on such preclinical evidence, the phase II FAME trial was designed to test the hypothesis that the addition of metformin, with or without cyclic FMD, to standard platinum-based chemotherapy improves the progression-free survival of patients with advanced, LKB-1 inactive lung adenocarcinoma. Enrolled patients will be randomized in a 1:1 ratio to receive cisplatin/carboplatin and pemetrexed with the addition of metformin alone (Arm A) or metformin plus FMD (Arm B). The FAME study will use a "pick-the-winner" design with the aim of establishing which of the 2 experimental treatments is superior in terms of antitumor efficacy and safety. The primary assumption of the study is that the combination of the 2 experimental treatments shall improve median progression-free survival from 7.6 months (historical data with chemotherapy alone) to 12 months. Secondary study endpoints are: objective response rate, overall survival, treatment tolerability, and compliance to the experimental treatment.Entities:
Keywords: Cancer metabolism; LKB1 inactivation; Overall survival; Progression-free survival; Safety
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Year: 2018 PMID: 30617039 DOI: 10.1016/j.cllc.2018.12.011
Source DB: PubMed Journal: Clin Lung Cancer ISSN: 1525-7304 Impact factor: 4.785