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模拟哺乳动物心肌中细肌丝近邻协同相互作用的影响。

Modeling the effects of thin filament near-neighbor cooperative interactions in mammalian myocardium.

作者信息

Phan Tuan A, Fitzsimons Daniel P

机构信息

Institute for Modeling Collaboration and Innovation, University of Idaho , Moscow, ID, USA.

Department of Animal, Veterinary, and Food Sciences, College of Agricultural and Life Sciences, University of Idaho, Moscow, ID, USA.

出版信息

J Gen Physiol. 2025 Mar 3;157(2). doi: 10.1085/jgp.202413582. Epub 2025 Jan 27.

Abstract

The mechanisms underlying cooperative activation and inactivation of myocardial force extend from local, near-neighbor interactions involving troponin-tropomyosin regulatory units (RU) and crossbridges (XB) to more global interactions across the sarcomere. To better understand these mechanisms in the hearts of small and large mammals, we undertook a simplified mathematical approach to assess the contribution of three types of near-neighbor cooperative interactions, i.e., RU-induced, RU-activation (RU-RU), crossbridge-induced, crossbridge-binding (XB-XB), and XB-induced, RU-activation (XB-RU). We measured the Ca2+ and activation dependence of the rate constant of force redevelopment in murine- and porcine-permeabilized ventricular myocardium. Mathematical modeling of these three near-neighbor interactions yielded nonlinear expressions for the RU-RU and XB-RU rate coefficients (kon and koff) and XB-XB rate coefficients describing the attachment of force-generating crossbridges (f and f'). The derivation of single cooperative coefficient parameters (u = RU-RU, w = XB-RU, and v = XB-XB) permitted an initial assessment of the strength of each near-neighbor interaction. The parameter sets describing the effects of discrete XB-XB or XB-RU interactions failed to adequately fit the in vitro contractility data in either murine or porcine myocardium. However, the Ca2+ dependence of ktr in murine and porcine ventricular myocardium was well fit by parameter sets incorporating the RU-RU cooperative interaction. Our results indicate that a significantly stronger RU-RU interaction is present in porcine ventricular myocardium compared with murine ventricular myocardium and that the relative strength of the near-neighbor RU-RU interaction contributes to species-specific myocardial contractile dynamics in small and large mammals.

摘要

心肌力协同激活和失活的潜在机制,从涉及肌钙蛋白 - 原肌球蛋白调节单位(RU)和横桥(XB)的局部近邻相互作用,延伸到整个肌节的更全局相互作用。为了更好地理解小型和大型哺乳动物心脏中的这些机制,我们采用了一种简化的数学方法,来评估三种近邻协同相互作用的贡献,即RU诱导的、RU激活(RU - RU)、横桥诱导的、横桥结合(XB - XB)以及XB诱导的、RU激活(XB - RU)。我们测量了小鼠和猪透化心室心肌中力重建速率常数的Ca²⁺和激活依赖性。对这三种近邻相互作用的数学建模,得出了RU - RU和XB - RU速率系数(kon和koff)以及描述产生力的横桥附着的XB - XB速率系数(f和f')的非线性表达式。单个协同系数参数(u = RU - RU,w = XB - RU,v = XB - XB)的推导,允许对每种近邻相互作用的强度进行初步评估。描述离散XB - XB或XB - RU相互作用影响的参数集,未能充分拟合小鼠或猪心肌的体外收缩性数据。然而,结合了RU - RU协同相互作用的参数集,很好地拟合了小鼠和猪心室心肌中ktr的Ca²⁺依赖性。我们的结果表明,与小鼠心室心肌相比,猪心室心肌中存在明显更强的RU - RU相互作用,并且近邻RU - RU相互作用的相对强度,有助于小型和大型哺乳动物中物种特异性的心肌收缩动力学。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8475/11771317/46010026c03b/jgp_202413582_fig1.jpg

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