Optimal Therapy for Secondary Acute Myeloid Leukemia after Prior Hypomethylating Therapy

Background: Patients (pts) with secondary acute myeloid leukemia (sAML) emerging from myelodysplastic syndrome (AML-MR) with extensive prior hypomethylating agent (HMA) exposure remain a high unmet need with significantly worse survival (4.2 months) and complete remission (CR) rate (32%) than sAML w...

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Published in:Blood 2024-11, Vol.144 (Supplement 1), p.4236-4236
Main Authors: Bawek, Sawyer, Green, Steven, Griffiths, Elizabeth A., Thompson, James E, Sung, Pamela J., Przespolewski, Amanda C., Wang, Eunice S.
Format: Article
Language:English
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Summary:Background: Patients (pts) with secondary acute myeloid leukemia (sAML) emerging from myelodysplastic syndrome (AML-MR) with extensive prior hypomethylating agent (HMA) exposure remain a high unmet need with significantly worse survival (4.2 months) and complete remission (CR) rate (32%) than sAML without prior HMA independent of age, cytogenetic risk, or treatment intensity. Because these pts are often specifically excluded from (and therefore vastly underrepresented in) AML clinical trials, the optimal therapy for these individuals is uncertain. For instance, although venetoclax (Ven) + HMA therapy is typically offered to these pts, the VIALE-A trial specifically excluded sAML pts with any prior HMA therapy. Here, we performed a single-center retrospective analysis of the outcomes of these pts following intensive chemotherapy (IC) vs low intensity (LI) regimens for sAML diagnosis, focusing on clinical outcomes, specifically response rates, overall survival (OS), and ability to proceed to allogeneic stem cell transplantation (alloSCT) in first or second CR. Patients and Methods: Medical records from pts treated at Roswell Park from June 2005 to January 2024 were retrospectively reviewed to identify adult pts with newly diagnosed sAML emerging from previously documented MDS who had received at least one cycle of prior single agent HMA (azacitidine (Aza), decitabine (Dec)). Induction regimens for sAML were divided into IC (7+3, CLAG+/-M, FLAG, CPX-351) vs LI (Ven-based, targeted agent, other) regimens. Results: We identified 105 pts meeting these criteria. Median age was 71.7 years (range 31-91), with younger pts (median 67.6 years) in the IC group and older pts (median age 73.7 years) in the LI group. Overall, 72 (68.6%) were men. Ninety pts were Caucasian, 6 African American, 1 Asian, 8 other/unknown ethnicity. Half of pts (52/105, 50%) received an intensive chemotherapy (IC) induction, and half (53/105) received a low intensity (LI) induction. Median months of prior HMA therapy was 11.1 (range 0.03-88.7) with fewer (5.2 months) in the IC group than LI (8.3 months). The majority (86/105, 82%) received prior Aza; the rest (19/105, 18%) received prior Dec. Most (65/105) were fit with ECOG PS of 0 (10%) or 1 (52%). Almost half (50/105 pts, 47.6%) had an adverse ELN risk stratification: 25/53 (47.2%) for LI and 25/52 (48.1%) for IC cohort. Among those receiving IC, the overall response rate (ORR=CR/CRi/CRh) was 60%, with 14 CR (27%) and 17 (33%) CRi/CRh. Pts
ISSN:0006-4971
1528-0020
DOI:10.1182/blood-2024-206258