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A Methodology for Individual-Specific Modeling of Rat Optic Nerve Head Biomechanics in Glaucoma

机译:大鼠光神经头生物力学在青光眼中的个体特异性建模方法

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Glaucoma is the leading cause of irreversible blindness and involves the death of retinal ganglion cells (RGCs). Although biomechanics likely contributes to axonal injury within the optic nerve head (ONH), leading to RGC death, the pathways by which this occurs are not well understood. While rat models of glaucoma are well-suited for mechanistic studies, the anatomy of the rat ONH is different from the human, and the resulting differences in biomechanics have not been characterized. The aim of this study is to describe a methodology for building individual-specific finite element (FE) models of rat ONHs. This method was used to build three rat ONH FE models and compute the biomechanical environment within these ONHs. Initial results show that rat ONH strains are larger and more asymmetric than those seen in human ONH modeling studies. This method provides a framework for building additional models of normotensive and glaucomatous rat ONHs. Comparing model strain patterns with patterns of cellular response seen in studies using rat glaucoma models will help us to learn more about the link between biomechanics and glaucomatous cell death, which in turn may drive the development of novel therapies for glaucoma.
机译:青光眼是不可逆转的失明的主要原因,涉及视网膜神经节细胞(RGCS)的死亡。尽管生物力学可能有助于视神经头部(ONH)内的轴突损伤,但导致RGC死亡,这发生这种情况的途径并不熟知。虽然青光眼的大鼠模型非常适合机械研究,但大鼠ONH的解剖学与人不同,并且尚未表征生物力学的产生差异。本研究的目的是描述用于构建大鼠ONHS的个体特定有限元(FE)模型的方法。该方法用于构建三个RAT ONH FE模型,并在这些ONH中计算生物力学环境。初始结果表明,大鼠ONH菌株比在人类持续模拟研究中观察到的人更大且更不对称。该方法提供了建立额外的标准姿态和青光瘤鼠ONHS型号的框架。比较模型应变模式与使用大鼠青光眼模型的研究中所见的细胞反应模式将有助于我们了解有关生物力学和青光瘤细胞死亡之间的联系,这反过来可能推动新的青光眼疗法的发展。

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