A Phase I Study of the IDH2 Inhibitor Enasidenib As Maintenance Therapy for IDH2-Mutant Myeloid Neoplasms Following Hematopoietic Cell Transplantation

ABSTRACT

Characterization of molecular alterations in acute myeloid leukemia (AML) has led to development of targeted therapies, including FLT3 and IDH1/2 inhibitors. Maintenance therapy following hematopoietic cell transplantation (HCT) has shown substantial promise. Enasidenib (ENA), a selective IDH2 inhibitor, was associated with impressive rates of response in relapsed/refractory (R/R) AML and is now FDA-approved for this indication. We sought to assess the tolerability and define the maximum tolerated dose (MTD) of ENA as maintenance following HCT for IDH2-mutated myeloid malignancy. HCT-eligible patients (pts) ≥ 18 years with AML in remission, or myelodysplastic syndrome (MDS) with <5% marrow blasts, were enrolled. There were no restrictions on conditioning or donor type. A 2-step registration process was utilized;1 before HCT and 1 before ENA initiation. Before HCT, pts were required to have normal organ and recovered marrow function (neutrophils > 1000/µL and platelets > 50000/µL). Those with prior HCT, active disease, QTc ≥450ms, and active infections were excluded. ENA was initiated between day 30 and 90 after HCT, at which time the following were required chimerism ≥70% of donor origin among blood/marrow cells, no acute graft versus host disease (aGVHD) requiring ≥0.5mg/kg/day prednisone or equivalent, and no relapse. ENA was taken orally (po) daily (qd) in 28-day cycles. The period for dose-limiting toxicity (DLT) evaluation was the first cycle, escalation to successive levels was guided by DLT incidence, and 2 levels (50mg,100mg) were studied. Following establishment of MTD or recommended phase 2 dose (RP2D), 10 pts would be enrolled in an expansion cohort. Pts were monitored for relapse and toxicity and continued until disease progression, intolerable toxicity, or receipt of 12 cycles. Nineteen pts have been registered prior to HCT at 3 sites, Massachusetts General Hospital, Dana Farber Cancer Institute, and Johns Hopkins Hospital. Three pts could not initiate ENA following HCT;2 due to logistic challenges of the COVID pandemic and 1 due to relapse. The remaining 16 pts initiated ENA treatment. The median age was 61 years (range 31-76);12 (75%) were male, and 13 (81%) were Caucasian. Fourteen (88%) had AML, of which 6 were AML with MDS related changes and 2 had antecedent myeloproliferative neoplasm. Two pts (13%) had MDS. Among these 16 pts, 9 (56%) had IDH2 R140, and 5 (25%) had IDH2 R172 mutations. IDH2 subtype data was unavailable for 2 pts. Of 15 pts with available data from time of diagnosis, 11 (73%) had intermediate-risk and 4 (27%) had adverse-risk cytogenetics. Among these 15 pts, common concurrent mutations were DNMT3A (47%), SRSF2 (33%), and RUNX1 (33%). Eleven AML pts (85%) received intensive versus non-intensive therapies (15%) prior to HCT, and among all pts, 7 (44%) had received ENA prior to HCT. HCT data was available for all 16 pts;4 pts (25%) received myeloablative, and 12 (75%) received reduced-intensity conditioning. Nine pts (56%) had a matched unrelated, 6 (38%) had haploidentical, and 1 (6%) had a matched related donor HCT. Three pts were enrolled at the 50mg dose level, 6 pts at 100mg, and after no DLTs were detected, the remaining were enrolled in an expansion cohort at 100mg qd. Median follow-up (F/U) for surviving patients is currently 11.7 months (range 1.5-18.9). 2 pts (13%) have relapsed during F/U, at 96 and 364 days post HCT. Additional ≥grade (G) 3 toxicities detected during treatment, possibly or probably related to ENA, included neutropenia, anemia, and bilirubinemia. Six pts (38%) required dose interruptions lasting a median 19 days (range 7-25), 4 required a dose reduction to 50mg, and 1 stopped treatment due to G3 bilirubinemia. In total, 3 pts (18%) discontinued study treatment, 1 for aforementioned G3 bilirubinemia, 1 to pursue a GVHD trial, and 1 for relapse. Six pts have completed the 12-month f/u without relapse, and 7 remain on study. 15 of 16 pts remain alive. Thus far, 3 pts have experienced ≥ G2 aGVHD, and 4 had moderate chronic GVHD. Serial me surement of 2HG is being conducted on samples, and these will be reported. Enasidenib is well-tolerated as post-HCT maintenance therapy for myeloid malignancy at the RP2D of 100mg qd. No DLTs have been detected, and a low rate of post-HCT relapse has been identified to date, although longer f/u is needed. Larger, randomized studies of ENA in the post-SCT setting would determine the true efficacy of this agent as maintenance therapy. Disclosures Fathi Blueprint Consultancy;Jazz Consultancy;Amgen Consultancy;Newlink Genetics Consultancy;Pfizer Consultancy;Abbvie Consultancy;Seattle Genetics Consultancy, Research Funding;Agios Consultancy, Research Funding;PTC Therapeutics Consultancy;Takeda Consultancy, Research Funding;Boston Biomedical Consultancy;Amphivena Consultancy;BMS/Celgene Consultancy, Research Funding;Kite Consultancy;Trovagene Consultancy;Forty Seven Consultancy;Novartis Consultancy;Daiichi Sankyo Consultancy;Astellas Consultancy;Trillium Consultancy;Kura Oncology Consultancy. Soiffer Gilead Consultancy;Novartis Consultancy;Juno Membership on an entity's Board of Directors or advisory committees;Celgene Membership on an entity's Board of Directors or advisory committees;VOR Biopharma Consultancy;alexion Consultancy;Rheos Therapeutics Consultancy;Cugene Consultancy;Precision Bioscience Consultancy;Be the Match/ National Marrow Donor Program Membership on an entity's Board of Directors or advisory committees;Kiadis Membership on an entity's Board of Directors or advisory committees;Mana Therapeutics Consultancy. Levis Menarini Honoraria;Amgen Honoraria;FujiFilm Honoraria, Research Funding;Astellas Honoraria, Research Funding;Daiichi-Sankyo Honoraria. Mims Novartis Speakers Bureau;Kura Oncology Membership on an entity's Board of Directors or advisory committees;Leukemia and Lymphoma Society Other Senior Medical Director for Beat AML Study;Agios Consultancy;Syndax Pharmaceuticals Membership on an entity's Board of Directors or advisory committees;Jazz Pharmaceuticals Other Data Safety Monitoring Board;Abbvie Membership on an entity's Board of Directors or advisory committees. Devine Magenta Therapeutics Consultancy. Defilipp Incyte Research Funding;Regimmune Research Funding;Syndax Pharmaceuticals Consultancy. Spitzer Jazz Pharmaceuticals, Inc. Membership on an entity's Board of Directors or advisory committees;Bluebird Bio Membership on an entity's Board of Directors or advisory committees. Frigault Celgene Consultancy;Arcellx Consultancy;Novartis Consultancy, Research Funding;Gilead/Kite Consultancy, Research Funding. Amrein Amgen Research Funding;AstraZeneca Consultancy, Research Funding;Takeda Research Funding. Hobbs Incyte Research Funding;Merck Research Funding;Bayer Research Funding;Constellation Honoraria, Research Funding;Jazz Honoraria;Celgene/BMS Honoraria;Novartis Honoraria. Brunner Janssen Research Funding;Acceleron Pharma Inc. Consultancy;GSK Research Funding;Xcenda Consultancy;Takeda Consultancy, Research Funding;Novartis Consultancy, Research Funding;Jazz Pharma Consultancy;Forty Seven, Inc Consultancy;Celgene/BMS Consultancy, Research Funding;Biogen Consultancy;Astra Zeneca Research Funding. Narayan Genentech Other Prior Spouse employment within 24 months and prior spouse equity divested within past 24 months;Takeda Other Prior Spouse employment within 24 months;Sanofi-Genzyme Other Current Spouse employment. Chen AbbVie Other Data and Safety Monitoring Board Member;Incyte Corporation Consultancy;Takeda Consultancy;Actinium Other Data and Safety Monitoring Board Member;Equillium Other Data and Safety Monitoring Board Member;Magenta Consultancy;Kiadis Consultancy. OffLabel Disclosure Enasidenib as post-transplant maintenance therapy