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一种用于评估细胞内区域机械异质性的心肌细胞二维机电模型。

A two dimensional electromechanical model of a cardiomyocyte to assess intra-cellular regional mechanical heterogeneities.

作者信息

Garcia-Canadilla Patricia, Rodriguez Jose F, Palazzi Maria J, Gonzalez-Tendero Anna, Schönleitner Patrick, Balicevic Vedrana, Loncaric Sven, Luiken Joost J F P, Ceresa Mario, Camara Oscar, Antoons Gudrun, Crispi Fatima, Gratacos Eduard, Bijnens Bart

机构信息

Dept. of Information and Communication Technologies, Universitat Pompeu Fabra, Barcelona, Spain.

LaBS, Chemistry, materials and chemical engineering department "Giulio Natta", Politecnico di Milano, Milano, Italy.

出版信息

PLoS One. 2017 Aug 24;12(8):e0182915. doi: 10.1371/journal.pone.0182915. eCollection 2017.

Abstract

Experimental studies on isolated cardiomyocytes from different animal species and human hearts have demonstrated that there are regional differences in the Ca2+ release, Ca2+ decay and sarcomere deformation. Local deformation heterogeneities can occur due to a combination of factors: regional/local differences in Ca2+ release and/or re-uptake, intra-cellular material properties, sarcomere proteins and distribution of the intracellular organelles. To investigate the possible causes of these heterogeneities, we developed a two-dimensional finite-element electromechanical model of a cardiomyocyte that takes into account the experimentally measured local deformation and cytosolic [Ca2+] to locally define the different variables of the constitutive equations describing the electro/mechanical behaviour of the cell. Then, the model was individualised to three different rat cardiac cells. The local [Ca2+] transients were used to define the [Ca2+]-dependent activation functions. The cell-specific local Young's moduli were estimated by solving an inverse problem, minimizing the error between the measured and simulated local deformations along the longitudinal axis of the cell. We found that heterogeneities in the deformation during contraction were determined mainly by the local elasticity rather than the local amount of Ca2+, while in the relaxation phase deformation was mainly influenced by Ca2+ re-uptake. Our electromechanical model was able to successfully estimate the local elasticity along the longitudinal direction in three different cells. In conclusion, our proposed model seems to be a good approximation to assess the heterogeneous intracellular mechanical properties to help in the understanding of the underlying mechanisms of cardiomyocyte dysfunction.

摘要

对来自不同动物物种和人类心脏的离体心肌细胞进行的实验研究表明,钙释放、钙衰减和肌节变形存在区域差异。局部变形异质性可能由多种因素共同导致:钙释放和/或再摄取的区域/局部差异、细胞内物质特性、肌节蛋白以及细胞内细胞器的分布。为了研究这些异质性的可能原因,我们建立了一个心肌细胞的二维有限元机电模型,该模型考虑了实验测量的局部变形和胞质[Ca2+],以局部定义描述细胞电/机械行为的本构方程的不同变量。然后,该模型针对三种不同的大鼠心脏细胞进行了个体化。局部[Ca2+]瞬变用于定义[Ca2+]依赖性激活函数。通过解决一个反问题来估计细胞特异性局部杨氏模量,即最小化沿细胞纵轴测量的和模拟的局部变形之间的误差。我们发现,收缩期间变形的异质性主要由局部弹性而非局部钙含量决定,而在舒张期,变形主要受钙再摄取的影响。我们的机电模型能够成功估计三种不同细胞沿纵向的局部弹性。总之,我们提出的模型似乎是评估细胞内异质力学特性的一个很好的近似方法,有助于理解心肌细胞功能障碍的潜在机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e5e8/5570434/5c467eb4045d/pone.0182915.g001.jpg

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