β受体阻滞剂相关的非缺血性扩张型心肌病逆向重构的治疗分子表型
Therapeutic Molecular Phenotype of β-Blocker-Associated Reverse-Remodeling in Nonischemic Dilated Cardiomyopathy.
作者信息
Kao David P, Lowes Brian D, Gilbert Edward M, Minobe Wayne, Epperson L Elaine, Meyer Leslie K, Ferguson Debra A, Volkman Ann Kirkpatrick, Zolty Ronald, Borg C Douglas, Quaife Robert A, Bristow Michael R
机构信息
From the Division of Cardiology, Department of Medicine, University of Colorado School of Medicine, Aurora (D.P.K., W.M., L.E.E., L.K.M., D.A.F., R.A.Q., M.R.B.); Division of Cardiology, Department of Medicine, University of Nebraska Medical Center, Omaha (B.D.L.); Division of Cardiology, Department of Medicine, University of Utah, Salt Lake City (E.M.G., A.K.V.); Division of Cardiology, Department of Medicine, Albert Einstein College of Medicine, Bronx, NY (R.Z.); and Heart Clinic of Arkansas, Little Rock (C.D.B.).
出版信息
Circ Cardiovasc Genet. 2015 Apr;8(2):270-83. doi: 10.1161/CIRCGENETICS.114.000767. Epub 2015 Jan 30.
BACKGROUND
When β-blockers produce reverse-remodeling in idiopathic dilated cardiomyopathy, they partially reverse changes in fetal-adult/contractile protein, natriuretic peptide, SR-Ca(2+)-ATPase gene program constituents. The objective of the current study was to further test the hypothesis that reverse-remodeling is associated with favorable changes in myocardial gene expression by measuring additional contractile, signaling, and metabolic genes that exhibit a fetal/adult expression predominance, are thyroid hormone-responsive, and are regulated by β1-adrenergic receptor signaling. A secondary objective was to identify which of these putative regulatory networks is most closely associated with observed changes.
METHODS AND RESULTS
Forty-seven patients with idiopathic dilated cardiomyopathy (left ventricular ejection fraction, 0.24±0.09) were randomized to the adrenergic-receptor blockers metoprolol (β1-selective), metoprolol+doxazosin (β1/α1), or carvedilol (β1/β2/α1). Serial radionuclide ventriculography and endomyocardial biopsies were performed at baseline, 3, and 12 months. Expression of 50 mRNA gene products was measured by quantitative polymerase chain reaction. Thirty-one patients achieved left ventricular ejection fraction reverse-remodeling response defined as improvement by ≥0.08 at 12 months or by ≥0.05 at 3 months (Δ left ventricular ejection fraction, 0.21±0.10). Changes in gene expression in responders versus nonresponders were decreases in NPPA and NPPB and increases in MYH6, ATP2A2, PLN, RYR2, ADRA1A, ADRB1, MYL3, PDFKM, PDHX, and CPT1B. All except PDHX involved increase in adult or decrease in fetal cardiac genes, but 100% were concordant with changes predicted by inhibition of β1-adrenergic signaling.
CONCLUSIONS
In addition to known gene expression changes, additional calcium-handling, sarcomeric, adrenergic signaling, and metabolic genes were associated with reverse-remodeling. The pattern suggests a fetal-adult paradigm but may be because of reversal of gene expression controlled by a β1-adrenergic receptor gene network.
CLINICAL TRIAL REGISTRATION
URL: www.clinicaltrials.gov. Unique Identifier: NCT01798992.
背景
当β受体阻滞剂在特发性扩张型心肌病中产生逆向重构时,它们会部分逆转胎儿-成人/收缩蛋白、利钠肽、肌浆网钙-ATP酶基因程序成分的变化。本研究的目的是通过测量额外的收缩、信号传导和代谢基因,进一步检验逆向重构与心肌基因表达的有利变化相关的假设,这些基因表现出胎儿/成人表达优势、对甲状腺激素有反应且受β1-肾上腺素能受体信号调节。第二个目的是确定这些假定的调控网络中哪一个与观察到的变化最密切相关。
方法与结果
47例特发性扩张型心肌病患者(左心室射血分数为0.24±0.09)被随机分为肾上腺素能受体阻滞剂美托洛尔(β1选择性)、美托洛尔+多沙唑嗪(β1/α1)或卡维地洛(β1/β2/α1)组。在基线、3个月和12个月时进行系列放射性核素心室造影和心内膜心肌活检。通过定量聚合酶链反应测量50种mRNA基因产物的表达。31例患者实现了左心室射血分数逆向重构反应,定义为12个月时改善≥0.08或3个月时改善≥0.05(左心室射血分数变化量为0.21±0.10)。反应者与非反应者基因表达的变化为NPPA和NPPB降低,MYH6、ATP2A2、PLN、RYR2、ADRA1A、ADRB1、MYL3、PDFKM、PDHX和CPT1B升高。除PDHX外,所有基因均涉及成人心脏基因增加或胎儿心脏基因减少,但100%与β1-肾上腺素能信号抑制预测的变化一致。
结论
除了已知的基因表达变化外,额外的钙处理、肌节、肾上腺素能信号传导和代谢基因与逆向重构相关。这种模式提示了胎儿-成人模式,但可能是由于β1-肾上腺素能受体基因网络控制的基因表达逆转。
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