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klotho 缺陷小鼠中骨基质蛋白分布改变和骨矿化缺陷。

Altered distribution of bone matrix proteins and defective bone mineralization in klotho-deficient mice.

机构信息

Department of Developmental Biology of Hard Tissue, Graduate School of Dental Medicine, Hokkaido University, Sapporo, Japan; Department of Gerodontology, Graduate School of Dental Medicine, Hokkaido University, Sapporo, Japan.

出版信息

Bone. 2013 Nov;57(1):206-19. doi: 10.1016/j.bone.2013.08.008. Epub 2013 Aug 14.

Abstract

In an attempt to identify the histological properties of the klotho-deficient (kl/kl) bone matrix, bone mineralization and the localization of Ca(2+)-binding bone matrix proteins - osteocalcin, dentin matrix protein-1 (DMP-1) and matrix Gla protein (MGP) - were examined in kl/kl tibiae. While a widespread osteocalcin staining could be verified in the wild-type bone matrix, localization of the same protein in the kl/kl tibiae seemed rather restricted to osteocytes with only a faint staining of the whole bone matrix. In wild-type mice, MGP immunoreactivity was present at the junction between the epiphyseal bone and cartilage, and at the insertion of the cruciate ligaments. In kl/kl mice, however, MGP was seen around the cartilaginous cores of the metaphyseal trabeculae and in the periphery of some cells of the bone surface. DMP-1 was identified in the osteocytic canalicular system of wild-type tibiae, but in the kl/kl tibiae this protein was mostly found in the osteocytic lacunae and in the periphery of some cells of the bone surface. Mineralization of the kl/kl bone seemed somewhat defective, with broad unmineralized areas within its matrix. In these areas, mineralized osteocytes along with their lacunae and osteocytic cytoplasmic processes were found to have intense osteocalcin and DMP-1 staining. Taken together, it might be that the excessive production of Ca(2+)-binding molecules such as osteocalcin and DMP-1 by osteocytes concentrates mineralization around such cells, disturbing the completeness of mineralization in the kl/kl bone matrix.

摘要

为了确定 klotho 缺陷(kl/kl)骨基质的组织学特性,我们检查了 kl/kl 胫骨中的骨矿化和 Ca(2+)结合骨基质蛋白 - 骨钙素、牙本质基质蛋白-1(DMP-1)和基质 Gla 蛋白(MGP)的定位。虽然在野生型骨基质中可以验证广泛的骨钙素染色,但在 kl/kl 胫骨中同种蛋白的定位似乎仅限于成骨细胞,整个骨基质的染色仅为微弱。在野生型小鼠中,MGP 免疫反应性存在于骺骨和软骨之间的交界处,以及十字韧带的插入处。然而,在 kl/kl 小鼠中,MGP 见于骺板骨小梁的软骨核心周围和骨表面一些细胞的周围。DMP-1 在野生型胫骨的成骨细胞管腔系统中被鉴定,但在 kl/kl 胫骨中,这种蛋白主要存在于成骨细胞陷窝中和骨表面一些细胞的周围。kl/kl 骨的矿化似乎有些缺陷,其基质中有广泛的未矿化区域。在这些区域中,矿化的成骨细胞及其陷窝和骨细胞质突起被发现具有强烈的骨钙素和 DMP-1 染色。总的来说,成骨细胞过度产生 Ca(2+)结合分子,如骨钙素和 DMP-1,可能会使这些细胞周围的矿化集中,干扰 kl/kl 骨基质中矿化的完整性。

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