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Genome-wide microarray analysis of MG-63 osteoblastic cells exposed to ultrasound

机译:暴露于超声的MG-63成骨细胞的全基因组微阵列分析

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It is well documented that low intensity pulsed ultrasound can be clinically used to accelerate bone fracture healing. Additionally, in vitro studies have shown that ultrasound can, for instance, increase mineralization, collagen production and alkaline phosphatase activity in osteoblasts. Despite the extensive research on the subject, the exact mechanism of ultrasound effect on bone cell gene regulation has not yet been deduced. In this study, we made an effort to reveal the features of genome-wide transcriptional response of osteoblast-type cells to ultrasound. MG-63 osteoblastic cell transcriptome was analyzed with whole genome microarray either 6 or 24 h after 30 min long exposure to 1.035 MHz pulsed ultrasound with three different acoustic pressures. Special attention was paid to the experimental design to minimize thermal effects and unwanted reflections of ultrasound. Microarray analysis suggested that ultrasound affects the genes involved with cellular membranes, and regulation of transcription as well. Several plasma membrane solute carriers were also regulated by ultrasound. It also changed the transcript level of several transcription factors belonging to the zinc finger proteins. However, ultrasound did not clearly promote genes involved with osteoblast differentiation.
机译:众所周知,低强度脉冲超声可以在临床上用于加速骨折愈合。另外,体外研究表明,超声可以例如增加成骨细胞的矿化,胶原蛋白的产生和碱性磷酸酶的活性。尽管对该主题进行了广泛的研究,但尚未推断出超声作用对骨细胞基因调控的确切机制。在这项研究中,我们努力揭示成骨细胞型细胞对超声的全基因组转录反应的特征。 MG-63成骨细胞转录组用全基因组微阵列分析了在三种不同声压下长时间暴露于1.035 MHz脉冲超声30分钟后6或24 h。特别注意实验设计,以最大程度地减少热效应和不必要的超声反射。微阵列分析表明,超声波会影响与细胞膜有关的基因,并影响转录调控。几种质膜溶质载体也通过超声调节。它还改变了属于锌指蛋白的几种转录因子的转录水平。然而,超声不能清楚地促进与成骨细胞分化有关的基因。

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