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Sox9和Col2a1在经历软骨形成的细胞中的平行表达。

Parallel expression of Sox9 and Col2a1 in cells undergoing chondrogenesis.

作者信息

Zhao Q, Eberspaecher H, Lefebvre V, De Crombrugghe B

机构信息

Department of Molecular Genetics, The University of Texas, M.D. Anderson Cancer Center, Houston 77030, USA.

出版信息

Dev Dyn. 1997 Aug;209(4):377-86. doi: 10.1002/(SICI)1097-0177(199708)209:4<377::AID-AJA5>3.0.CO;2-F.

Abstract

To assess the role of the transcription factor Sox9 in cartilage formation we have compared the expression pattern of Sox9 and Col2a1 at various stages of mouse embryonic development. Expression of Col2a1 colocalized with expression of Sox9 in all chondroprogenitor cells. In the sclerotomal compartment of somites the onset of Sox9 expression preceded that of Col2a1. A perfect correlation was also seen between high levels of Sox9 expression and high levels of Col2a1 expression in chondrocytic cells. However, no Sox9 expression was detected in hypertrophic chondrocytes; only low levels of Col2a1 RNA were found in the upper hypertrophic zone. Coexpression of Sox9 and Col2a1 was also seen in the notochord. At E11.5 Sox9 expression in the brain and spinal neural tube was more widespread than that of Col2a1 although at E14.5 Sox9 and Col2a1 transcripts were colocalized in discrete areas of the brain. Distinct differences between Sox9 and Col2a1 expression were observed in the otic vesicle at E11.5. At E8.5, expression of Sox9 but not of Col2a1 was seen in the dorsal tips of the neural folds and after neural tube closure also in presumptive crest cells emigrating from the dorsal pole of the neural tube. No Col2a1 expression was detected in gonadal ridges in which high levels of Sox9 expression were detected. Together with our previous results showing that the chondrocyte-specific enhancer element of the Col2a1 gene is a direct target for Sox9, these results suggest that Sox9 plays a major role in expression of Col2a1. The correlation between high expression levels of Sox9 and high expression levels of Col2a1 in chondrocytes suggests the hypothesis that high levels of Sox9 are needed for full expression of the chondrocyte phenotype; lower levels of Sox9 such as in neuronal tissues which are also associated with lower expression levels of Col2a1 would be compatible with other cell specifications.

摘要

为了评估转录因子Sox9在软骨形成中的作用,我们比较了Sox9和Col2a1在小鼠胚胎发育各个阶段的表达模式。在所有软骨祖细胞中,Col2a1的表达与Sox9的表达共定位。在体节的硬骨节区域,Sox9表达的起始先于Col2a1。在软骨细胞中,Sox9高表达水平与Col2a1高表达水平之间也呈现出完美的相关性。然而,在肥大软骨细胞中未检测到Sox9表达;仅在肥大带上部发现低水平的Col2a1 RNA。在脊索中也观察到Sox9和Col2a1的共表达。在E11.5时,Sox9在脑和脊髓神经管中的表达比Col2a1更广泛,尽管在E14.5时,Sox9和Col2a1转录本在脑的离散区域中共定位。在E11.5时,在内耳泡中观察到Sox9和Col2a1表达的明显差异。在E8.5时,在神经褶的背侧尖端可见Sox9的表达,但未见Col2a1的表达,在神经管闭合后,从神经管背极迁出的假定嵴细胞中也可见Sox9的表达。在检测到高水平Sox9表达的性腺嵴中未检测到Col2a1表达。连同我们之前的结果表明Col2a1基因的软骨细胞特异性增强子元件是Sox9的直接靶点,这些结果表明Sox9在Col2a1的表达中起主要作用。软骨细胞中Sox9高表达水平与Col2a1高表达水平之间的相关性提示了这样一个假说,即高水平的Sox9是软骨细胞表型充分表达所必需的;较低水平的Sox9,如在神经元组织中,其也与较低水平的Col2a1表达相关,这与其他细胞特异性是相符的。

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