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Trabecular bone remodelling under pathological conditions based on biochemical and mechanical processes involved in BMU activity

机译:基于BMU活动涉及的生化和机械过程,在病理条件下进行小梁骨重塑

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摘要

In adulthood, bone tissue is continuously renewed by processes governed by basic multicellular units composed of osteocytes, osteoclasts and osteoblasts, which are subjected to local mechanical loads. Osteocytes are known to be integrated mechanosensors that regulate the activation of the osteoclasts and osteoblasts involved in bone resorption and apposition processes, respectively. After collagen tissue apposition, a process of collagen mineralisation takes place, gradually increasing the effective stiffness of bone. This study presents a new model based on physicochemical parameters involved in spongy bone remodelling under pathological conditions. Our model simulates the transient evolution of both geometry and effective Young's modulus of the trabeculae, also taking turnover into account. Various loads were applied on a trabecula in order to determine the evolution of bone volume fraction under pathological conditions. A parametric study performed on the model showed that one key parameter here is the kinetic constant of hydroxyapatite crystallisation. We subsequently tested our model on a pathological case approaching osteoporosis, involving a decrease in the number of viable osteocytes present in bone. The model converges to a lower value (-5%) for bone volume fraction than with a normal quantity of osteocytes. This useful tool offers new perspectives for predicting bone remodelling deficits on a local scale in patients with pathological conditions such as osteoporosis and in bedridden patients, as well as for astronauts subjected to weightlessness in space.
机译:在成年期,骨骼组织通过由多细胞基本单位控制的过程不断更新,这些基本多细胞单位由骨细胞,破骨细胞和成骨细胞组成,这些细胞承受局部机械负荷。已知成骨细胞是整合的机械传感器,其分别调节参与骨吸收和并置过程的破骨细胞和成骨细胞的活化。胶原组织并置后,发生胶原矿化过程,逐渐增加骨骼的有效刚度。这项研究提出了一种基于病理状态下海绵状骨重塑的理化参数的新模型。我们的模型模拟了小梁的几何形状和有效杨氏模量的瞬态演化,同时也考虑了周转率。为了确定在病理条件下骨体积分数的演变,对小梁施加了各种载荷。对模型进行的参数研究表明,此处的一个关键参数是羟基磷灰石结晶的动力学常数。随后,我们在接近骨质疏松症的病理病例中测试了我们的模型,该病例涉及骨中存在的存活骨细胞数量的减少。与正常量的骨细胞相比,该模型的骨体积分数收敛到较低的值(-5%)。这个有用的工具为在患有骨质疏松症等病态患者和卧床不起的患者以及太空失重的宇航员中预测局部规模的骨重塑缺陷提供了新的视角。

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    CNRS - UMR6233, Institut des Sciences du Mouvement, Universite de la Mediterranee, 163 Avenue de Luminy, Case 910,13 288 Marseille, France;

    CNRS - UMR6233, Institut des Sciences du Mouvement, Universite de la Mediterranee, 163 Avenue de Luminy, Case 910,13 288 Marseille, France;

    CNRS - UMR6233, Institut des Sciences du Mouvement, Universite de la Mediterranee, 163 Avenue de Luminy, Case 910,13 288 Marseille, France;

    CNRS - UMR6233, Institut des Sciences du Mouvement, Universite de la Mediterranee, 163 Avenue de Luminy, Case 910,13 288 Marseille, France;

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  • 正文语种 eng
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  • 关键词

    osteocytes; osteoclast; osteoblast; bone pathology; mineralisation;

    机译:骨细胞破骨细胞成骨细胞骨病理学矿化;

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