基于急性髓系白血病中拷贝数变异(CNV)和CNV调控的基因表达鉴定预后特征。
Identification of a prognostic signature based on copy number variations (CNVs) and CNV-modulated gene expression in acute myeloid leukemia.
作者信息
Niu Changchun, Wu Di, Li Alexander J, Qin Kevin H, Hu Daniel A, Wang Eric J, Tucker Andrew Blake, He Fang, Huang Linjuan, Wang Hao, Liu Qing, Ni Na, Shi Deyao, Zhao Xia, Wan Yafang, Li Tian, He Tongchuan, Liao Pu
机构信息
Department of Laboratory Diagnostic Medicine, The Affiliated Chongqing Hospital of The University of Chinese Academy of Sciences, Chongqing General Hospital Chongqing 400021, China.
Molecular Oncology Laboratory, Department of Orthopaedic Surgery and Rehabilitation Medicine, The University of Chicago Medical Center Chicago, IL 60637, USA.
出版信息
Am J Transl Res. 2021 Dec 15;13(12):13683-13696. eCollection 2021.
OBJECTIVES
Acute myeloid leukemia (AML) is caused by multiple genetic alterations in hematopoietic progenitors, and molecular genetic analyses have provided useful information for AML diagnosis and prognostication. This study aimed to integratively understand the prognostic value of specific copy number variation (CNV) patterns and CNV-modulated gene expression in AML.
METHODS
We conducted integrative CNV profiling and gene expression analysis using data from the Therapeutically Applicable Research To Generate Effective Treatments (TARGET) and The Cancer Genome Atlas (TCGA) AML cohorts. CNV-related genes associated with survival were identified using the TARGET AML cohort and validated using the TCGA AML cohort. Genes whose CNV-modulated expression was associated with survival were also identified using the TARGET AML cohort and validated using the TCGA AML cohort, and patient bone marrow samples were then used to further validate the effects of CNV-modulated gene expression on survival. CNV and mRNA survival analyses were conducted using proportional hazards regression models (Cox regression) and the "survminer" and "survival" packages of the R Project for Statistical Computing. Genes belonging to the Kyoto Encyclopedia of Genes and Genomes (KEGG) cancer panel were extracted from KEGG cancer-related pathways.
RESULTS
One hundred two CNV-related genes (located at 7q31-34, 16q24) associated with patient survival were identified using the TARGET cohort and validated with the TCGA AML cohort. Among these 102 validated genes, three miRNA genes ( and ) were included in the KEGG cancer panel. Five genes ( and ) whose expression was modulated by CNVs and significantly associated with clinical outcomes were identified, and the deletion of and was found to potentially exert protective effects against AML. The results of these five genes were also validated using patient marrow samples. Additionally, the distribution of CNVs affecting these five CNV-modulated genes was independent of the risk group (favorable-, intermediate-, and adverse-risk groups).
CONCLUSIONS
Overall, this study identified 102 CNV-related genes associated with patient survival and identified five genes whose expression was modulated by CNVs and associated with patient survival. Our findings are crucial for the development of new modes of prognosis evaluation and targeted therapy for AML.
目的
急性髓系白血病(AML)由造血祖细胞中的多种基因改变引起,分子遗传学分析为AML的诊断和预后提供了有用信息。本研究旨在综合了解特定拷贝数变异(CNV)模式和CNV调节的基因表达在AML中的预后价值。
方法
我们使用来自治疗性应用研究以产生有效治疗(TARGET)和癌症基因组图谱(TCGA)AML队列的数据进行综合CNV分析和基因表达分析。使用TARGET AML队列鉴定与生存相关的CNV相关基因,并使用TCGA AML队列进行验证。还使用TARGET AML队列鉴定其CNV调节表达与生存相关的基因,并使用TCGA AML队列进行验证,然后使用患者骨髓样本进一步验证CNV调节的基因表达对生存的影响。使用比例风险回归模型(Cox回归)以及R统计计算项目的“survminer”和“survival”软件包进行CNV和mRNA生存分析。从京都基因与基因组百科全书(KEGG)癌症面板中提取属于KEGG癌症相关途径的基因。
结果
使用TARGET队列鉴定了102个与患者生存相关的CNV相关基因(位于7q31 - 34、16q24),并通过TCGA AML队列进行了验证。在这102个经过验证的基因中,三个miRNA基因(和)包含在KEGG癌症面板中。鉴定出五个其表达受CNV调节且与临床结果显著相关的基因(和),并且发现和的缺失可能对AML具有保护作用。这五个基因的结果也使用患者骨髓样本进行了验证。此外,影响这五个CNV调节基因的CNV分布与风险组(有利、中等和不利风险组)无关。
结论
总体而言,本研究鉴定了102个与患者生存相关的CNV相关基因,并鉴定了五个其表达受CNV调节且与患者生存相关的基因。我们的发现对于AML新的预后评估模式和靶向治疗的发展至关重要。
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