作者
Daniël A Pijnappels, John van Tuyn, Antoine AF de Vries, Robert W Grauss, Arnoud van der Laarse, Dirk L Ypey, Douwe E Atsma, Martin J Schalij
发表日期
2007/10/30
期刊
Circulation
卷号
116
期号
18
页码范围
2018-2028
出版商
Lippincott Williams & Wilkins
简介
Background— Nonresponse to cardiac resynchronization therapy is associated with the presence of slow or nonconducting scar tissue. Genetic modification of scar tissue, aimed at improving conduction, may be a novel approach to achieve effective resynchronization. Therefore, the feasibility of resynchronization with genetically modified human ventricular scar fibroblasts was studied in a coculture model.
Methods and Results— An in vitro model was used to study the effects of forced expression of the myocardin (MyoC) gene in human ventricular scar fibroblasts (hVSFs) on resynchronization of 2 rat cardiomyocyte fields separated by a strip of hVSFs. Furthermore, the effects of MyoC expression on the capacity of hVSFs to serve as pacing sites were studied. MyoC-dependent gene activation in hVSFs was examined by gene and immunocytochemical analysis. Forced MyoC expression in hVSFs decreased …
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