TP53 and Decitabine in Acute Myeloid Leukemia and Myelodysplastic Syndromes

John S Welch; Allegra A Petti; Christopher A Miller; Catrina C Fronick; Michelle O'Laughlin; Robert S Fulton; Richard K Wilson; Jack D Baty; Eric J Duncavage; Bevan Tandon; Yi-Shan Lee; Lukas D Wartman; Geoffrey L Uy; Armin Ghobadi; Michael H Tomasson; Iskra Pusic; Rizwan Romee; Todd A Fehniger; Keith E Stockerl-Goldstein; Ravi Vij; Stephen T Oh; Camille N Abboud; Amanda F Cashen; Mark A Schroeder; Meagan A Jacoby; Sharon E Heath; Kierstin Luber; Megan R Janke; Andrew Hantel; Niloufer Khan; Madina J Sukhanova; Randall W Knoebel; Wendy Stock; Timothy A Graubert; Matthew J Walter; Peter Westervelt; Daniel C Link; John F DiPersio; Timothy J Ley

doi:10.1056/NEJMoa1605949

TP53 and Decitabine in Acute Myeloid Leukemia and Myelodysplastic Syndromes

N Engl J Med. 2016 Nov 24;375(21):2023-2036. doi: 10.1056/NEJMoa1605949.

Authors

John S Welch^#¹, Allegra A Petti^#¹, Christopher A Miller¹, Catrina C Fronick¹, Michelle O'Laughlin¹, Robert S Fulton¹, Richard K Wilson¹, Jack D Baty¹, Eric J Duncavage¹, Bevan Tandon¹, Yi-Shan Lee¹, Lukas D Wartman¹, Geoffrey L Uy¹, Armin Ghobadi¹, Michael H Tomasson¹, Iskra Pusic¹, Rizwan Romee¹, Todd A Fehniger¹, Keith E Stockerl-Goldstein¹, Ravi Vij¹, Stephen T Oh¹, Camille N Abboud¹, Amanda F Cashen¹, Mark A Schroeder¹, Meagan A Jacoby¹, Sharon E Heath¹, Kierstin Luber¹, Megan R Janke¹, Andrew Hantel¹, Niloufer Khan¹, Madina J Sukhanova¹, Randall W Knoebel¹, Wendy Stock¹, Timothy A Graubert¹, Matthew J Walter¹, Peter Westervelt¹, Daniel C Link¹, John F DiPersio¹, Timothy J Ley¹

Affiliation

¹ the Department of Internal Medicine, Division of Oncology (J.S.W., L.D.W., G.L.U., A.G., M.H.T., I.P., R.R., T.A.F., K.E.S.-G., R.V., S.T.O., C.N.A., A.F.C., M.A.S., M.A.J., S.E.H., K.L., M.R.J., M.J.W., P.W., D.C.L., J.F.D., T.J.L.), and the Division of Biostatistics (J.D.B.), and the Department of Pathology and Immunology (E.J.D., B.T., Y.-S.L.), Washington University School of Medicine, and McDonnell Genome Institute, Washington University in St. Louis (A.A.P., C.A.M., C.C.F., M.O., R.S.F., R.K.W., L.D.W., T.J.L.) - both in St. Louis; the Departments of Internal Medicine (A.H., N.K., M.J.S., W.S.) and Pharmacy (R.W.K.), University of Chicago, Chicago; and the Department of Internal Medicine (T.A.G.), Massachusetts General Hospital, Boston.

^# Contributed equally.

Abstract

Background: The molecular determinants of clinical responses to decitabine therapy in patients with acute myeloid leukemia (AML) or myelodysplastic syndromes (MDS) are unclear.

Methods: We enrolled 84 adult patients with AML or MDS in a single-institution trial of decitabine to identify somatic mutations and their relationships to clinical responses. Decitabine was administered at a dose of 20 mg per square meter of body-surface area per day for 10 consecutive days in monthly cycles. We performed enhanced exome or gene-panel sequencing in 67 of these patients and serial sequencing at multiple time points to evaluate patterns of mutation clearance in 54 patients. An extension cohort included 32 additional patients who received decitabine in different protocols.

Results: Of the 116 patients, 53 (46%) had bone marrow blast clearance (<5% blasts). Response rates were higher among patients with an unfavorable-risk cytogenetic profile than among patients with an intermediate-risk or favorable-risk cytogenetic profile (29 of 43 patients [67%] vs. 24 of 71 patients [34%], P<0.001) and among patients with TP53 mutations than among patients with wild-type TP53 (21 of 21 [100%] vs. 32 of 78 [41%], P<0.001). Previous studies have consistently shown that patients with an unfavorable-risk cytogenetic profile and TP53 mutations who receive conventional chemotherapy have poor outcomes. However, in this study of 10-day courses of decitabine, neither of these risk factors was associated with a lower rate of overall survival than the rate of survival among study patients with intermediate-risk cytogenetic profiles.

Conclusions: Patients with AML and MDS who had cytogenetic abnormalities associated with unfavorable risk, TP53 mutations, or both had favorable clinical responses and robust (but incomplete) mutation clearance after receiving serial 10-day courses of decitabine. Although these responses were not durable, they resulted in rates of overall survival that were similar to those among patients with AML who had an intermediate-risk cytogenetic profile and who also received serial 10-day courses of decitabine. (Funded by the National Cancer Institute and others; ClinicalTrials.gov number, NCT01687400 .).

Publication types

Clinical Trial

MeSH terms

5-Methylcytosine / analysis
Adult
Aged
Aged, 80 and over
Antimetabolites, Antineoplastic / administration & dosage*
Antimetabolites, Antineoplastic / adverse effects
Azacitidine / administration & dosage
Azacitidine / adverse effects
Azacitidine / analogs & derivatives*
Biomarkers, Tumor / analysis
Bone Marrow / chemistry
Bone Marrow / pathology*
Decitabine
Exome
Female
Humans
Leukemia, Myeloid, Acute / drug therapy*
Leukemia, Myeloid, Acute / genetics
Leukemia, Myeloid, Acute / mortality
Male
Middle Aged
Mutation*
Myelodysplastic Syndromes / drug therapy*
Myelodysplastic Syndromes / genetics
Myelodysplastic Syndromes / mortality
Prospective Studies
Risk Factors
Survival Rate
Tumor Suppressor Protein p53 / genetics*

Substances

Antimetabolites, Antineoplastic
Biomarkers, Tumor
TP53 protein, human
Tumor Suppressor Protein p53
5-Methylcytosine
Decitabine
Azacitidine

Associated data

ClinicalTrials.gov/NCT01687400

Abstract

Publication types

MeSH terms

Substances

Associated data

Grants and funding