CELF4基因变异与蒽环类药物相关心肌病:儿童肿瘤研究组全基因组关联研究
CELF4 Variant and Anthracycline-Related Cardiomyopathy: A Children's Oncology Group Genome-Wide Association Study.
作者信息
Wang Xuexia, Sun Can-Lan, Quiñones-Lombraña Adolfo, Singh Purnima, Landier Wendy, Hageman Lindsey, Mather Molly, Rotter Jerome I, Taylor Kent D, Chen Yii-Der Ida, Armenian Saro H, Winick Naomi, Ginsberg Jill P, Neglia Joseph P, Oeffinger Kevin C, Castellino Sharon M, Dreyer Zoann E, Hudson Melissa M, Robison Leslie L, Blanco Javier G, Bhatia Smita
机构信息
Xuexia Wang, University of Wisconsin-Milwaukee, Milwaukee, WI; Can-Lan Sun, Molly Mather, Saro H. Armenian, City of Hope, Duarte; Jerome I. Rotter, Kent D. Taylor, Yii-Der Ida Chen, Los Angeles Biomedical Research Institute at Harbor-University of California, Los Angeles, Torrance, CA; Adolfo Quiñones-Lombraña, Javier G. Blanco, State University of New York at Buffalo, Buffalo; Kevin C. Oeffinger, Memorial Sloan Kettering Cancer Center, New York, NY; Purnima Singh, Wendy Landier, Lindsey Hageman, Smita Bhatia, University of Alabama at Birmingham, Birmingham, AL; Naomi Winick, University of Texas Southwestern Medical Center, Dallas; Zoann E. Dreyer, Texas Children's Cancer Center, Houston, TX; Jill P. Ginsberg, Childrens Hospital of Philadelphia, Philadelphia, PA; Joseph P. Neglia, University of Minnesota, Minneapolis, MN; Sharon M. Castellino, Emory University and Children's Healthcare of Atlanta, Atlanta, GA; and Melissa M. Hudson, Leslie L. Robison, St Jude Children's Research Hospital, Memphis, TN.
出版信息
J Clin Oncol. 2016 Mar 10;34(8):863-70. doi: 10.1200/JCO.2015.63.4550. Epub 2016 Jan 25.
PURPOSE
Interindividual variability in the dose-dependent association between anthracyclines and cardiomyopathy suggests that genetic susceptibility could play a role. The current study uses an agnostic approach to identify genetic variants that could modify cardiomyopathy risk.
METHODS
A genome-wide association study was conducted in childhood cancer survivors with and without cardiomyopathy (cases and controls, respectively). Single-nucleotide polymorphisms (SNPs) that surpassed a prespecified threshold for statistical significance were independently replicated. The possible mechanistic significance of validated SNP(s) was sought by using healthy heart samples.
RESULTS
No SNP was marginally associated with cardiomyopathy. However, SNP rs1786814 on the CELF4 gene passed the significance cutoff for gene-environment interaction (Pge = 1.14 × 10(-5)). Multivariable analyses adjusted for age at cancer diagnosis, sex, anthracycline dose, and chest radiation revealed that, among patients with the A allele, cardiomyopathy was infrequent and not dose related. However, among those exposed to greater than 300 mg/m(2) of anthracyclines, the rs1786814 GG genotype conferred a 10.2-fold (95% CI, 3.8- to 27.3-fold; P < .001) increased risk of cardiomyopathy compared with those who had GA/AA genotypes and anthracycline exposure of 300 mg/m(2) or less. This gene-environment interaction was successfully replicated in an independent set of anthracycline-related cardiomyopathy. CUG-BP and ETR-3-like factor proteins control developmentally regulated splicing of TNNT2, the gene that encodes for cardiac troponin T (cTnT), a biomarker of myocardial injury. Coexistence of more than one cTnT variant results in a temporally split myofilament response to calcium, which causes decreased contractility. Analysis of TNNT2 splicing variants in healthy human hearts suggested an association between the rs1786814 GG genotype and coexistence of more than one TNNT2 splicing variant (90.5% GG v 41.7% GA/AA; P = .005).
CONCLUSION
We report a modifying effect of a polymorphism of CELF4 (rs1786814) on the dose-dependent association between anthracyclines and cardiomyopathy, which possibly occurs through a pathway that involves the expression of abnormally spliced TNNT2 variants.
目的
蒽环类药物与心肌病之间剂量依赖性关联的个体间差异表明,遗传易感性可能起作用。本研究采用一种无偏倚的方法来识别可能改变心肌病风险的基因变异。
方法
对患有和未患心肌病的儿童癌症幸存者(分别为病例组和对照组)进行全基因组关联研究。超过预先设定的统计学显著性阈值的单核苷酸多态性(SNP)进行独立验证。通过使用健康心脏样本探究已验证SNP的可能机制意义。
结果
没有SNP与心肌病有边缘关联。然而,CELF4基因上的SNP rs1786814通过了基因 - 环境相互作用的显著性阈值(Pge = 1.14×10⁻⁵)。对癌症诊断时的年龄、性别、蒽环类药物剂量和胸部放疗进行多变量分析显示,在携带A等位基因的患者中,心肌病不常见且与剂量无关。然而,在接受超过300 mg/m²蒽环类药物治疗的患者中,与携带GA/AA基因型且蒽环类药物暴露量为300 mg/m²或更低的患者相比,rs1786814 GG基因型使心肌病风险增加了10.2倍(95% CI,3.8至27.3倍;P <.001)。这种基因 - 环境相互作用在一组独立的蒽环类药物相关心肌病中成功得到验证。CUG - BP和ETR - 3样因子蛋白控制TNNT2(编码心肌肌钙蛋白T(cTnT)的基因,cTnT是心肌损伤的生物标志物)的发育调控剪接。多种cTnT变体共存导致肌丝对钙的反应在时间上出现分裂,从而导致收缩力下降。对健康人心脏中TNNT2剪接变体的分析表明,rs1786814 GG基因型与多种TNNT2剪接变体共存之间存在关联(90.5%为GG,41.7%为GA/AA;P =.005)。
结论
我们报告了CELF4基因多态性(rs1786814)对蒽环类药物与心肌病之间剂量依赖性关联的修饰作用,这可能通过涉及异常剪接的TNNT2变体表达的途径发生。
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