首页> 外文会议>PSB;Pacific symposium on biocomputing; 20090105-09;20090105-09; Kohala Coast, HI(US);Kohala Coast, HI(US) >TOWARDS COMPUTATIONAL MODELING OF EXCITATION-CONTRACTION COUPLING IN CARDIAC MYOCYTES: RECONSTRUCTION OF STRUCTURES AND PROTEINS FROM CONFOCAL IMAGING
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TOWARDS COMPUTATIONAL MODELING OF EXCITATION-CONTRACTION COUPLING IN CARDIAC MYOCYTES: RECONSTRUCTION OF STRUCTURES AND PROTEINS FROM CONFOCAL IMAGING

机译:心肌细胞兴奋-收缩耦合计算模型的研究:共聚焦成像重建结构和蛋白质

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Computational models of excitation-contraction (EC) coupling in myocytes are valuable tools for studying the signaling cascade that transduces transmembrane voltage into mechanical responses. A key component of these models is the appropriate description of structures involved in EC coupling, such as the sarcolemma and ion channels. This study aims at developing an approach for spatial reconstruction of these structures. We exemplified our approach by reconstructing clusters of ryanodine receptors (RyRs) together with the sarcolemma of rabbit ventricular myocytes. The reconstructions were based on dual labeling and three-dimensional (3D) confocal imaging of segments of fixed and permeabilized myocytes lying flat or on end. The imaging led to 3D stacks of cross-sections through myocytes. Methods of digital image processing were applied to deconvolve, filter and segment these stacks. Finally, we created point meshes representing RyR distributions together with volume and surface meshes of the sarcolemma. We suggest that these meshes are suitable for computational studies of structure-function relationships in EC conpling. We propose that this approach can be extended to reconstruct other structures and proteins involved in EC coupling.
机译:肌细胞中兴奋收缩(EC)耦合的计算模型是研究将跨膜电压转换成机械反应的信号级联的有价值的工具。这些模型的关键组成部分是对EC耦合涉及的结构的适当描述,例如肌膜和离子通道。这项研究旨在开发一种空间重建这些结构的方法。我们通过重建ryanodine受体(RyRs)簇以及兔心室肌细胞的肌膜来举例说明我们的方法。重建是基于双标记和平面或末端固定和透化的心肌细胞节的三维(3D)共聚焦成像。成像导致穿过心肌细胞的3D横截面堆栈。应用数字图像处理方法对这些堆栈进行反卷积,滤波和分割。最后,我们创建了代表RyR分布的点网格,以及肉瘤的体积和表面网格。我们建议这些网格适用于EC交叠中结构-功能关系的计算研究。我们建议可以将此方法扩展为重建参与EC耦合的其他结构和蛋白质。

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