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AG1(Dmp1)基因的原位定位与染色体图谱分析

In situ localization and chromosomal mapping of the AG1 (Dmp1) gene.

作者信息

George A, Gui J, Jenkins N A, Gilbert D J, Copeland N G, Veis A

机构信息

Division of Oral Biology, Northwestern University, Chicago, Illinois.

出版信息

J Histochem Cytochem. 1994 Dec;42(12):1527-31. doi: 10.1177/42.12.7983353.

Abstract

Dentinogenesis is being used as a model for understanding the biomineralization process. The odontoblasts synthesize a structural matrix comprised of Type I collagen fibrils which define the basic architecture of the tissue. The odontoblasts also synthesize and deliver a number of dentin-specific acidic macromolecules into the extracellular compartment. These acidic macromolecules may be involved in regulating the ordered deposition of hydroxyapatite crystals within the matrix. AG1 is the first tooth-specific acidic macromolecule to have been cloned and sequenced. To identify which cells of the rat incisor pulp/odontoblast complex were responsible for synthesis of AG1, in situ hybridization was used. Digoxigenin labeled sense and anti-sense AG1 riboprobes were prepared. The AG1 mRNA was found to be expressed in the mature secretory odontoblasts. Neither pulp cells nor pre-odontoblasts showed any staining with the anti-sense probes. Chromosomal localization studies placed the AG1 gene on mouse chromosome 5q21, in tight linkage with Fgf5. AG1 has been renamed Dmp1 (dentin matrix protein 1) in accordance with present chromosomal nomenclature. Mouse 5q21 corresponds to the 4q21 locus in humans. This is the locus for the human tooth mineralization disorder dentinogenesis imperfecta Type II (DI-II). These data suggest that the Dmp1 gene is involved in mineralization and is a candidate gene for DI-II.

摘要

牙本质生成正被用作理解生物矿化过程的模型。成牙本质细胞合成一种由I型胶原纤维组成的结构基质,该基质定义了组织的基本结构。成牙本质细胞还合成并将多种牙本质特异性酸性大分子输送到细胞外区室。这些酸性大分子可能参与调节基质中羟基磷灰石晶体的有序沉积。AG1是第一个被克隆和测序的牙齿特异性酸性大分子。为了确定大鼠切牙髓/成牙本质细胞复合体中哪些细胞负责AG1的合成,采用了原位杂交技术。制备了地高辛标记的正义和反义AG1核糖探针。发现AG1 mRNA在成熟的分泌性成牙本质细胞中表达。牙髓细胞和前成牙本质细胞用反义探针均未显示任何染色。染色体定位研究将AG1基因定位在小鼠5号染色体的5q21上,与Fgf5紧密连锁。根据目前的染色体命名法,AG1已被重新命名为Dmp1(牙本质基质蛋白1)。小鼠5q21对应于人类的4q21位点。这是人类牙齿矿化障碍II型牙本质发育不全(DI-II)的位点。这些数据表明Dmp1基因参与矿化,是DI-II的候选基因。

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