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两种犬类心房颤动模型中基因表达谱的对比

Contrasting gene expression profiles in two canine models of atrial fibrillation.

作者信息

Cardin Sophie, Libby Eric, Pelletier Patricia, Le Bouter Sabrina, Shiroshita-Takeshita Akiko, Le Meur Nolwenn, Léger Jean, Demolombe Sophie, Ponton André, Glass Leon, Nattel Stanley

机构信息

Department of Medicine and Research Center, Montreal Heart Institute and Université de Montréal, Montreal, Quebec, Canada.

出版信息

Circ Res. 2007 Feb 16;100(3):425-33. doi: 10.1161/01.RES.0000258428.09589.1a. Epub 2007 Jan 18.

Abstract

Gene-expression changes in atrial fibrillation patients reflect both underlying heart-disease substrates and changes because of atrial fibrillation-induced atrial-tachycardia remodeling. These are difficult to separate in clinical investigations. This study assessed time-dependent mRNA expression-changes in canine models of atrial-tachycardia remodeling and congestive heart failure. Five experimental groups (5 dogs/group) were submitted to atrial (ATP, 400 bpm x 24 hours, 1 or 6 weeks) or ventricular (VTP, 240 bpm x 24 hours or 2 weeks) tachypacing. The expression of approximately 21,700 transcripts was analyzed by microarray in isolated left-atrial cardiomyocytes and (for 18 genes) by real-time RT-PCR. Protein-expression changes were assessed by Western blot. In VTP, a large number of significant mRNA-expression changes occurred after both 24 hours (2209) and 2 weeks (2720). In ATP, fewer changes occurred at 24 hours (242) and fewer still (87) at 1 week, with no statistically-significant alterations at 6 weeks. Expression changes in VTP varied over time in complex ways. Extracellular matrix-related transcripts were strongly upregulated by VTP consistent with its pathophysiology, with 8 collagen-genes upregulated >10-fold, fibrillin-1 8-fold and MMP2 4.5-fold at 2 weeks (time of fibrosis) but unchanged at 24 hours. Other extracellular matrix genes (eg, fibronectin, lysine oxidase-like 2) increased at both time-points ( approximately 10, approximately 5-fold respectively). In ATP, mRNA-changes almost exclusively represented downregulation and were quantitatively smaller. This study shows that VTP-induced congestive heart failure and ATP produce qualitatively different temporally-evolving patterns of gene-expression change, and that specific transcriptomal responses associated with atrial fibrillation versus underlying heart disease substrates must be considered in assessing gene-expression changes in man.

摘要

心房颤动患者的基因表达变化既反映了潜在的心脏病基质,也反映了因心房颤动诱发的房性心动过速重塑所导致的变化。在临床研究中,很难将这两者区分开来。本研究评估了犬房性心动过速重塑和充血性心力衰竭模型中随时间变化的mRNA表达变化。五个实验组(每组5只狗)接受了心房(ATP,400次/分钟×24小时,1或6周)或心室(VTP,240次/分钟×24小时或2周)快速起搏。通过微阵列分析分离的左心房心肌细胞中约21,700个转录本的表达,并(针对18个基因)通过实时RT-PCR进行分析。通过蛋白质印迹评估蛋白质表达变化。在VTP中,24小时(2209个)和2周(2720个)后均发生了大量显著的mRNA表达变化。在ATP中,24小时时变化较少(242个),1周时更少(87个),6周时无统计学显著变化。VTP中的表达变化随时间以复杂的方式变化。与细胞外基质相关的转录本被VTP强烈上调,这与其病理生理学一致,在2周(纤维化时间)时8种胶原基因上调超过10倍,原纤蛋白-1上调8倍,MMP2上调4.5倍,但在24小时时未发生变化。其他细胞外基质基因(如纤连蛋白、赖氨酸氧化酶样2)在两个时间点均增加(分别约为10倍、约5倍)。在ATP中,mRNA变化几乎完全表现为下调,且数量上较少。本研究表明,VTP诱导的充血性心力衰竭和ATP产生了在时间演变上性质不同的基因表达变化模式,并且在评估人类基因表达变化时,必须考虑与心房颤动和潜在心脏病基质相关的特定转录组反应。

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