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2'-脱氧三磷酸腺苷对心肌钙处理影响的多尺度计算建模

Multiscale computational modeling of the effects of 2'-deoxy-ATP on cardiac muscle calcium handling.

作者信息

Hock Marcus T, Teitgen Abigail E, McCabe Kimberly J, Hirakis Sophia P, Huber Gary A, Regnier Michael, Amaro Rommie E, McCammon J Andrew, McCulloch Andrew D

机构信息

Department of Bioengineering, University of California San Diego, La Jolla, California 92093, USA.

Department of Computational Physiology, Simula Resesarch Laboratory, Oslo 0164, Norway.

出版信息

J Appl Phys. 2023 Aug 21;134(7):074905. doi: 10.1063/5.0157935. Epub 2023 Aug 16.

Abstract

2'-Deoxy-ATP (dATP), a naturally occurring near analog of ATP, is a well-documented myosin activator that has been shown to increase contractile force, improve pump function, and enhance lusitropy in the heart. Calcium transients in cardiomyocytes with elevated levels of dATP show faster calcium decay compared with cardiomyocytes with basal levels of dATP, but the mechanisms behind this are unknown. Here, we design and utilize a multiscale computational modeling framework to test the hypothesis that dATP acts on the sarcoendoplasmic reticulum calcium-ATPase (SERCA) pump to accelerate calcium re-uptake into the sarcoplasmic reticulum during cardiac relaxation. Gaussian accelerated molecular dynamics simulations of human cardiac SERCA2A in the E1 , ATP-bound and dATP-bound states showed that dATP forms more stable contacts in the nucleotide binding pocket of SERCA and leads to increased closure of cytosolic domains. These structural changes ultimately lead to changes in calcium binding, which we assessed using Brownian dynamics simulations. We found that dATP increases calcium association rate constants to SERCA and that dATP binds to SERCA more rapidly than ATP. Using a compartmental ordinary differential equation model of human cardiomyocyte excitation-contraction coupling, we found that these increased association rate constants contributed to the accelerated rates of calcium transient decay observed experimentally. This study provides clear mechanistic evidence of enhancements in cardiac SERCA2A pump function due to interactions with dATP.

摘要

2'-脱氧三磷酸腺苷(dATP)是一种天然存在的与三磷酸腺苷(ATP)极为相似的物质,是一种有充分文献记载的肌球蛋白激活剂,已被证明可增加收缩力、改善泵功能并增强心脏舒张功能。与处于dATP基础水平的心肌细胞相比,dATP水平升高的心肌细胞中的钙瞬变显示出更快的钙衰减,但其背后的机制尚不清楚。在这里,我们设计并利用了一个多尺度计算建模框架来检验以下假设:dATP作用于肌浆网钙-ATP酶(SERCA)泵,以在心脏舒张期间加速钙重新摄取到肌浆网中。对处于E1、ATP结合状态和dATP结合状态的人类心脏SERCA2A进行的高斯加速分子动力学模拟表明,dATP在SERCA的核苷酸结合口袋中形成更稳定的接触,并导致胞质结构域的闭合增加。这些结构变化最终导致钙结合的变化,我们使用布朗动力学模拟对此进行了评估。我们发现dATP增加了钙与SERCA的结合速率常数,并且dATP比ATP更快地与SERCA结合。使用人类心肌细胞兴奋-收缩偶联的房室常微分方程模型,我们发现这些增加的结合速率常数促成了实验中观察到的钙瞬变衰减速率的加快。这项研究提供了明确的机制证据,证明由于与dATP的相互作用,心脏SERCA2A泵功能得到增强。

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