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对小鼠颅骨成骨细胞进行的全转录组分析突出了受模拟微重力调控的基因集,并确定了一种“机械反应性成骨细胞基因特征”。

Global transcriptome analysis in mouse calvarial osteoblasts highlights sets of genes regulated by modeled microgravity and identifies a "mechanoresponsive osteoblast gene signature".

作者信息

Capulli Mattia, Rufo Anna, Teti Anna, Rucci Nadia

机构信息

Department of Experimental Medicine, University of L'Aquila, Italy.

出版信息

J Cell Biochem. 2009 May 15;107(2):240-52. doi: 10.1002/jcb.22120.

Abstract

Mechanical unloading is known to be detrimental for the skeleton, but the underlying molecular mechanisms are not fully elucidated. We performed global transcriptome analysis of mouse calvarial osteoblasts grown for 5 days at unit gravity (1g) or under modeled microgravity (0.008g) in the NASA-developed rotating wall vessel (RWV) bioreactor. Elaboration of gene profiling data evidenced that, among the >20,000 gene probes evaluated, 45 genes were significantly up-regulated (cut-off >2) and 88 were down-regulated (cut-off <0.5) in modeled microgravity versus 1g. This set of regulated genes includes genes involved in osteoblast differentiation, function, and osteoblast-osteoclast cross-talk, as well as new genes not previously correlated with bone metabolism. Microarray data were validated for subsets of genes by real-time RT-PCR, Western blot, or functional analysis. The significantly modulated genes were then clustered using the GOTM (Gene Ontology Tree Machine) software. This analysis evidenced up-regulation of genes involved in the induction of apoptosis, in response to stress and in the activity of selected growth factors. Other molecular functions, such as extracellular matrix structural constituent, glycosaminoglycan/heparin-binding activity, and other growth factor activity, were instead down-regulated. We finally matched our transcriptome results with other public global gene profiles obtained in loading and unloading conditions, identifying 10 shared regulated genes which could represent an "osteoblast mechanoresponsive gene signature."

摘要

已知机械卸载对骨骼有害,但其潜在的分子机制尚未完全阐明。我们对在NASA研发的旋转壁式生物反应器中于单位重力(1g)或模拟微重力(0.008g)条件下培养5天的小鼠颅骨成骨细胞进行了全转录组分析。基因谱数据的详细分析表明,在评估的20000多个基因探针中,与1g相比,在模拟微重力条件下有45个基因显著上调(临界值>2),88个基因下调(临界值<0.5)。这组受调控的基因包括参与成骨细胞分化、功能以及成骨细胞-破骨细胞相互作用的基因,还有一些以前与骨代谢无关的新基因。通过实时RT-PCR、蛋白质印迹或功能分析对基因子集的微阵列数据进行了验证。然后使用GOTM(基因本体树机器)软件对显著调节的基因进行聚类。该分析表明,与应激反应和选定生长因子活性相关的凋亡诱导相关基因上调。相反,其他分子功能,如细胞外基质结构成分、糖胺聚糖/肝素结合活性和其他生长因子活性则下调。我们最终将我们的转录组结果与在加载和卸载条件下获得的其他公共全基因谱进行匹配,确定了10个共同调节的基因,它们可能代表一种“成骨细胞机械反应基因特征”。

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