Circulation:疾病特异性hiPSC-CM预测药物心脏毒性更准确

2013-04-03 高晓方 译 医学论坛网

  美国学者的一项研究表明,疾病特异性人类诱导多能干细胞衍生心肌细胞(hiPSC-CM)可更为准确的预测药物不良反应。论文于2013年3月21日在线发表于《循环》(Circulation)。   此项研究构建了来自于健康受试者以及遗传性QT间期延长综合征(LQT)、家族性肥厚性心肌病(HCM)和家族性扩张性心肌病(DCM)患者的hiPSC-CM细胞库,并在单细胞水平测定了动作电位时程(APD)和

  美国学者的一项研究表明,疾病特异性人类诱导多能干细胞衍生心肌细胞(hiPSC-CM)可更为准确的预测药物不良反应。论文于2013年3月21日在线发表于《循环》(Circulation)。

  此项研究构建了来自于健康受试者以及遗传性QT间期延长综合征(LQT)、家族性肥厚性心肌病(HCM)和家族性扩张性心肌病(DCM)患者的hiPSC-CM细胞库,并在单细胞水平测定了动作电位时程(APD)和药物诱导的心律失常。利用免疫染色和单细胞膜片钳确认疾病表型。以人类胚胎干细胞衍生心肌细胞(hESC-CM)和表达人类eag相关基因(hERG)的人胚肾(HEK293)细胞作为对照。

  结果显示,单细胞PCR证实,患者特异性hiPSC-CM和hESC-CM中均表达所有心脏离子通道,但HEK293细胞未表达。APD测定以及早期后除极化(EAD)和延迟后去极化(DAD)等药物诱导心律失常定量分析显示,疾病特异性hiPSC-CM对已知心脏毒性药物的敏感性升高。


Drug Screening Using a Library of Human Induced Pluripotent Stem Cell-Derived Cardiomyocytes Reveals Disease Specific Patterns of Cardiotoxicity

Background
Cardiotoxicity is a leading cause for drug attrition during pharmaceutical development and has resulted in numerous preventable patient deaths. Incidents of adverse cardiac drug reactions are more common in patients with pre-existing heart disease than the general population. Here we generated a library of human induced pluripotent stem cell-derived cardiomyocytes (hiPSC-CMs) from patients with various hereditary cardiac disorders to model differences in cardiac drug toxicity susceptibility for patients of different genetic backgrounds.
Methods and Results
Action potential duration (APD) and drug-induced arrhythmia were measured at the single cell level in hiPSC-CMs derived from healthy subjects and patients with hereditary long QT syndrome (LQT), familial hypertrophic cardiomyopathy (HCM), and familial dilated cardiomyopathy (DCM). Disease phenotypes were verified in LQT, HCM, and DCM iPSC-CMs by immunostaining and single cell patch clamp. Human embryonic stem cell-derived cardiomyocytes (hESC-CMs) and the human ether-a-go-go-related gene (hERG) expressing human embryonic kidney (HEK293) cells were used as controls. Single cell PCR confirmed expression of all cardiac ion channels in patient-specific hiPSC-CMs as well as hESC-CMs, but not in HEK293 cells. Disease-specific hiPSC-CMs demonstrated increased susceptibility to known cardiotoxic drugs as measured by APD and quantification of drug-induced arrhythmias such as early afterdepolarizations (EADs) and delayed afterdepolarizations (DADs).
Conclusions
We have recapitulated drug-induced cardiotoxicity profiles for healthy subjects, LQT, HCM, and DCM patients at the single cell level for the first time. Our data indicate that healthy and diseased individuals exhibit different susceptibilities to cardiotoxic drugs and that use of disease-specific hiPSC-CMs may predict adverse drug responses more accurately than standard hERG test or healthy control hiPSC-CM/hESC-CM screening assays.

    

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    2013-04-05 chengjn
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    2013-04-05 gjsgj
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    2013-04-05 neurosurgeon