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一种通过基因组学方法来确定纳米形貌对间充质干细胞表型的影响。

A genomics approach in determining nanotopographical effects on MSC phenotype.

机构信息

Centre for Cell Engineering, Institute of Molecular, Cell and Systems Biology, College of Medical, Veterinary and Life Sciences, University of Glasgow, Glasgow G12 8QQ, Scotland, UK.

出版信息

Biomaterials. 2013 Mar;34(9):2177-84. doi: 10.1016/j.biomaterials.2012.12.019. Epub 2013 Jan 9.

Abstract

Topography and its effects on cell adhesion, morphology, growth and differentiation are well documented. Thus, current advances with the use of nanotopographies offer promising results in the field of regenerative medicine. Studies have also shown nanotopographies to have strong effects on stem cell self-renewal and differentiation. What is less clear however is what mechanotransductive mechanisms are employed by the cells to facilitate such changes. In fastidious cell types, it has been suggested that direct mechanotransduction producing morphological changes in the nucleus, nucleoskeleton and chromosomes themselves may be central to cell responses to topography. In this report we move these studies into human skeletal or mesenchymal stem cells and propose that direct (mechanical) signalling is important in the early stages of tuning stem cell fate to nanotopography. Using fluorescence in situ hybridization (FISH) and Affymetrix arrays we have evidence that nanotopography stimulates changes in nuclear organisation that can be linked to spatially regulated genes expression with a particular focus on phenotypical genes. For example, chromosome 1 was seen to display the largest numbers of gene deregulations and also a concomitant change in nuclear positioning in response to nanotopography. Plotting of deregulated genes in reference to band positioning showed that topographically related changes tend to happen towards the telomeric ends of the chromosomes, where bone related genes are generally clustered. Such an approach offers a better understanding of cell-surface interaction and, critically, provides new insights of how to control stem cell differentiation with future applications in areas including regenerative medicine.

摘要

地形及其对细胞黏附、形态、生长和分化的影响已有充分的记载。因此,目前利用纳米形貌的进展为再生医学领域带来了有希望的结果。研究还表明,纳米形貌对干细胞自我更新和分化有很强的影响。然而,目前尚不清楚细胞采用什么机械转导机制来促进这种变化。在精细的细胞类型中,有人提出,细胞核、核骨架和染色体本身的直接机械转导产生形态变化可能是细胞对地形反应的核心。在本报告中,我们将这些研究扩展到人类骨骼或间充质干细胞,并提出直接(机械)信号在调节干细胞命运对纳米形貌的早期阶段很重要。通过荧光原位杂交(FISH)和 Affymetrix 芯片,我们有证据表明纳米形貌刺激核组织发生变化,这种变化可以与空间调节基因表达相关联,特别关注表型基因。例如,发现染色体 1显示出最多的基因失调,并且在响应纳米形貌时核定位也发生了相应的变化。对参照带定位的失调基因进行绘图表明,与地形相关的变化往往发生在染色体的端粒末端,那里通常聚集着与骨骼相关的基因。这种方法可以更好地了解细胞表面的相互作用,并且关键是提供了如何控制干细胞分化的新见解,未来在再生医学等领域有应用前景。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1031/3573234/9d3af8df4cca/gr1.jpg

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