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网格蛋白依赖的分化破骨细胞表面结合型 RANKL 的内吞作用。

Clathrin-dependent endocytosis of membrane-bound RANKL in differentiated osteoclasts.

机构信息

Clinical Department of Biomedicine, University of Trieste, Trieste, Italy.

出版信息

Eur J Histochem. 2010 Mar 8;54(1):e6. doi: 10.4081/ejh.2010.e6.

Abstract

Bone is continuously repaired and remodelled through well-coordinated activity of osteoblasts that form new bone and osteoclasts, which resorb it. Osteoblasts synthesize and secrete two key molecules that are important for osteoclast differentiation, namely the ligand for the receptor of activator of nuclear factor kappaB (RANKL) and its decoy receptor osteoprotegerin (OPG). Active membrane transport is a typical feature of the resorbing osteoclast during bone resorption. Normally, one resorption cycle takes several hours as observed by monitoring actin ring formation and consequent disappearance in vitro. During these cyclic changes, the cytoskeleton undergoes remarkable dynamic rearrangement. Active cells show a continuous process of exocytosis that plays an essential role in transport of membrane components, soluble molecules and receptor-mediated ligands thus allowing them to communicate with the environment. The processes that govern intracellular transport and trafficking in mature osteoclasts are poorly known. The principal methodological problem that have made these studies difficult is a physiological culture of osteoclasts that permit observing the vesicle apparatus in conditions similar to the in vivo conditions. In the present study we have used a number of morphological approaches to characterize the composition, formation and the endocytic and biosynthetic pathways that play roles in dynamics of differentiation of mature bone resorbing cells using a tri-dimensional system of physiologic coculture.

摘要

骨骼通过成骨细胞和破骨细胞的协调活动不断进行修复和重塑,成骨细胞形成新的骨骼,破骨细胞则吸收它。成骨细胞合成并分泌两种对破骨细胞分化很重要的关键分子,即核因子κB 受体激活物配体(RANKL)及其诱饵受体骨保护素(OPG)。主动膜转运是破骨细胞在骨吸收过程中的典型特征。在体外观察到,通常一个吸收周期需要几个小时,因为可以监测到肌动蛋白环的形成和随后的消失。在这些周期性变化中,细胞骨架经历了显著的动态重排。活跃的细胞表现出连续的胞吐过程,这在膜成分、可溶性分子和受体介导的配体的运输中起着至关重要的作用,从而使它们能够与环境进行通信。成熟破骨细胞中细胞内运输和运输的过程知之甚少。这些研究之所以困难,主要的方法学问题是破骨细胞的生理培养,这使得在类似于体内条件的情况下观察囊泡装置变得困难。在本研究中,我们使用了多种形态学方法来描述组成、形成以及内吞和生物合成途径,这些途径在成熟的骨吸收细胞的分化动力学中发挥作用,使用了一种三维生理性共培养系统。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/40cd/3167292/11be45247835/ejh-2010-1-e6-g001.jpg

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