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一种用于研究负重骨中转运过程和流体流动的体外模型。

An ex vivo model to study transport processes and fluid flow in loaded bone.

作者信息

Knothe Tate M L, Knothe U

机构信息

Institute of Biomedical Engineering and Medical Informatics, University and Swiss Federal Institute of Technology, Zurich.

出版信息

J Biomech. 2000 Feb;33(2):247-54. doi: 10.1016/s0021-9290(99)00143-8.

Abstract

Load-induced fluid flow has been postulated to provide a mechanism for the transmission of mechanical signals (e.g. via shear stresses, enhancement of molecular transport, and/or electrical effects) and the subsequent elicitation of a functional adaptation response (e.g. modeling, remodeling, homeostasis) in bone. Although indirect evidence for such fluid flow phenomena can be found in the literature pertaining to strain generated potentials, actual measurement of fluid displacements in cortical bone is inherently difficult. This problem motivated us to develop and introduce an ex vivo perfusion model for the study of transport processes and fluid flow within bone under controlled mechanical loading conditions. To this end, a closed-loop system of perfusion was established in the explanted forelimb of the adult Swiss alpine sheep. Immediately prior to mechanical loading, a bolus of tracer was introduced intraarterially into the system. Thereafter, the forelimb of the left or right side (randomized) was loaded cyclically, via Schanz screws inserted through the metaphyses, producing a peak compressive strain of 0.2% at the middiaphysis of the anterior metacarpal cortex. In paired experiments with perfusion times totalling 2, 4, 8 and 16 min, the concentration of tracer measured at the middiaphysis of the cortex in cross section was significantly higher in the loaded bone than in the unloaded contralateral control. Fluorometric measurements of procion red concentration in the anterior aspect alone showed an enhancement in transport at early stages of loading (8 cycles, 2 min) but no effect in transport after higher number of cycles or increased perfusion times, respectively. This reflects both the small size of the molecular tracer, which would be expected to be transported rapidly by way of diffusive mechanisms alone, as well as the loading mode to which the anterior aspect was exposed. Thus, using our new model it could be shown that load-induced fluid flow represents a powerful mechanism to enhance molecular transport within the lacunocanalicular system of compact bone tissue. Based on these as well as previous studies, it appears that the degree of this effect is dependent on tracer size as well as the mechanical loading mode to which a given area of tissue is exposed.

摘要

负荷诱导的流体流动被认为是一种传递机械信号(例如通过剪切应力、分子运输增强和/或电效应)以及随后引发骨骼功能适应性反应(例如塑形、重塑、内环境稳定)的机制。尽管在与应变产生电位相关的文献中可以找到这种流体流动现象的间接证据,但在皮质骨中实际测量流体位移本身就很困难。这个问题促使我们开发并引入一种体外灌注模型,用于研究在受控机械负荷条件下骨内的运输过程和流体流动。为此,在成年瑞士高山羊的离体前肢中建立了一个闭环灌注系统。在机械负荷之前,将一剂示踪剂经动脉注入系统。此后,通过插入干骺端的斯氏针,对左侧或右侧(随机)前肢进行周期性加载,在前掌骨皮质中部产生0.2%的峰值压缩应变。在灌注时间总计为2、4、8和16分钟的配对实验中,在加载骨的皮质中部横截面处测得的示踪剂浓度明显高于未加载的对侧对照。仅在前侧进行的荧光素测量显示,在加载早期(8个循环,2分钟)运输增强,但在更多循环数或增加灌注时间后对运输没有影响。这既反映了分子示踪剂的小尺寸,预计其仅通过扩散机制就能快速运输,也反映了前侧所承受的加载模式。因此,使用我们的新模型可以表明,负荷诱导的流体流动是增强致密骨组织腔隙小管系统内分子运输的有力机制。基于这些以及先前的研究,这种效应的程度似乎取决于示踪剂大小以及给定组织区域所承受的机械加载模式。

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