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T 小管的扩散和电导特性由其狭窄和扩张决定。

Diffusional and Electrical Properties of T-Tubules Are Governed by Their Constrictions and Dilations.

机构信息

Department of Molecular and Integrative Physiology, University of Michigan, Ann Arbor, Michigan.

Department of Molecular and Integrative Physiology, University of Michigan, Ann Arbor, Michigan.

出版信息

Biophys J. 2018 Jan 23;114(2):437-449. doi: 10.1016/j.bpj.2017.11.3742.

Abstract

Cardiac t-tubules (TTs) form a network of complex surface membrane invaginations that is essential for proper excitation-contraction coupling. Although electron and optical microscopy studies provided a wealth of important information about the structure of TTs, assessing their functional properties remains a challenge. In this study, we investigated the diffusional accessibility of TTs in intact isolated adult mouse ventricular myocytes using, to our knowledge, a novel fluorescence-based assay. In this approach, a small part of TTs is first locally filled with fluorescent dextran and then its diffusion out of TTs is monitored after rapid removal of extracellular dextran. In normal cells, diffusion of 3 kDa dextran is characterized by an average time constant of 3.9 ± 1.2 s with the data ranging from 1.8 to 10.5 s. The data are consistent with essentially free diffusion of dextran in TTs although measurable contribution of binding is also evident. TT fluorescence is abolished in cells treated with high concentration of formamide or after hyposmotic stress. Importantly, the assay we use allows for quantitative, repetitive measurements of subtle dynamic changes in TT structure of the same cell that are not possible to observe with other approaches. In particular, dextran diffusion rate decreases two-to-threefold during cell swelling, suggesting significant structural remodeling of TTs. Computer modeling shows that diffusional accessibility and electrical properties of TTs are primarily determined by the constrictions and dilations of individual TTs and that, from a functional perspective, TTs cannot be considered as a network of cylinders of the same average diameter. Constriction/dilation model of cardiac TTs is in a quantitative agreement with previous high-resolution microscopy studies of TT structure and alternative measurements of diffusional and electrical time constants of TTs. The data also show that the apparent electrical length constant of cardiac TTs is likely several-fold smaller than that estimated in earlier studies.

摘要

心肌 T 小管(TTs)形成了复杂的细胞膜内陷网络,对于正常的兴奋-收缩偶联至关重要。尽管电子显微镜和光学显微镜研究为 TTs 的结构提供了大量重要信息,但评估其功能特性仍然是一个挑战。在这项研究中,我们使用一种新颖的荧光基础测定法,研究了完整的分离成年小鼠心室肌细胞中 TTs 的扩散可及性。在这种方法中,首先将 TTs 的一小部分局部填充荧光葡聚糖,然后在快速去除细胞外葡聚糖后监测其从 TTs 中的扩散。在正常细胞中,3 kDa 葡聚糖的扩散特征是平均时间常数为 3.9 ± 1.2 s,数据范围为 1.8 至 10.5 s。这些数据与葡聚糖在 TTs 中基本自由扩散一致,尽管也可以明显看出结合的可测量贡献。用高浓度甲酰胺处理或在低渗应激后,TT 荧光会被消除。重要的是,我们使用的测定法允许对同一细胞中 TT 结构的细微动态变化进行定量、重复测量,而其他方法则无法观察到这些变化。特别是,在细胞肿胀过程中,葡聚糖扩散率降低了两到三倍,这表明 TTs 的结构发生了显著的重塑。计算机建模表明,TTs 的扩散可及性和电学特性主要由单个 TTs 的收缩和扩张决定,从功能角度来看,TTs 不能被视为相同平均直径的圆柱网络。心脏 TTs 的收缩/扩张模型与之前 TTs 结构的高分辨率显微镜研究和 TTs 的扩散和电时间常数的替代测量结果在定量上是一致的。这些数据还表明,心脏 TTs 的表观电长度常数可能比早期研究中估计的要小几个数量级。

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