Repurposing Atovaquone as a Therapeutic against Acute Myeloid Leukemia (AML): Combination with Conventional Chemotherapy Is Feasible and Well Tolerated

Authors

Alexandra McLean Stevens
Eric S Schafer
Minhua Li
Maci Terrell
Raushan Rashid
Hana Paek
Melanie B Bernhardt
Allison Weisnicht
Wesley T Smith
Noah J Keogh
Michelle C Alozie
Hailey H Oviedo
Alan K Gonzalez
Tamilini Ilangovan
Alicia Mangubat-Medina
Haopei Wang
Eunji Jo
Cara A Rabik
Claire Bocchini
Susan Hilsenbeck
Zachary T Ball
Todd M Cooper
Michele S Redell

Publication Date

2-20-2023

Journal

Cancers

DOI

10.3390/cancers15041344

PMID

36831684

PMCID

PMC9954468

PubMedCentral® Posted Date

2-20-2023

PubMedCentral® Full Text Version

Post-print

Published Open-Access

yes

Keywords

pediatric, oxidative phosphorylation, metabolism, xenograft, patient-derived, oxygen consumption rate, pneumocystis jiroveci pneumonia

Abstract

Survival of pediatric AML remains poor despite maximized myelosuppressive therapy. The pneumocystis jiroveci pneumonia (PJP)-treating medication atovaquone (AQ) suppresses oxidative phosphorylation (OXPHOS) and reduces AML burden in patient-derived xenograft (PDX) mouse models, making it an ideal concomitant AML therapy. Poor palatability and limited product formulations have historically limited routine use of AQ in pediatric AML patients. Patients with de novo AML were enrolled at two hospitals. Daily AQ at established PJP dosing was combined with standard AML therapy, based on the Medical Research Council backbone. AQ compliance, adverse events (AEs), ease of administration score (scale: 1 (very difficult)-5 (very easy)) and blood/marrow pharmacokinetics (PK) were collected during Induction 1. Correlative studies assessed AQ-induced apoptosis and effects on OXPHOS. PDX models were treated with AQ. A total of 26 patients enrolled (ages 7.2 months-19.7 years, median 12 years); 24 were evaluable. A total of 14 (58%) and 19 (79%) evaluable patients achieved plasma concentrations above the known anti-leukemia concentration (>10 µM) by day 11 and at the end of Induction, respectively. Seven (29%) patients achieved adequate concentrations for PJP prophylaxis (>40 µM). Mean ease of administration score was 3.8. Correlative studies with AQ in patient samples demonstrated robust apoptosis, OXPHOS suppression, and prolonged survival in PDX models. Combining AQ with chemotherapy for AML appears feasible and safe in pediatric patients during Induction 1 and shows single-agent anti-leukemic effects in PDX models. AQ appears to be an ideal concomitant AML therapeutic but may require intra-patient dose adjustment to achieve concentrations sufficient for PJP prophylaxis.