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Governing Equations of Tissue Modelling and Remodelling: A Unified Generalised Description of Surface and Bulk Balance

机译:组织建模和重塑的控制方程式:表面和体积平衡的统一广义描述

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摘要

Several biological tissues undergo changes in their geometry and in their bulk material properties by modelling and remodelling processes. Modelling synthesises tissue in some regions and removes tissue in others. Remodelling overwrites old tissue material properties with newly formed, immature tissue properties. As a result, tissues are made up of different “patches”, i.e., adjacent tissue regions of different ages and different material properties, within evolving boundaries. In this paper, generalised equations governing the spatio-temporal evolution of such tissues are developed within the continuum model. These equations take into account nonconservative, discontinuous surface mass balance due to creation and destruction of material at moving interfaces, and bulk balance due to tissue maturation. These equations make it possible to model patchy tissue states and their evolution without explicitly maintaining a record of when/where resorption and formation processes occurred. The time evolution of spatially averaged tissue properties is derived systematically by integration. These spatially-averaged equations cannot be written in closed form as they retain traces that tissue destruction is localised at tissue boundaries. The formalism developed in this paper is applied to bone tissues, which exhibit strong material heterogeneities due to their slow mineralisation and remodelling processes. Evolution equations are proposed in particular for osteocyte density and bone mineral density. Effective average equations for bone mineral density (BMD) and tissue mineral density (TMD) are derived using a mean-field approximation. The error made by this approximation when remodelling patchy tissue is investigated. The specific signatures of the time evolution of BMD or TMD during remodelling events are exhibited. These signatures may provide a way to detect remodelling events at lower, unseen spatial resolutions from microCT scans.
机译:通过建模和重塑过程,几种生物组织的几何形状和整体材料特性都会发生变化。建模可以合成某些区域的组织,而去除其他区域的组织。重塑会用新形成的未成熟组织特性覆盖旧的组织材料特性。结果,组织由不同的“斑块”组成,即在不断发展的边界内具有不同年龄和不同材料特性的相邻组织区域。在本文中,在连续模型中建立了控制此类组织的时空演化的广义方程。这些方程式考虑了非保守的,由于移动界面处材料的产生和破坏而造成的不连续表面质量平衡,以及由于组织成熟而引起的体积平衡。这些方程式可以对斑块状的组织状态及其演化进行建模,而无需明确维护何时发生吸收和形成过程的记录。空间平均组织特性的时间演变是通过积分系统得出的。这些空间平均方程无法以封闭形式编写,因为它们保留了组织破坏位于组织边界的痕迹。本文开发的形式主义适用于骨骼组织,这些骨骼组织由于其缓慢的矿化和重塑过程而显示出强烈的材料异质性。特别针对骨细胞密度和骨矿物质密度提出了演化方程。使用平均场近似法可以得出有效的骨矿物质密度(BMD)和组织矿物质密度(TMD)平均方程。研究了重塑斑片组织时这种近似所产生的误差。展示了重塑事件期间BMD或TMD时间演变的特定特征。这些签名可以提供一种从microCT扫描以较低的,看不见的空间分辨率检测重塑事件的方法。

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    Pascal R. Buenzli;

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  • 年(卷),期 -1(11),4
  • 年度 -1
  • 页码 e0152582
  • 总页数 25
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