| Literature DB >> 33314700 |
Sophia Ceder1, Sofi E Eriksson1, Emarndeena H Cheteh1, Swati Dawar2, Mariana Corrales Benitez2, Vladimir J N Bykov1, Kenji M Fujihara2,3, Mélodie Grandin4,5, Xiaodun Li6, Susanne Ramm7, Corina Behrenbruch3,4, Kaylene J Simpson7, Frédéric Hollande4,5, Lars Abrahmsen8, Nicholas J Clemons2,3, Klas G Wiman1.
Abstract
The tumor suppressor gene TP53 is the most frequently mutated gene in cancer. The compound APR-246 (PRIMA-1Met/Eprenetapopt) is converted to methylene quinuclidinone (MQ) that targets mutant p53 protein and perturbs cellular antioxidant balance. APR-246 is currently tested in a phase III clinical trial in myelodysplastic syndrome (MDS). By in vitro, ex vivo, and in vivo models, we show that combined treatment with APR-246 and inhibitors of efflux pump MRP1/ABCC1 results in synergistic tumor cell death, which is more pronounced in TP53 mutant cells. This is associated with altered cellular thiol status and increased intracellular glutathione-conjugated MQ (GS-MQ). Due to the reversibility of MQ conjugation, GS-MQ forms an intracellular drug reservoir that increases availability of MQ for targeting mutant p53. Our study shows that redox homeostasis is a critical determinant of the response to mutant p53-targeted cancer therapy.Entities:
Keywords: APR-246; Eprenetapopt; MRP1; glutathione; p53
Year: 2020 PMID: 33314700 DOI: 10.15252/emmm.201910852
Source DB: PubMed Journal: EMBO Mol Med ISSN: 1757-4676 Impact factor: 12.137