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通过附着于定向纤维诱导的持续细胞变形增强成纤维细胞迁移。

Continual cell deformation induced via attachment to oriented fibers enhances fibroblast cell migration.

作者信息

Qin Sisi, Ricotta Vincent, Simon Marcia, Clark Richard A F, Rafailovich Miriam H

机构信息

Materials Sciences and Engineering Department, Stony Brook University, Stony Brook, NY, United States of America.

Dental School, Stony Brook University, Stony Brook, NY, United States of America.

出版信息

PLoS One. 2015 Mar 16;10(3):e0119094. doi: 10.1371/journal.pone.0119094. eCollection 2015.

Abstract

Fibroblast migration is critical to the wound healing process. In vivo, migration occurs on fibrillar substrates, and previous observations have shown that a significant time lag exists before the onset of granulation tissue. We therefore conducted a series of experiments to understand the impact of both fibrillar morphology and migration time. Substrate topography was first shown to have a profound influence. Fibroblasts preferentially attach to fibrillar surfaces, and orient their cytoplasm for maximal contact with the fiber edge. In the case of en-mass cell migration out of an agarose droplet, fibroblasts on flat surfaces emerged with an enhanced velocity, v = 52μm/h, that decreases to the single cell value, v = 28μm/h within 24 hours and remained constant for at least four days. Fibroblasts emerging on fibrillar surfaces emerged with the single cell velocity, which remained constant for the first 24 hours and then increased reaching a plateau with more than twice the initial velocity within the next three days. The focal adhesions were distributed uniformly in cells on flat surfaces, while on the fibrillar surface they were clustered along the cell periphery. Furthermore, the number of focal adhesions for the cells on the flat surfaces remained constant, while it decreased on the fibrillar surface during the next three days. The deformation of the cell nuclei was found to be 50% larger on the fiber surfaces for the first 24 hours. While the mean deformation remained constant on the flat surface, it increased for the next three days by 24% in cells on fibers. On the fourth day, large actin/myosin fibers formed in cells on fibrillar surfaces only and coincided with a change from the standard migration mechanism involving extension of lamellipodia, and retraction of the rear, to one involving strong contractions oriented along the fibers and centered about the nucleus.

摘要

成纤维细胞迁移对伤口愈合过程至关重要。在体内,迁移发生在纤维状基质上,先前的观察表明,在肉芽组织形成之前存在显著的时间滞后。因此,我们进行了一系列实验,以了解纤维形态和迁移时间的影响。首先发现底物拓扑结构有深远影响。成纤维细胞优先附着于纤维状表面,并使其细胞质定向,以与纤维边缘实现最大程度的接触。在大量细胞从琼脂糖滴中迁移出来的情况下,平坦表面上的成纤维细胞以较高速度出现,v = 52μm/h,在24小时内降至单细胞速度,v = 28μm/h,并在至少四天内保持恒定。在纤维状表面出现的成纤维细胞以单细胞速度出现,在最初24小时内保持恒定,然后在接下来的三天内增加,达到比初始速度高出两倍多的平稳状态。粘着斑在平坦表面的细胞中均匀分布,而在纤维状表面上它们沿细胞周边聚集。此外,平坦表面上细胞的粘着斑数量保持恒定,而在纤维状表面上,其在接下来的三天内减少。发现细胞核在纤维表面上最初24小时的变形比在平坦表面上大50%。虽然平坦表面上的平均变形保持恒定,但在纤维上的细胞中,其在接下来的三天内增加了24%。在第四天,仅在纤维状表面的细胞中形成了大的肌动蛋白/肌球蛋白纤维,并且这与迁移机制从涉及片状伪足延伸和后部收缩的标准机制转变为涉及沿纤维并以细胞核为中心的强烈收缩的机制相吻合。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0d76/4361054/8c9a05c2134b/pone.0119094.g001.jpg

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