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Original Articles

Interrogation of molecular profiles can help in differentiating between MDS and AML with MDS-related changes

ORCID Icon, , , , , , ORCID Icon & show all
Pages 1418-1427 | Received 17 Jul 2019, Accepted 10 Jan 2020, Published online: 04 Feb 2020
 

Abstract

A subset of AML with myelodysplastic syndrome (MDS)-related changes (MRCs) occurs without a documented MDS phase. We studied genomic profile of 646 patients: 310 with MDS, 167 with AML without (w/o) MRC, 99 with primary (p) AML-MRC, and 70 with secondary (s) AML-MRC and sought to find differences in mutational patterns. Among the 32-myeloid associated genes studied, SF3B1 (p ≤ .001) was significantly mutated in higher proportion of patients with MDS, compared to other categories. NPM1 (p < .001), FLT3 ITD (p = .08), and NRAS (p = .02) mutations showed trend toward significance for AML w/o MRC, compared to other categories. In pAML-MRC, TP53 (p < .001) was significantly mutated in higher proportion of patients. Similarly, SETBP1 (p = .001), RUNX1 (p = .004), and SRSF2 (p = .04) mutations were more commonly seen in sAML-MRC. While these signatures may not be diagnostically discriminatory, they may help in disease categorization when other data are absent or in challenging cases.

Author contributions

TB, AS, JS and MOH designed the research, analyzed the data, interpreted the results and wrote the manuscript; DS, RK, JL and EP contributed patients assisted in manuscript preparation; all authors approved the final draft of the manuscript.

Disclosure statement

No potential conflict of interest was reported by the authors.

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