Coupling Langevin Dynamics With Continuum Mechanics: Exposing the Role of Sarcomere Stretch Activation Mechanisms to Cardiac Function

Takumi Washio; Takumi Washio; Seiryo Sugiura; Seiryo Sugiura; Ryo Kanada; Jun-Ichi Okada; Jun-Ichi Okada; Toshiaki Hisada; Toshiaki Hisada

doi:10.3389/fphys.2018.00333

Frontiers in Physiology (Apr 2018)

Coupling Langevin Dynamics With Continuum Mechanics: Exposing the Role of Sarcomere Stretch Activation Mechanisms to Cardiac Function

Takumi Washio,
Takumi Washio,
Seiryo Sugiura,
Seiryo Sugiura,
Ryo Kanada,
Jun-Ichi Okada,
Jun-Ichi Okada,
Toshiaki Hisada,
Toshiaki Hisada

Affiliations

Takumi Washio: UT-Heart Inc., Kashiwa, Japan
Takumi Washio: Graduate School of Frontier Sciences, University of Tokyo, Kashiwa, Japan
Seiryo Sugiura: UT-Heart Inc., Kashiwa, Japan
Seiryo Sugiura: Graduate School of Frontier Sciences, University of Tokyo, Kashiwa, Japan
Ryo Kanada: Predictive Health Team, Integrated Research Group, Compass to Healthy Life Research Complex Program, RIKEN, Kobe, Japan
Jun-Ichi Okada: UT-Heart Inc., Kashiwa, Japan
Jun-Ichi Okada: Graduate School of Frontier Sciences, University of Tokyo, Kashiwa, Japan
Toshiaki Hisada: UT-Heart Inc., Kashiwa, Japan
Toshiaki Hisada: Graduate School of Frontier Sciences, University of Tokyo, Kashiwa, Japan

DOI: https://doi.org/10.3389/fphys.2018.00333
Journal volume & issue: Vol. 9

Abstract

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High-performance computing approaches that combine molecular-scale and macroscale continuum mechanics have long been anticipated in various fields. Such approaches may enrich our understanding of the links between microscale molecular mechanisms and macroscopic properties in the continuum. However, there have been few successful examples to date owing to various difficulties associated with overcoming the large spatial (from 1 nm to 10 cm) and temporal (from 1 ns to 1 ms) gaps between the two scales. In this paper, we propose an efficient parallel scheme to couple a microscopic model using Langevin dynamics for a protein motor with a finite element continuum model of a beating heart. The proposed scheme allows us to use a macroscale time step that is an order of magnitude longer than the microscale time step of the Langevin model, without loss of stability or accuracy. This reduces the overhead required by the imbalanced loads of the microscale computations and the communication required when switching between scales. An example of the Langevin dynamics model that demonstrates the usefulness of the coupling approach is the molecular mechanism of the actomyosin system, in which the stretch-activation phenomenon can be successfully reproduced. This microscopic Langevin model is coupled with a macroscopic finite element ventricle model. In the numerical simulations, the Langevin dynamics model reveals that a single sarcomere can undergo spontaneous oscillation (15 Hz) accompanied by quick lengthening due to cooperative movements of the myosin molecules pulling on the common Z-line. Also, the coupled simulations using the ventricle model show that the stretch-activation mechanism contributes to the synchronization of the quick lengthening of the sarcomeres at the end of the systolic phase. By comparing the simulation results given by the molecular model with and without the stretch-activation mechanism, we see that this synchronization contributes to maintaining the systolic blood pressure by providing sufficient blood volume without slowing the diastolic process.

Published in Frontiers in Physiology

ISSN: 1664-042X (Online)
Publisher: Frontiers Media S.A.
Country of publisher: Switzerland
LCC subjects: Science: Physiology
Website: https://www.frontiersin.org/journals/physiology

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