Complex I inhibitor of oxidative phosphorylation in advanced solid tumors and acute myeloid leukemia: phase I trials.
Timothy Anthony YapNaval G DaverMikhila MahendraJixiang ZhangCarlos Kamiya-MatsuokaFunda Meric-BernstamHagop M KantarjianFarhad RavandiMeghan E CollinsMaria Emilia Di FrancescoEcaterina E DumbravaSiqing FuSisi GaoJason P GaySonal GeraJing HanDavid S HongElias J JabbourZhenlin JuDaniel D KarpAlessia LodiJennifer R MolinaNatalia BaranAung NaingMaro OhanianShubham PantNaveen PemmarajuPrithviraj BoseSarina A Piha-PaulJordi RodonCarolina SalgueroKoiji SasakiAnand K SinghVivek SubbiahApostolia M TsimberidouQuanyun A XuMusa YlimazQi ZhangYuan LiChristopher A BristowMeenakshi B BhattacharjeeStefano TizianiTimothy P HeffernanChristopher P VellanoPhilip JonesCobi J HeijnenAnnemieke KavelaarsJoseph R MarszalekMarina Y KonoplevaPublished in: Nature medicine (2023)
Although targeting oxidative phosphorylation (OXPHOS) is a rational anticancer strategy, clinical benefit with OXPHOS inhibitors has yet to be achieved. Here we advanced IACS-010759, a highly potent and selective small-molecule complex I inhibitor, into two dose-escalation phase I trials in patients with relapsed/refractory acute myeloid leukemia (NCT02882321, n = 17) and advanced solid tumors (NCT03291938, n = 23). The primary endpoints were safety, tolerability, maximum tolerated dose and recommended phase 2 dose (RP2D) of IACS-010759. The PK, PD, and preliminary antitumor activities of IACS-010759 in patients were also evaluated as secondary endpoints in both clinical trials. IACS-010759 had a narrow therapeutic index with emergent dose-limiting toxicities, including elevated blood lactate and neurotoxicity, which obstructed efforts to maintain target exposure. Consequently no RP2D was established, only modest target inhibition and limited antitumor activity were observed at tolerated doses, and both trials were discontinued. Reverse translational studies in mice demonstrated that IACS-010759 induced behavioral and physiological changes indicative of peripheral neuropathy, which were minimized with the coadministration of a histone deacetylase 6 inhibitor. Additional studies are needed to elucidate the association between OXPHOS inhibition and neurotoxicity, and caution is warranted in the continued development of complex I inhibitors as antitumor agents.
Keyphrases
- acute myeloid leukemia
- small molecule
- histone deacetylase
- clinical trial
- end stage renal disease
- open label
- newly diagnosed
- chronic kidney disease
- diffuse large b cell lymphoma
- prognostic factors
- case control
- drug delivery
- metabolic syndrome
- patient reported outcomes
- high glucose
- high fat diet induced
- patient reported