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人成骨细胞对表面固定微柱的小窝介导吞噬作用的尝试。

Attempted caveolae-mediated phagocytosis of surface-fixed micro-pillars by human osteoblasts.

机构信息

University Medical Center Rostock, Dept. of Cell Biology, Rostock, Germany.

University Medical Center Rostock, Dept. of Cell Biology, Rostock, Germany.

出版信息

Biomaterials. 2016 Jan;76:102-14. doi: 10.1016/j.biomaterials.2015.10.030. Epub 2015 Oct 23.

DOI:10.1016/j.biomaterials.2015.10.030
PMID:26519652
Abstract

Cells are sensitive to their underlying micro- and nano-topography, but the complex interplay is not completely understood especially if sharp edges and ridges of stochastically modified surfaces interfere with an attached cell body. Micro-topography offers cues that evoke a large range of cell responses e.g. altered adhesion behavior and integrin expression resulting in disturbed cell functions. In this study, we analyzed why osteoblastic cells mimic the underlying geometrical micro-pillar structure (5 × 5 × 5 μm, spacing of 5 μm) with their actin cytoskeleton. Interestingly, we discovered an attempted caveolae-mediated phagocytosis of each micro-pillar beneath the cells, which was accompanied by increased intracellular reactive oxygen species (ROS) production and reduced intracellular ATP levels. This energy consuming process hampered the cells in their function as osteoblasts at the interface. The raft-dependent/caveolae-mediated phagocytic pathway is regulated by diverse cellular components including caveolin-1 (Cav-1), cholesterol, actin cytoskeleton as well as actin-binding proteins like annexin A2 (AnxA2). Our results show a new aspect of osteoblast-material interaction and give insight into how cells behave on extraordinary micro-structures. We conclude that stochastically structured implants used in orthopedic surgery should avoid any topographical heights which induce phagocytosis to prevent their successful ingrowth.

摘要

细胞对其下伏的微观和纳米形貌非常敏感,但这种复杂的相互作用还不完全清楚,特别是如果随机修饰表面的锐利边缘和脊线干扰附着的细胞体。微观形貌提供了大量的细胞反应线索,例如改变的黏附行为和整合素表达,从而导致细胞功能紊乱。在这项研究中,我们分析了为什么成骨细胞会用它们的肌动蛋白细胞骨架模拟下面的几何微柱结构(5×5×5μm,间隔 5μm)。有趣的是,我们发现细胞下面的每个微柱都试图被小窝蛋白介导的吞噬作用所吞噬,这伴随着细胞内活性氧(ROS)产生的增加和细胞内 ATP 水平的降低。这个消耗能量的过程阻碍了细胞在界面处作为成骨细胞的功能。筏依赖/小窝蛋白介导的吞噬途径受多种细胞成分调节,包括小窝蛋白-1(Cav-1)、胆固醇、肌动蛋白细胞骨架以及肌动蛋白结合蛋白,如膜联蛋白 A2(AnxA2)。我们的研究结果展示了成骨细胞-材料相互作用的一个新方面,并深入了解了细胞在特殊微结构上的行为。我们得出结论,用于骨科手术的随机结构植入物应避免任何诱导吞噬作用的形貌高度,以防止其成功的生长。

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