Item Type: | Article |
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Title: | Titin based viscosity in ventricular physiology: An integrative investigation of PEVK-actin interactions |
Creators Name: | Chung, C.S., Methawasin, M., Nelson, O.L., Radke, M.H., Hidalgo, C.G., Gotthardt, M. and Granzier, H.L. |
Abstract: | Viscosity is proposed to modulate diastolic function, but only limited understanding of the source(s) of viscosity exists. In vitro experiments have shown that the proline-glutamic acid-valine-lysine (PEVK) rich element of titin interacts with actin, causing a viscous force in the sarcomere. It is unknown whether this mechanism contributes to viscosity in vivo. We tested the hypothesis that PEVK-actin interaction causes cardiac viscosity and is important in vivo via an integrative physiological study on a unique PEVK knockout (KO) model. Both skinned cardiomyocytes and papillary muscle fibers were isolated from wildtype (WT) and PEVK KO mice and passive viscosity was examined using stretch-hold-release and sinusoidal analysis. Viscosity was reduced by ~60% in KO myocytes and ~50% in muscle fibers at room temperature. The PEVK-actin interaction was not modulated by temperature or diastolic calcium, but was increased by lattice compression. Stretch-hold and sinusoidal frequency protocols on intact isolated mouse hearts showed a smaller, 30-40% reduction in viscosity, possibly due to actomyosin interactions, and showed that microtubules did not contribute to viscosity. Transmitral Doppler echocardiography similarly revealed a 40% decrease in LV chamber viscosity in the PEVK KO in vivo. This integrative study is the first to quantify the influence of a specific molecular (PEVK-actin) viscosity in vivo and shows that PEVK-actin interactions are an important physiological source of viscosity. |
Keywords: | Titin/Connectin, Actin, Diastole, In vivo, Passive Force, Animals, Mice |
Source: | Journal of Molecular and Cellular Cardiology |
ISSN: | 0022-2828 |
Publisher: | Elsevier |
Volume: | 51 |
Number: | 3 |
Page Range: | 428-434 |
Date: | September 2011 |
Official Publication: | https://doi.org/10.1016/j.yjmcc.2011.06.006 |
PubMed: | View item in PubMed |
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