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骨骼中的初级钙化发生在核心蛋白聚糖去除以及胶原纤维融合之后。

The primary calcification in bones follows removal of decorin and fusion of collagen fibrils.

作者信息

Hoshi K, Kemmotsu S, Takeuchi Y, Amizuka N, Ozawa H

机构信息

First Department of Oral Anatomy, Niigata University School of Dentistry, Niigata, Japan.

出版信息

J Bone Miner Res. 1999 Feb;14(2):273-80. doi: 10.1359/jbmr.1999.14.2.273.

Abstract

To elucidate the mechanisms of primary calcification in bone, ultrastructural changes in collagen fibrils, as well as cytochemical alteration of proteoglycan, especially decorin, were investigated morphologically in 19-day postcoitum embryonic rat calvariae. Below the osteoblast layer, calcification of the osteoid area increased in direct proportion to its distance from the osteoblasts. In the uncalcified osteoid area, collagen fibrils near matrix vesicles possessed sharp contours and were a uniform 50 nm in diameter. Immunoelectron microscopy revealed decorin to be abundantly localized in the vicinity of the collagen fibrils. In the osteoid area undergoing the process of calcification, collagen fibrils tended to fuse side by side. Where calcification was progressed, this fusion was even more so. Some very large fibrils exhibited complicated contours, 400 nm or more in diameter. Although the calcification at this stage affected areas both inside and outside of the collagen fibrils, the interior areas manifested a lower density of calcification. The immunolocalization of decorin was also much decreased around these fibrils. Thus, primary calcification in bone matrix follows the removal of decorin and fusion of collagen fibrils. This phenomenon may aid in the process of calcification and bone formation, because (1) inhibitors of calcification, such as decorin, are removed, (2) the fusion of collagen fibrils provides the room necessary for rapid growth of mineral crystals, and (3) the soft elastic bone matrix containing abundant fused collagen fibrils less subjective to calcification is safe for both maternal and embryonic bodies and is convenient for subsequent bone remodeling.

摘要

为阐明骨原发性钙化的机制,对妊娠19天的胚胎大鼠颅骨进行了形态学研究,观察胶原纤维的超微结构变化以及蛋白聚糖尤其是核心蛋白聚糖的细胞化学改变。在成骨细胞层下方,类骨质区域的钙化与距成骨细胞的距离成正比增加。在未钙化的类骨质区域,靠近基质小泡的胶原纤维轮廓清晰,直径均匀为50nm。免疫电子显微镜显示核心蛋白聚糖大量定位于胶原纤维附近。在正在进行钙化过程的类骨质区域,胶原纤维倾向于并排融合。在钙化进展的部位,这种融合更为明显。一些非常大的纤维呈现出复杂的轮廓,直径达400nm或更大。尽管此阶段的钙化影响胶原纤维内外的区域,但内部区域的钙化密度较低。这些纤维周围核心蛋白聚糖的免疫定位也明显减少。因此,骨基质中的原发性钙化伴随着核心蛋白聚糖的去除和胶原纤维的融合。这种现象可能有助于钙化和骨形成过程,因为(1)钙化抑制剂如核心蛋白聚糖被去除,(2)胶原纤维的融合为矿物晶体的快速生长提供了必要的空间,(3)含有大量融合胶原纤维且较不易钙化的柔软弹性骨基质对母体和胚胎体都是安全的,并且便于随后的骨重塑。

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