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纯化的骨基质成分对破骨细胞前体的募集作用。

Recruitment of osteoclast precursors by purified bone matrix constituents.

作者信息

Malone J D, Teitelbaum S L, Griffin G L, Senior R M, Kahn A J

出版信息

J Cell Biol. 1982 Jan;92(1):227-30. doi: 10.1083/jcb.92.1.227.

Abstract

The osteoclast, the multinucleated giant cell of bone, is derived from circulating blood cells, most likely monocytes. Evidence has accrued that is consistent with the hypothesis that the recruitment of monocytes for osteoclast development occurs by chemotaxis. In the present study, we have examined the chemotactic response of human peripheral blood monocytes and related polymorphonuclear leucocytes to three constituents of bone matrix: peptides from Type I collagen, alpha 2-HS glycoprotein, and osteocalcin (bone gla protein). The latter two substances are among the major noncollagenous proteins of bone and are uniquely associated with calcified connective tissue. In chemotaxis assays using modified Boyden chambers, Type I collagen peptides, alpha 2HS glycoprotein, and osteocalcin evoke a dose-dependent chemotactic response in human monocytes. No chemotaxis is observed on PMNs despite their ontogenetic relationship to monocytes and their documented sensitivity to a broad range of other chemical substances. Our observations are consistent with the view that osteoclast precursors (monocytes) are mobilized by chemotaxis, and suggest that the chemoattractants responsible for this activity are derived from the bone matrix or, in the case of collagen and osteocalcin; directly from the osteoblasts which produce them.

摘要

破骨细胞,即骨的多核巨细胞,源自循环血细胞,极有可能是单核细胞。已有证据支持这样的假说,即单核细胞通过趋化作用被募集用于破骨细胞的发育。在本研究中,我们检测了人外周血单核细胞及相关多形核白细胞对骨基质的三种成分的趋化反应:I型胶原肽、α2-HS糖蛋白和骨钙素(骨γ-羧基谷氨酸蛋白)。后两种物质是骨的主要非胶原蛋白,且与钙化结缔组织独特相关。在使用改良Boyden小室的趋化实验中,I型胶原肽、α2-HS糖蛋白和骨钙素在人单核细胞中引发剂量依赖性趋化反应。尽管多形核白细胞与单核细胞有个体发生学关系且已证明它们对多种其他化学物质敏感,但未观察到它们有趋化现象。我们的观察结果与破骨细胞前体(单核细胞)通过趋化作用被动员的观点一致,并表明负责这种活性的趋化因子源自骨基质,或者就胶原和骨钙素而言,直接源自产生它们的成骨细胞。

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本文引用的文献

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Osteoclasts derived from haematopoietic stem cells.破骨细胞源自造血干细胞。
Nature. 1980 Feb 14;283(5748):669-70. doi: 10.1038/283669a0.
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