AI Article Synopsis
- MOG1 is a crucial protein that interacts with the cardiac sodium channel Nav 1.5, influencing its physiological function and implicating it in cardiac arrhythmias when mutated.
- Through various experiments, including yeast two-hybrid screens and co-immunoprecipitation assays, it was shown that MOG1 enhances sodium current densities by increasing the cell surface expression of Nav 1.5 in both HEK293 cells and cardiac myocytes.
- MOG1 is predominantly expressed in heart tissues, particularly at intercalated discs, and plays a significant role in regulating sodium channel function, highlighting its importance in cardiac health.
Article Abstract
The cardiac sodium channel Nav 1.5 is essential for the physiological function of the heart and contributes to lethal cardiac arrhythmias and sudden death when mutated. Here, we report that MOG1, a small protein that is highly conserved from yeast to humans, is a central component of the channel complex and modulates the physiological function of Nav 1.5. The yeast two-hybrid screen identified MOG1 as a new protein that interacts with the cytoplasmic loop II (between transmembrane domains DII and DIII) of Nav 1.5. The interaction was further demonstrated by both in vitro glutathione S-transferase pull-down and in vivo co-immunoprecipitation assays in both HEK293 cells with co-expression of MOG1 and Nav1.5 and native cardiac cells. Co-expression of MOG1 with Nav1.5 in HEK293 cells increased sodium current densities. In neonatal myocytes, overexpression of MOG1 increased current densities nearly 2-fold. Western blot analysis revealed that MOG1 increased cell surface expression of Nav1.5, which may be the underlying mechanism by which MOG1 increased sodium current densities. Immunostaining revealed that in the heart, MOG1 was expressed in both atrial and ventricular tissues with predominant localization at the intercalated discs. In cardiomyocytes, MOG1 is mostly localized in the cell membrane and co-localized with Nav1.5. These results indicate that MOG1 is a critical regulator of sodium channel function in the heart and reveal a new cellular function for MOG1. This study further demonstrates the functional diversity of Nav1.5-binding proteins, which serve important functions for Nav1.5 under different cellular conditions.
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| http://dx.doi.org/10.1074/jbc.M709721200 | DOI Listing |
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