Genetic abnormalities in AML can be classified as disease-defining abnormalities that are mutually exclusive. So far, they encompass the 7 genetically defined WHO entities, 2 provisional WHO entities (NPM1 mutated, CEBPA double-mutated), and 2 suggested new WHO entities (MYST3-CREBBP, NUP98-NSD1). These are associated with a distinct cytomorphology and gene expression pattern. In addition, a specific pattern of HOXA and HOXB genes is recognized with MYST3-CREBBP being related to an elevated expression of HOXA, but not of HOXB genes. A further class comprises mutations that concomitantly occur and alter different cellular processes, such as signaling, chromatin modification, DNA methylation, RNA splicing, cohesion of sister chromatids, transcription, and tumor suppression.

Genetic abnormalities in AML can be classified as disease-defining abnormalities that are mutually exclusive. So far, they encompass the 7 genetically defined WHO entities, 2 provisional WHO entities (NPM1 mutated, CEBPA double-mutated), and 2 suggested new WHO entities (MYST3-CREBBP, NUP98-NSD1). These are associated with a distinct cytomorphology and gene expression pattern. In addition, a specific pattern of HOXA and HOXB genes is recognized with MYST3-CREBBP being related to an elevated expression of HOXA, but not of HOXB genes. A further class comprises mutations that concomitantly occur and alter different cellular processes, such as signaling, chromatin modification, DNA methylation, RNA splicing, cohesion of sister chromatids, transcription, and tumor suppression.

Close Modal
This Feature Is Available To Subscribers Only

or Create an Account

Close Modal
Close Modal