| Literature DB >> 29296935 |
Lynn Quek1,2,3, Paul Ferguson4,5, Marlen Metzner1,3, Ikhlaaq Ahmed5, Alison Kennedy1,3, Catherine Garnett1,3, Sally Jeffries6, Claudia Walter7, Kim Piechocki6, Adele Timbs8, Robert Danby2,3, Manoj Raghavan4, Andrew Peniket2,3, Mike Griffiths6, Andrew Bacon4, Janice Ward4, Keith Wheatley5, Paresh Vyas1,2,3, Charles Craddock4,5.
Abstract
Disease relapse is the major cause of treatment failure after allogeneic stem cell transplantation (allo-SCT) in acute myeloid leukemia (AML). To identify AML-associated genes prognostic of AML relapse post-allo-SCT, we resequenced 35 genes in 113 adults at diagnosis, 49 of whom relapsed. Two hundred sixty-two mutations were detected in 102/113 (90%) patients. An increased risk of relapse was observed in patients with mutations in WT1 (P = .018), DNMT3A (P = .045), FLT3 ITD (P = .071), and TP53 (P = .06), whereas mutations in IDH1 were associated with a reduced risk of disease relapse (P = .018). In 29 patients, we additionally compared mutational profiles in bone marrow at diagnosis and relapse to study changes in clonal structure at relapse. In 13/29 patients, mutational profiles altered at relapse. In 9 patients, mutations present at relapse were not detected at diagnosis. In 15 patients, additional available pre-allo-SCT samples demonstrated that mutations identified posttransplant but not at diagnosis were detectable immediately prior to transplant in 2 of 15 patients. Taken together, these observations, if confirmed in larger studies, have the potential to inform the design of novel strategies to reduce posttransplant relapse highlighting the potential importance of post-allo-SCT interventions with a broad antitumor specificity in contrast to targeted therapies based on mutational profile at diagnosis.Entities:
Year: 2016 PMID: 29296935 PMCID: PMC5737177 DOI: 10.1182/bloodadvances.2016000760
Source DB: PubMed Journal: Blood Adv ISSN: 2473-9529