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Publication : Conserved Asp-137 is important for both structure and regulatory functions of cardiac α-tropomyosin (α-TM) in a novel transgenic mouse model expressing α-TM-D137L.

First Author  Yar S Year  2013
Journal  J Biol Chem Volume  288
Issue  23 Pages  16235-46
PubMed ID  23609439 Mgi Jnum  J:199610
Mgi Id  MGI:5503280 Doi  10.1074/jbc.M113.458695
Citation  Yar S, et al. (2013) Conserved Asp-137 is important for both structure and regulatory functions of cardiac alpha-tropomyosin (alpha-TM) in a novel transgenic mouse model expressing alpha-TM-D137L. J Biol Chem 288(23):16235-46
abstractText  alpha-Tropomyosin (alpha-TM) has a conserved, charged Asp-137 residue located in the hydrophobic core of its coiled-coil structure, which is unusual in that the residue is found at a position typically occupied by a hydrophobic residue. Asp-137 is thought to destabilize the coiled-coil and so impart structural flexibility to the molecule, which is believed to be crucial for its function in the heart. A previous in vitro study indicated that the conversion of Asp-137 to a more typical canonical Leu alters flexibility of TM and affects its in vitro regulatory functions. However, the physiological importance of the residue Asp-137 and altered TM flexibility is unknown. In this study, we further analyzed structural properties of the alpha-TM-D137L variant and addressed the physiological importance of TM flexibility in cardiac function in studies with a novel transgenic mouse model expressing alpha-TM-D137L in the heart. Our NMR spectroscopy data indicated that the presence of D137L introduced long range rearrangements in TM structure. Differential scanning calorimetry measurements demonstrated that alpha-TM-D137L has higher thermal stability compared with alpha-TM, which correlated with decreased flexibility. Hearts of transgenic mice expressing alpha-TM-D137L showed systolic and diastolic dysfunction with decreased myofilament Ca(2+) sensitivity and cardiomyocyte contractility without changes in intracellular Ca(2+) transients or post-translational modifications of major myofilament proteins. We conclude that conversion of the highly conserved Asp-137 to Leu results in loss of flexibility of TM that is important for its regulatory functions in mouse hearts. Thus, our results provide insight into the link between flexibility of TM and its function in ejecting hearts.
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