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Integration of cytogenetic and molecular alterations in risk stratification of 318 patients with de novo non-M3 acute myeloid leukemia
by
Lee, M-C
, Chen, C-Y
, Chen, Y-C
, Chiang, Y-C
, Ko, B-S
, Liu, C-Y
, Liu, C-W
, Lin, C-C
, Tseng, M-H
, Hsu, S-C
, Hou, H-A
, Lai, Y-J
, Lee, F-Y
, Huang, S-Y
, Chou, W-C
, Huang, C-F
, Tien, H-F
, Kuo, Y-Y
, Lin, L-I
, Yao, M
, Tsay, W
, Tang, J-L
, Liu, M-C
, Wu, S-J
in
631/208/1405
/ 631/208/737
/ 692/699/67/1990/283/1897
/ 692/700/1750
/ Adolescent
/ Adult
/ Aged
/ Aged, 80 and over
/ Cancer Research
/ Chemotherapy
/ Chromosome Aberrations
/ Critical Care Medicine
/ Cytogenetics
/ Drug dosages
/ Female
/ Gene mutations
/ Genes
/ Genetic research
/ Hematology
/ Hospitals
/ Humans
/ Identification and classification
/ Intensive
/ Internal Medicine
/ Laboratories
/ Leukemia
/ Leukemia, Myeloid, Acute - genetics
/ Male
/ Medical prognosis
/ Medicine
/ Medicine & Public Health
/ Middle Aged
/ Mutation
/ Oncology
/ original-article
/ Risk Factors
/ Young Adult
2014
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Integration of cytogenetic and molecular alterations in risk stratification of 318 patients with de novo non-M3 acute myeloid leukemia
by
Lee, M-C
, Chen, C-Y
, Chen, Y-C
, Chiang, Y-C
, Ko, B-S
, Liu, C-Y
, Liu, C-W
, Lin, C-C
, Tseng, M-H
, Hsu, S-C
, Hou, H-A
, Lai, Y-J
, Lee, F-Y
, Huang, S-Y
, Chou, W-C
, Huang, C-F
, Tien, H-F
, Kuo, Y-Y
, Lin, L-I
, Yao, M
, Tsay, W
, Tang, J-L
, Liu, M-C
, Wu, S-J
in
631/208/1405
/ 631/208/737
/ 692/699/67/1990/283/1897
/ 692/700/1750
/ Adolescent
/ Adult
/ Aged
/ Aged, 80 and over
/ Cancer Research
/ Chemotherapy
/ Chromosome Aberrations
/ Critical Care Medicine
/ Cytogenetics
/ Drug dosages
/ Female
/ Gene mutations
/ Genes
/ Genetic research
/ Hematology
/ Hospitals
/ Humans
/ Identification and classification
/ Intensive
/ Internal Medicine
/ Laboratories
/ Leukemia
/ Leukemia, Myeloid, Acute - genetics
/ Male
/ Medical prognosis
/ Medicine
/ Medicine & Public Health
/ Middle Aged
/ Mutation
/ Oncology
/ original-article
/ Risk Factors
/ Young Adult
2014
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Integration of cytogenetic and molecular alterations in risk stratification of 318 patients with de novo non-M3 acute myeloid leukemia
by
Lee, M-C
, Chen, C-Y
, Chen, Y-C
, Chiang, Y-C
, Ko, B-S
, Liu, C-Y
, Liu, C-W
, Lin, C-C
, Tseng, M-H
, Hsu, S-C
, Hou, H-A
, Lai, Y-J
, Lee, F-Y
, Huang, S-Y
, Chou, W-C
, Huang, C-F
, Tien, H-F
, Kuo, Y-Y
, Lin, L-I
, Yao, M
, Tsay, W
, Tang, J-L
, Liu, M-C
, Wu, S-J
in
631/208/1405
/ 631/208/737
/ 692/699/67/1990/283/1897
/ 692/700/1750
/ Adolescent
/ Adult
/ Aged
/ Aged, 80 and over
/ Cancer Research
/ Chemotherapy
/ Chromosome Aberrations
/ Critical Care Medicine
/ Cytogenetics
/ Drug dosages
/ Female
/ Gene mutations
/ Genes
/ Genetic research
/ Hematology
/ Hospitals
/ Humans
/ Identification and classification
/ Intensive
/ Internal Medicine
/ Laboratories
/ Leukemia
/ Leukemia, Myeloid, Acute - genetics
/ Male
/ Medical prognosis
/ Medicine
/ Medicine & Public Health
/ Middle Aged
/ Mutation
/ Oncology
/ original-article
/ Risk Factors
/ Young Adult
2014
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Integration of cytogenetic and molecular alterations in risk stratification of 318 patients with de novo non-M3 acute myeloid leukemia
Journal Article
Integration of cytogenetic and molecular alterations in risk stratification of 318 patients with de novo non-M3 acute myeloid leukemia
2014
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Overview
Conventionally, acute myeloid leukemia (AML) patients are categorized into good-, intermediate- and poor-risk groups according to cytogenetic changes. However, patients with intermediate-risk cytogenetics represent a largely heterogeneous population regarding treatment response and clinical outcome. In this study, we integrated cytogenetics and molecular mutations in the analysis of 318 patients with
de novo
non-M3 AML who received standard chemotherapy. According to the mutation status of eight genes, including
NPM1
,
CEBPA
,
IDH2
,
RUNX1
,
WT1
,
ASXL1
,
DNMT3A
and
FLT3
, that had prognostic significance, 229 patients with intermediate-risk cytogenetics could be refinedly stratified into three groups with distinct prognosis (
P
<0.001); patients with good-risk genotypes had a favorable outcome (overall survival, OS, not reached) similar to those with good-risk cytogenetics, whereas those with poor-risk genotypes had an unfavorable prognosis (OS, 10 months) similar to those with poor-risk cytogenetics (OS, 13.5 months), and the remaining patients with other genotypes had an intermediate outcome (OS, 25 months). Integration of cytogenetic and molecular profiling could thus reduce the number of intermediate-risk AML patients from around three-fourth to one-fourth. In conclusion, integration of cytogenetic and molecular changes improves the prognostic stratification of AML patients, especially those with intermediate-risk cytogenetics, and may lead to better decision on therapeutic strategy.
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