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骨折愈合过程中合成的胶原蛋白。

Collagens synthesized by healing fractures.

作者信息

Ashhurst D E

机构信息

Department of Anatomy, St. George's Hospital Medical School, Tooting, London, England.

出版信息

Clin Orthop Relat Res. 1990 Jun(255):273-83.

PMID:2189630
Abstract

Several extracellular matrices are formed by healing fractures, and the collagens within these matrices have been identified in rabbit and rat fracture models. Type III collagen is the major collagen of the fibrous matrix that forms along the periosteal surface. Type I collagen is secreted in large amounts as trabeculae of bone develop within the fibrous tissue. Type V collagen is found in both the fibrous tissue and bone; it is particularly associated with blood vessels. Type II collagen is the last of the major collagens to be synthesized; its synthesis is dependent on the mechanical conditions under which the fractures are healing. A large area of cartilage, and hence of Type II collagen, is formed only if the fracture is mechanically unstable. Of the minor collagens, only Types IX and X have been identified to date. Type IX collagen is present throughout the large areas of cartilage, and Type X is present only in calcified regions. The matrices are compared with those produced during embryonic limb development. Although cartilage in the embryo provides a rapidly growing model of the future bone, in healing fractures cartilage is produced only where the cellular environment precludes the differentiation of osteoblasts. The effects of mechanical stability on the matrices support and illustrate this conclusion.

摘要

愈合的骨折会形成几种细胞外基质,并且在兔和大鼠骨折模型中已鉴定出这些基质中的胶原蛋白。III型胶原蛋白是沿骨膜表面形成的纤维基质的主要胶原蛋白。随着纤维组织内骨小梁的发育,大量分泌I型胶原蛋白。V型胶原蛋白存在于纤维组织和骨骼中;它尤其与血管有关。II型胶原蛋白是最后合成的主要胶原蛋白;其合成取决于骨折愈合时的力学条件。只有当骨折力学不稳定时,才会形成大面积的软骨,进而形成II型胶原蛋白。在次要胶原蛋白中,迄今为止仅鉴定出IX型和X型。IX型胶原蛋白存在于大面积的软骨中,而X型仅存在于钙化区域。将这些基质与胚胎肢体发育过程中产生的基质进行比较。尽管胚胎中的软骨为未来的骨骼提供了快速生长的模型,但在愈合的骨折中,只有在细胞环境阻止成骨细胞分化的地方才会产生软骨。力学稳定性对基质的影响支持并说明了这一结论。

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