大鼠、小鼠皮下植入骨颗粒巨细胞浸润的超微结构。

S N Popoff, S C Marks
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引用次数: 33

摘要

软组织巨细胞与矿化组织巨细胞(破骨细胞)具有明显不同的细胞表面受体和超微结构特征。最近,在皮下环境中去除死骨颗粒被描述为骨吸收的一个原型,一个主要的问题是这些异位骨植入物周围的巨细胞和骨表面破坏的过程是否与骨骼中的相同。我们比较了年轻正常大鼠和小鼠干骺端皮下植入具有类似破骨细胞特征的同种骨颗粒募集的巨细胞的细胞学和超微结构。植入后2、3、4周骨颗粒表面巨细胞为多核,胞质均匀,无空泡,光镜下骨表面界面不明显。在随机分布的少数细胞中,高倍镜下可见小的细胞质空泡,在骨表面附近可见大的空泡。在透射电镜下,与相邻细胞形成广泛交叉的折叠膜结构是大多数巨细胞表面的突出特征。在这些指间排列毗邻骨表面的情况下,可以注意到类似皱褶边界的结构,但在较低放大倍率或连续切片检查时,这些区域总是两个不同细胞的一部分。骨颗粒的分解似乎是通过小块的吞噬和随后在电子密集的细胞质液泡内的细胞内消化来实现的。这些幼龄动物的破骨细胞体积更小,细胞核更少,细胞质空泡集中在骨表面附近,具有特征性的褶皱边界和清晰区。这些结果证实了在死骨颗粒上的原生破骨细胞和多核巨细胞在超微结构和骨表面破坏机制上有明显不同。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Ultrastructure of the giant cell infiltrate of subcutaneously implanted bone particles in rats and mice.

The giant cells of soft tissues and those of mineralized tissues (osteoclasts) have distinctly different cell surface receptors and ultrastructural characteristics. Recently, the removal of dead bone particles in a subcutaneous environment has been described as a prototype of bone resorption, and a major issue is whether the giant cells that surround these ectopic bone implants and the processes involved in the disruption of bone surfaces are the same as those in the skeleton. We have compared the cytology and ultrastructure of giant cells recruited to subcutaneously implanted isogeneic bone particles with similar features of osteoclasts in metaphyseal bone of young normal rats and mice. Giant cells on surfaces of bone particles 2, 3, and 4 weeks after implantation were multinucleated, had a homogeneous, nonvacuolated cytoplasm, and had a bone surface interface unremarkable by light microscopy. In a few cells randomly distributed, small cytoplasmic vacuoles were present and large vacuoles were noted next to the bone surface at high magnification. By transmission electron microscopy, folded membrane configurations forming extensive interdigitations with adjacent cells were prominent features on most surfaces of giant cells. In instances where these interdigitations abutted bone surfaces, configuration resembling a ruffled border were noted, but these regions were always part of two different cells when examined at lower magnification or in serial sections. Breakdown of bone particles appeared to be by phagocytosis of small pieces and subsequent intracellular digestion in electron-dense cytoplasmic vacuoles. Osteoclasts from these same young animals were smaller with fewer nuclei, had cytoplasmic vacuoles concentrated next to bone surfaces, and had characteristic ruffled borders and clear zones. These results confirm those of others that native osteoclasts and multinucleated giant cells on dead bone particles are distinctly different with respect to both ultrastructure and mechanism of disruption of bone surfaces.

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