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首页> 外文期刊>Clinics in plastic surgery >Stiffening of human skin fibroblasts with age
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Stiffening of human skin fibroblasts with age

机译:随着年龄的增长人类皮肤成纤维细胞的增硬

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摘要

Changes in mechanical properties are an essential characteristic of the aging process of human skin. Previous studies attribute these changes predominantly to the altered collagen and elastin organization and density of the extracellular matrix. Here, we show that individual dermal fibroblasts also exhibit a significant increase in stiffness during aging in vivo. With the laser-based optical cell stretcher we examined the viscoelastic biomechanics of dermal fibroblasts isolated from 14 human donors aged 27 to 80. Increasing age was clearly accompanied by a stiffening of the investigated cells. We found that fibroblasts from old donors exhibited an increase in rigidity of ~60% with respect to cells of the youngest donors. A FACS analysis of the content of the cytoskeletal polymers shows a shift from monomeric G-actin to polymerized, filamentous F-actin, but no significant changes in the vimentin and microtubule content. The rheological analysis of fibroblast-populated collagen gels demonstrates that cell stiffening directly results in altered viscoelastic properties of the collagen matrix. These results identify a new mechanism that may contribute to the age-related impairment of elastic properties in human skin. The altered mechanical behavior might influence cell functions involving the cytoskeleton, such as contractility, motility, and proliferation, which are essential for reorganization of the extracellular matrix.
机译:机械性能的变化是人类皮肤老化过程的基本特征。先前的研究将这些变化主要归因于胶原蛋白和弹性蛋白组织的改变以及细胞外基质的密度。在这里,我们表明,单个的皮肤成纤维细胞还表现出体内衰老过程中刚度的显着增加。使用基于激光的光学细胞拉伸器,我们检查了从14位年龄在27至80岁之间的人类供体中分离出的皮肤成纤维细胞的粘弹性生物力学。随着年龄的增长,被研究的细胞明显变硬。我们发现,相对于最年轻供体的细胞,来自旧供体的成纤维细胞显示出约60%的刚性增加。 FACS分析细胞骨架聚合物的含量表明,从单体G-肌动蛋白转变为聚合的丝状F-肌动蛋白,但波形蛋白和微管含量没有明显变化。成纤维细胞填充胶原蛋白凝胶的流变学分析表明,细胞变硬直接导致胶原蛋白基质的粘弹性变。这些结果确定了一种新的机制,该机制可能导致与年龄有关的人类皮肤弹性特性受损。改变的机械行为可能会影响涉及细胞骨架的细胞功能,例如收缩性,运动性和增殖,这对于重组细胞外基质至关重要。

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