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An investigation in the cellular mechanisms of bone remodeling using a hybrid cellular automaton approach.

机译:使用混合细胞自动机方法进行骨重塑的细胞机制研究。

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摘要

One of the most intriguing aspects of bone is its ability to grow, repair damage, adapt to mechanical loads, and maintain mineral homeostasis. It is generally accepted that bone adaptation occurs in response to the mechanical demands of our daily activities; moreover, strain and microdamage have been implicated as potential stimuli that regulate this sophisticated process. While researchers have made significant advances in our understanding of the bone adaptation process, there are many aspects that remain unknown. For instance, it is not fully understood how the mechanical stimulation experienced by bones influences the biochemical signaling that drives the cellular activity of remodeling. Due to the fact that evidence for bone metabolic diseases points toward the disruption of the cellular mechanisms of remodeling, such a relationship is crucial to understanding the key factors that result in pathological remodeling activity.;Over the past several decades, various theoretical and computational models have been developed to study the bone adaptation process. These computational models have primarily focused on predicting net changes in organ and tissue level bone architecture. While these simulations are able to capture phenomena such as net increases or decreases in bone volume or reorientation of tissue level structures, they do not capture cellular level details. In an attempt to ameliorate this deficiency of previous models, more recent studies have focused on simulating the remodeling response at a single site in bone. However, few models attempt to combine models of cellular activity with the classical phenomenological remodeling paradigms.;The primary focus of this dissertation is to present a new computational framework that mechanistically models the cellular behavior involved in the bone remodeling process. This framework uniquely combines established phenomenological remodeling paradigms with cellular mechanisms to predict remodeling activity for a damaged site in bone. Biological rules were implemented to control the recruitment, differentiation, and activation of osteoclasts and osteoblasts, based on observations from histological studies. The results of this work are the first of their kind to demonstrate spatially and temporally accurate remodeling behavior at the cellular level. Furthermore, these results provide unique insights regarding key parameters that influence cellular level remodeling activity.
机译:骨骼最引人入胜的方面之一是其生长,修复损伤,适应机械负荷和维持矿物质稳态的能力。人们普遍认为,骨骼适应是根据我们日常活动的机械需求而发生的。此外,应变和微损伤被认为是调节这种复杂过程的潜在刺激。尽管研究人员在我们对骨骼适应过程的理解上取得了长足的进步,但仍有许多方面仍然未知。例如,还没有完全理解骨骼受到的机械刺激如何影响驱动细胞重塑的生物化学信号传导。由于骨代谢疾病的证据指向细胞重塑机制的破坏,因此这种关系对于理解导致病理重塑活动的关键因素至关重要。;在过去的几十年中,各种理论和计算模型已经研究骨适应过程。这些计算模型主要集中在预测器官和组织水平骨结构的净变化。虽然这些模拟能够捕获诸如骨骼体积净增加或减少或组织水平结构重新定向之类的现象,但它们无法捕获细胞水平细节。为了减轻以前模型的这种缺陷,最近的研究集中在模拟骨骼中单个部位的重塑反应。然而,很少有模型试图将细胞活动模型与经典的现象学重塑范例相结合。本论文的主要重点是提出一种新的计算框架,以机械方式模拟参与骨骼重塑过程的细胞行为。该框架将建立起来的现象学重塑范例与细胞机制独特地结合在一起,以预测骨骼受损部位的重塑活动。根据组织学研究的结果,实施了生物学规则来控制破骨细胞和成骨细胞的募集,分化和激活。这项工作的结果是首次证明在细胞水平上时空上正确的重塑行为。此外,这些结果提供了有关影响细胞水平重塑活性的关键参数的独特见解。

著录项

  • 作者

    Penninger, Charles L.;

  • 作者单位

    University of Notre Dame.;

  • 授予单位 University of Notre Dame.;
  • 学科 Engineering Biomedical.;Biophysics Biomechanics.;Engineering Mechanical.
  • 学位 Ph.D.
  • 年度 2011
  • 页码 226 p.
  • 总页数 226
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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