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迈向对SOX9在软骨细胞分化中功能的理解。

Toward understanding SOX9 function in chondrocyte differentiation.

作者信息

Lefebvre V, de Crombrugghe B

机构信息

Department of Molecular Genetics, The University of Texas M.D. Anderson Cancer Center, Houston, USA.

出版信息

Matrix Biol. 1998 Mar;16(9):529-40. doi: 10.1016/s0945-053x(98)90065-8.

Abstract

The transcription factors that trigger the determinative switch to chondrocyte differentiation in mesenchymal cells are still unknown. In humans, mutations in the gene for SOX9, a transcription factor with a DNA-binding domain similar to that of the mammalian testis-determining factor SRY, cause campomelic dysplasia, a severe dwarfism syndrome which affects all cartilage-derived structures. During mouse embryonic development, the Sox9 gene becomes active in all prechondrocytic mesenchymal condensations, and at later stages its expression is maintained at high levels in fully differentiated chondrocytes. A chondrocyte-specific enhancer in the gene for collagen type II (Col2a1), a characteristic marker of chondrocytes, is a direct target for SOX9, and ectopic expression of SOX9 in transgenic mouse embryos is sufficient to activate the endogenous Col2a1 gene in some tissues. These data suggest that SOX9 could have a major role in chondrogenesis. Studies are in progress to identify other target genes for SOX9 in chondrocytes and also other transcription factors that are believed to cooperate with SOX9 in the activation of chondrocyte-specific genes. Defining SOX9 function and the mechanisms that regulate SOX9 gene expression should contribute to a better understanding of chondrocyte differentiation.

摘要

触发间充质细胞向软骨细胞分化的决定性转变的转录因子仍然未知。在人类中,SOX9基因发生突变会导致弯肢侏儒症,这是一种严重的侏儒症综合征,会影响所有软骨衍生结构。SOX9是一种转录因子,其DNA结合结构域与哺乳动物睾丸决定因子SRY相似。在小鼠胚胎发育过程中,Sox9基因在所有软骨前间充质凝聚物中变得活跃,在后期阶段,其表达在完全分化的软骨细胞中维持在高水平。II型胶原蛋白(Col2a1)基因中的软骨细胞特异性增强子是软骨细胞的特征性标志物,是SOX9的直接靶点,在转基因小鼠胚胎中SOX9的异位表达足以在某些组织中激活内源性Col2a1基因。这些数据表明SOX9可能在软骨形成中起主要作用。目前正在进行研究以鉴定软骨细胞中SOX9的其他靶基因,以及其他据信与SOX9协同激活软骨细胞特异性基因的转录因子。明确SOX9的功能以及调节SOX9基因表达的机制,应有助于更好地理解软骨细胞分化。

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