| Literature DB >> 30900772 |
Garret M K Leung1, Chunxiao Zhang1, Nelson K L Ng1, Ning Yang1, Stephen S Y Lam1, Chun H Au2, Tsun L Chan2, Edmond S K Ma2, Sze P Tsui3, Ho W Ip3, Jason C C So3, Margaret H L Ng4, Kelvin C K Cheng4, Kit F Wong5, Lisa L P Siu5, Sze F Yip6, Shek Y Lin7, June S M Lau8, Tsan H Luk8, Harold K K Lee9, Chi K Lau10, Bonnie Kho11, Yok L Kwong1, Anskar Y H Leung1.
Abstract
The present study aimed to define a subtype of complex/monosomal karyotype (CK/MK) acute myeloid leukemia (AML) by its distinct clinical features, p53 signaling and responses to p53 targeting agents. Ninety-eight young adults (range: 21-60 years; median: 49 years) with CK/MK AML were studied. They received standard induction, consolidation and allogeneic hematopoietic stem cell transplantation from siblings or matched unrelated donors if available. Chromosomal abnormalities most commonly affected chromosome 5 (30%), 7 (22%) and 17 (21%). Next generation sequencing of a 54-myeloid gene panel were available in 76 patients. Tumor protein 53 (TP53) mutations were most common (49%) and associated with the presence of -5/5q- (P < .001) and -17/17p- (P < .001), but not -7/7q- (P = .370). This "typical" CK/MK AML subtype was associated with significantly lower presenting white cell counts, higher number of karyotypic abnormalities, and inferior leukemia-free and overall survivals, compared with CK/MK AML without the typical features. Blood or bone marrow samples from typical CK/MK AML patients showed defective p53 signaling upon induction by etoposide. In vitro drug sensitivity analysis showed that they were sensitive to APR-246 that targeted mutant p53, but resistant to MDM2 antagonist MI-77301. Novel therapeutic strategies targeting TP53 mutations in CK/MK AML should be developed and tested in clinical trials.Entities:
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Year: 2019 PMID: 30900772 DOI: 10.1002/ajh.25469
Source DB: PubMed Journal: Am J Hematol ISSN: 0361-8609 Impact factor: 10.047