作者
Sabina Kupershmidt, Iris C-H Yang, Margaret Sutherland, K Sam Wells, Tao Yang, Ping Yang, Jeffrey R Balser, Dan M Roden
发表日期
2002/10/1
期刊
Cardiovascular research
卷号
56
期号
1
页码范围
93-103
出版商
Elsevier Science
简介
Objective: Co-expression of the KvLQT1 and minK potassium channel subunits is required to recapitulate IKs, the slow component of the cardiac delayed rectifier current, and mutations in either gene cause the congenital Long QT syndrome. It is becoming increasingly well-recognized that multiprotein channel complexes containing proteins capable of modulating channel function assemble at the plasma membrane. Thus, the aim of our study was to identify proteins involved in IKs modulation. Methods and results: Using a yeast-two-hybrid screen with the intracytoplasmic C-terminus of minK as bait, we identified the cardiac-enriched four-and-a-half LIM domain-containing protein (fhl2) as a potential minK partner. We show interaction between the two proteins in GST pulldown assays and demonstrate overlapping subcellular localization using immunocytochemistry of transfected cells supporting a …
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