Table 4.

Deciding between chemotherapy and epigenetic therapy in patients with AML

Factors in favor of ICTFactors in favor of epigenetic therapy
Age <70 y Age ≥80 y 
ECOG PS < 2 ECOG PS ≥ 2 
Low CCI, HCT-CI (<3) High CCI, HCT-CI (≥3) 
Higher WBC* Lower WBC* 
De novo AML Secondary AML (post-MDS, post-MPN) 
AML not classified as WHO MRC-AML AML classified as WHO MRC-AML 
Favorable genetics: favorable ELN category (Table 1) Unfavorable genetics: monosomy 5 or 7, del(5q); complex, monosomal karyotype; TP53 gene mutation 
FLT3-ITD No FLT3-ITD 
No epigenetic gene mutation? Epigenetic gene mutations (TET2, DNMT3A)? 
Factors in favor of ICTFactors in favor of epigenetic therapy
Age <70 y Age ≥80 y 
ECOG PS < 2 ECOG PS ≥ 2 
Low CCI, HCT-CI (<3) High CCI, HCT-CI (≥3) 
Higher WBC* Lower WBC* 
De novo AML Secondary AML (post-MDS, post-MPN) 
AML not classified as WHO MRC-AML AML classified as WHO MRC-AML 
Favorable genetics: favorable ELN category (Table 1) Unfavorable genetics: monosomy 5 or 7, del(5q); complex, monosomal karyotype; TP53 gene mutation 
FLT3-ITD No FLT3-ITD 
No epigenetic gene mutation? Epigenetic gene mutations (TET2, DNMT3A)? 

CCI, Charlson Comorbidity Index; ELN, European LeukemiaNet; HCT-CI, Hematopoietic Cell Transplantation Comorbidity Index; ITD, internal tandem duplication; MPN, myeloproliferative neoplasm; MRC, myelodysplastic-related change.

*

Higher WBC is associated with a worse prognosis after ICT; nevertheless, the prognosis of patients with WBC > 15 000 G9/L might be even worse after HMA therapy, at least when treated with AZA55  and maybe less when treated with DAC.41 

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