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在衰竭和非衰竭人类心脏中的电生理基因表达的性别差异。

Gender differences in electrophysiological gene expression in failing and non-failing human hearts.

机构信息

Department of Biomedical Engineering, Washington University in St. Louis, St. Louis, Missouri, United States of America.

出版信息

PLoS One. 2013;8(1):e54635. doi: 10.1371/journal.pone.0054635. Epub 2013 Jan 23.

Abstract

The increasing availability of human cardiac tissues for study are critically important in increasing our understanding of the impact of gender, age, and other parameters, such as medications and cardiac disease, on arrhythmia susceptibility. In this study, we aimed to compare the mRNA expression of 89 ion channel subunits, calcium handling proteins, and transcription factors important in cardiac conduction and arrhythmogenesis in the left atria (LA) and ventricles (LV) of failing and nonfailing human hearts of both genders. Total RNA samples, prepared from failing male (n = 9) and female (n = 7), and from nonfailing male (n = 9) and female (n = 9) hearts, were probed using custom-designed Taqman gene arrays. Analyses were performed to explore the relationships between gender, failure state, and chamber expression. Hierarchical cluster analysis revealed chamber specific expression patterns, but failed to identify disease- or gender-dependent clustering. Gender-specific analysis showed lower expression levels in transcripts encoding for K(v)4.3, KChIP2, K(v)1.5, and K(ir)3.1 in the failing female as compared with the male LA. Analysis of LV transcripts, however, did not reveal significant differences based on gender. Overall, our data highlight the differential expression and transcriptional remodeling of ion channel subunits in the human heart as a function of gender and cardiac disease. Furthermore, the availability of such data sets will allow for the development of disease-, gender-, and, most importantly, patient-specific cardiac models, with the ability to utilize such information as mRNA expression to predict cardiac phenotype.

摘要

人类心脏组织越来越容易获得,这对于研究性别、年龄和其他参数(如药物和心脏病)对心律失常易感性的影响至关重要。在这项研究中,我们旨在比较男女两性衰竭和非衰竭人心房(LA)和心室(LV)中 89 个离子通道亚基、钙处理蛋白和心脏传导及心律失常发生中重要的转录因子的 mRNA 表达。使用定制的 Taqman 基因芯片对来自衰竭男性(n = 9)和女性(n = 7)以及非衰竭男性(n = 9)和女性(n = 9)心脏的总 RNA 样本进行了探测。进行了分析以探讨性别、衰竭状态和心腔表达之间的关系。层次聚类分析显示出腔特异性表达模式,但未能确定疾病或性别依赖性聚类。性别特异性分析表明,与男性 LA 相比,衰竭女性中编码 K(v)4.3、KChIP2、K(v)1.5 和 K(ir)3.1 的转录本表达水平较低。然而,对 LV 转录本的分析并未显示出基于性别的显著差异。总体而言,我们的数据强调了人类心脏中离子通道亚基的差异表达和转录重塑是性别和心脏疾病的功能。此外,此类数据集的可用性将允许开发基于疾病、性别、最重要的是基于患者的心脏模型,并能够利用此类 mRNA 表达信息来预测心脏表型。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a1ea/3552854/5ac8e9f2dd71/pone.0054635.g001.jpg

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