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细胞内孔隙弹性对工程组织中细胞冷冻诱导变形的作用。

Role of intracellular poroelasticity on freezing-induced deformation of cells in engineered tissues.

作者信息

Ghosh Soham, Ozcelikkale Altug, Dutton J Craig, Han Bumsoo

机构信息

School of Mechanical Engineering, Purdue University, West Lafayette, IN, USA.

Department of Aerospace Engineering, University of Illinois at Urbana-Champaign, Urbana, IL, USA.

出版信息

J R Soc Interface. 2016 Oct;13(123). doi: 10.1098/rsif.2016.0480.

Abstract

Freezing of biomaterials is important in a wide variety of biomedical applications, including cryopreservation and cryosurgeries. For the success of these applications to various biomaterials, biophysical mechanisms, which determine freezing-induced changes in cells and tissues, need to be well understood. Specifically, the significance of the intracellular mechanics during freezing is not well understood. Thus, we hypothesize that cells interact during freezing with the surroundings such as suspension media and the extracellular matrix (ECM) via two distinct but related mechanisms-water transport and cytoskeletal mechanics. The underlying rationale is that the cytoplasm of the cells has poroelastic nature, which can regulate both cellular water transport and cytoskeletal mechanics. A poroelasticity-based cell dehydration model is developed and confirmed to provide insight into the effects of the hydraulic conductivity and stiffness of the cytoplasm on the dehydration of cells in suspension during freezing. We further investigated the effect of the cytoskeletal structures on the cryoresponse of cells embedded in the ECM by measuring the spatio-temporal intracellular deformation with dermal equivalent as a model tissue. The freezing-induced change in cell, nucleus and cytoplasm volume was quantified, and the possible mechanism of the volumetric change was proposed. The results are discussed considering the hierarchical poroelasticity of biological tissues.

摘要

生物材料的冷冻在包括冷冻保存和冷冻手术在内的各种生物医学应用中都很重要。对于这些应用于各种生物材料的成功而言,决定细胞和组织中冷冻诱导变化的生物物理机制需要得到充分理解。具体而言,冷冻过程中细胞内力学的重要性尚未得到充分理解。因此,我们假设细胞在冷冻过程中通过两种不同但相关的机制——水运输和细胞骨架力学,与周围环境如悬浮介质和细胞外基质(ECM)相互作用。其基本原理是细胞的细胞质具有多孔弹性性质,这可以调节细胞的水运输和细胞骨架力学。开发并证实了一种基于多孔弹性的细胞脱水模型,以深入了解细胞质的水力传导率和刚度对冷冻过程中悬浮细胞脱水的影响。我们通过以真皮等效物作为模型组织测量时空细胞内变形,进一步研究了细胞骨架结构对嵌入ECM中的细胞冷冻反应的影响。对冷冻诱导的细胞、细胞核和细胞质体积变化进行了量化,并提出了体积变化的可能机制。结合生物组织的分层多孔弹性对结果进行了讨论。

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