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大鼠成骨细胞表型在体外的渐进性发育:在骨细胞外基质形成过程中,与成骨细胞增殖和分化相关基因表达的相互关系。

Progressive development of the rat osteoblast phenotype in vitro: reciprocal relationships in expression of genes associated with osteoblast proliferation and differentiation during formation of the bone extracellular matrix.

作者信息

Owen T A, Aronow M, Shalhoub V, Barone L M, Wilming L, Tassinari M S, Kennedy M B, Pockwinse S, Lian J B, Stein G S

机构信息

Department of Cell Biology, University of Massachusetts Medical Center, Worcester 01655.

出版信息

J Cell Physiol. 1990 Jun;143(3):420-30. doi: 10.1002/jcp.1041430304.

Abstract

The relationship of cell proliferation to the temporal expression of genes characterizing a developmental sequence associated with bone cell differentiation was examined in primary diploid cultures of fetal calvarial derived osteoblasts by the combined use of autoradiography, histochemistry, biochemistry, and mRNA assays of osteoblast cell growth and phenotypic genes. Modifications in gene expression define a developmental sequence that has 1) three principle periods--proliferation, extracellular matrix maturation, and mineralization--and 2) two restriction points to which the cells can progress but cannot pass without further signals--the first when proliferation is down-regulated and gene expression associated with extracellular matrix maturation is induced, and the second when mineralization occurs. Initially, actively proliferating cells, expressing cell cycle- and cell growth-regulated genes, produce a fibronectin/type I collagen extracellular matrix. A reciprocal and functionally coupled relationship between the decline in proliferative activity and the subsequent induction of genes associated with matrix maturation and mineralization is supported by 1) a temporal sequence of events in which there is an enhanced expression of alkaline phosphatase immediately following the proliferative period, and later, an increased expression of osteocalcin and osteopontin at the onset of mineralization; 2) increased expression of a specific subset of osteoblast phenotype markers, alkaline phosphatase and osteopontin, when proliferation is inhibited by hydroxyurea; and 3) enhanced levels of expression of the osteoblast markers as a function of ascorbic acid-induced collagen deposition, suggesting that the extracellular matrix contributes to both the shutdown of proliferation and the development of the osteoblast phenotype.

摘要

通过联合运用放射自显影术、组织化学、生物化学以及成骨细胞生长和表型基因的mRNA检测方法,在源自胎儿颅骨的原代二倍体成骨细胞培养物中,研究了细胞增殖与表征骨细胞分化相关发育序列的基因的时间表达之间的关系。基因表达的改变定义了一个发育序列,该序列具有:1)三个主要时期——增殖期、细胞外基质成熟期和矿化期;2)两个限制点,细胞可以进展到这两个点,但若无进一步信号则无法通过——第一个限制点是增殖下调且与细胞外基质成熟相关的基因表达被诱导时,第二个限制点是矿化发生时。最初,活跃增殖的细胞表达细胞周期和细胞生长调节基因,产生纤连蛋白/Ⅰ型胶原细胞外基质。增殖活性下降与随后诱导的与基质成熟和矿化相关的基因之间存在相互的且功能耦合的关系,这一关系得到以下几点支持:1)一系列按时间顺序发生的事件,即增殖期之后立即碱性磷酸酶表达增强,随后在矿化开始时骨钙素和骨桥蛋白表达增加;2)当用羟基脲抑制增殖时,成骨细胞表型标志物(碱性磷酸酶和骨桥蛋白)的特定子集表达增加;3)成骨细胞标志物的表达水平随着抗坏血酸诱导的胶原沉积而增强,这表明细胞外基质既有助于增殖的停止,也有助于成骨细胞表型的发育。

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