A thiol-bound drug reservoir enhances APR-246-induced mutant p53 tumor cell death.
Sophia CederSofi E ErikssonEmarndeena H ChetehSwati DawarMariana Corrales BenitezVladimir J N BykovKenji M FujiharaMélodie GrandinXiaodun LiSusanne RammCorina BehrenbruchKaylene J SimpsonFrédéric HollandeLars AbrahmsenNicholas James ClemonsKlas G WimanPublished in: EMBO molecular medicine (2020)
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.
Keyphrases
- cancer therapy
- cell death
- wild type
- clinical trial
- phase iii
- cell cycle arrest
- drug delivery
- open label
- genome wide
- emergency department
- phase ii
- oxidative stress
- reactive oxygen species
- copy number
- squamous cell
- papillary thyroid
- cell proliferation
- high glucose
- squamous cell carcinoma
- adverse drug
- young adults
- study protocol
- amino acid
- pi k akt
- electronic health record
- protein protein
- childhood cancer