| 伴NPM1突变急性髓系白血病二代测序突变基因谱与MICM分型特征关联性分析 |
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| 引用本文: | 王彪,凌云,戴莉,顾伟英,张修文,邢珊珊,李海乾.伴NPM1突变急性髓系白血病二代测序突变基因谱与MICM分型特征关联性分析[J].中国实验血液学杂志,2022(1):56-64. |
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| 作者姓名: | 王彪 凌云 戴莉 顾伟英 张修文 邢珊珊 李海乾 |
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| 作者单位: | 苏州大学附属第三医院(常州市第一人民医院)血液科;南京医科大学附属常州第二人民医院血液科;浙江医院血液科 |
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| 摘 要: | 目的:分析伴NPM1突变(NPM1mut)急性髓系白血病(AML)患者二代测序(NGS)法检测的突变基因谱与MICM特征间的关系,解释NPM1mutAML的临床生物学异质性.方法:收集苏州大学附属第三医院、南京医科大学附属常州第二人民医院和浙江医院收治的成人初诊AML患者,选取NGS资料完整的NPM1mut患者238例...
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| 关 键 词: | NPM1 FLT3-ITD 急性髓系白血病 免疫表型 二代测序 |
Association of Next Generation Sequencing Based Genotypic Profiling with MICM Characteristics in NPM1 Mutated Acute Myeloid Leukemia |
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| WANG Biao,LING Yun,DAI Li,GU Wei-Ying,ZHANG Xiu-Wen,XING Shan-Shan,LI Hai-Qian.Association of Next Generation Sequencing Based Genotypic Profiling with MICM Characteristics in NPM1 Mutated Acute Myeloid Leukemia[J].Journal of Experimental Hematology,2022(1):56-64. |
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| Authors: | WANG Biao LING Yun DAI Li GU Wei-Ying ZHANG Xiu-Wen XING Shan-Shan LI Hai-Qian |
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| Institution: | (Department of Hematology,The Third Affiliated Hospital of Soochow University(The First People's Hospital of Changzhou),Changzhou 213003,Jiangsu Province,China;Department of Hematology,Nanjing Medical University Affiliated Changzhou Second Hospital,Changzhou 213164,Jiangsu Province,China;Department of Hematology,Zhejiang Hospital,Hangzhou 310013,Zhejiang Province,China) |
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| Abstract: | Objective:To explain the clinicobiological heterogeneity of NPM1 mutated(NPM1mut)acute myeloid leukemia(AML)by analyzing the association between next-generation sequencing(NGS)profiles and MICM characteristics in patients with this AML subtype.Methods:Data of 238 NPM1mut patients with available NGS information on 112 genes related to blood disease was collected,andχ2 test and nonparametric test were used to analyze the distribution association between NGS-detecting mutations and conventional MICM parameters.Results:In entire NPM1mut cohort,totaling 240 NPM1 mutation events were identified,of whom 10(10/240,4.2%)were missense mutations,which did not involve any W288 or W290 locus and were found exclusively in NPM1mut/FLT3-ITD-group.All but one of these missense mutations(9/10,90%)were accompanied by AML subtype-defining recurrent cytogenetic or molecular abnormalities,of which 7 cases were in the low risk and 2 in the high risk.NPM1mut occurred solely as an insertion/deletion(indel)type in the NPM1mut/FLT3-ITD+ group.The incidence of favorable plus unfavorable karyotypes in NPM1mut/FLT3-ITD- group was higher than in NPM1mut/FLT3-ITD+ group(6.4%vs.0,P=0.031).The positive rates of CD34 and CD7 in NPM1mut/FLT3-ITD+ group were significantly higher than in NPM1mut/FLT3-ITD- group(CD34:47.9%vs.20.6%,P<0.001;CD7:61.5%vs.29.9%,P<0.001).Logistic analysis showed that FLT3-ITD independently predicted for CD34+ and CD7+odds ratio(OR)=5.29,95%CI:2.64-10.60,P<0.001;OR=3.47,95%CI:1.79-6.73,P<0.001;respectively].Ras-pathway mutations independently predicted for HLA-DR+(OR=4.05,95%CI:1.70-9.63,P=0.002),and KRAS mutation for MPO-(OR=0.18,95%CI:0.05-0.62,P=0.007).TET2/IDH1 mutations independently predicted for CD34-and CD7-(OR=0.26,95%CI:0.11-0.62,P=0.002;OR=0.30,95%CI:0.14-0.62,P=0.001;respectively),and MPO+(OR=3.52,95%CI:1.48-8.38,P=0.004).DNMT3 A-RS882 independently predicted for CD7+and HLA-DR+(OR=3.59,95%CI:1.80-7.16,P<0.001;OR=13.41,95%CI:4.56-39.45,P<0.001;respectively),and DNMT3 A mutation for MPO-(OR=0.35,95%CI:1.48-8.38,P=0.004).Conclusion:Co-existing FLT3-ITD in NPM1mut AML independently predicts for CD34+ and CD7+,co-existing Ras-pathway mutation for HLA-DR+ and MPO-,co-existing TET2/IDH1 mutation for CD34-,CD7-,and MPO+,and co-existing DNMT3 A mutation for HLA-DR+,CD7+,and MPO-,thereby providing a new mechanism explanation for the immunophenotypic heterogeneity of these AML patients. |
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| Keywords: | NPM1 FLT3-ITD acute myeloid leukemia immunophenotype next generation sequencing |
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