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压力和变形调节人间充质干细胞基因表达。

Pressure and distortion regulate human mesenchymal stem cell gene expression.

作者信息

Haudenschild Anne K, Hsieh Adam H, Kapila Sunil, Lotz Jeffrey C

机构信息

UCSF/UCB Joint Graduate Group in Bioengineering, San Francisco, CA, USA.

出版信息

Ann Biomed Eng. 2009 Mar;37(3):492-502. doi: 10.1007/s10439-008-9629-2. Epub 2009 Jan 6.

Abstract

While the concept that physical forces such as tension and compression are involved in mature tissue modeling is widely accepted, the role of these specific types of mechanical loading in the differentiation and maturation of uncommitted cell types like human mesenchymal stem cells (hMSCs) is currently unknown. We observed that hMSCs have the fundamental ability to distinguish between dynamic tensile and compressive loading by regulating distinct gene expression patterns and that these differences in gene expression can be related to conformational changes in cell shape and volume. Dynamic tension was found to regulate both fibroblastic and osteogenic associated genes while dynamic compression up-regulated genes associated with chondrogenesis. Identifying genes involved in the mechanotransduction of different modes of physical loading in hMSC may greatly enhance the ability to rationally design tissue regeneration systems to restore proper tissue function.

摘要

虽然诸如张力和压缩力等物理力参与成熟组织建模的概念已被广泛接受,但这些特定类型的机械负荷在人骨髓间充质干细胞(hMSC)等未分化细胞类型的分化和成熟中的作用目前尚不清楚。我们观察到,hMSC具有通过调节不同的基因表达模式来区分动态拉伸和压缩负荷的基本能力,并且这些基因表达的差异可能与细胞形状和体积的构象变化有关。发现动态张力调节成纤维细胞和成骨相关基因,而动态压缩上调与软骨生成相关的基因。鉴定参与hMSC中不同物理负荷模式机械转导的基因,可能会大大提高合理设计组织再生系统以恢复适当组织功能的能力。

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