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机械重编程和再分化使成纤维细胞年轻化。

Fibroblast rejuvenation by mechanical reprogramming and redifferentiation.

机构信息

Mechanobiology Institute, National University of Singapore, 117411 Singapore.

Institute of Molecular Oncology, Italian Foundation for Cancer Research, 20139 Milan, Italy.

出版信息

Proc Natl Acad Sci U S A. 2020 May 12;117(19):10131-10141. doi: 10.1073/pnas.1911497117. Epub 2020 Apr 29.

Abstract

Over the course of the aging process, fibroblasts lose contractility, leading to reduced connective-tissue stiffness. A promising therapeutic avenue for functional rejuvenation of connective tissue is reprogrammed fibroblast replacement, although major hurdles still remain. Toward this, we recently demonstrated that the laterally confined growth of fibroblasts on micropatterned substrates induces stem-cell-like spheroids. In this study, we embedded these partially reprogrammed spheroids in collagen-I matrices of varying densities, mimicking different three-dimensional (3D) tissue constraints. In response to such matrix constraints, these spheroids regained their fibroblastic properties and sprouted to form 3D connective-tissue networks. Interestingly, we found that these differentiated fibroblasts exhibit reduced DNA damage, enhanced cytoskeletal gene expression, and actomyosin contractility. In addition, the rejuvenated fibroblasts show increased matrix protein (fibronectin and laminin) deposition and collagen remodeling compared to the parental fibroblast tissue network. Furthermore, we show that the partially reprogrammed cells have comparatively open chromatin compaction states and may be more poised to redifferentiate into contractile fibroblasts in 3D-collagen matrix. Collectively, our results highlight efficient fibroblast rejuvenation through laterally confined reprogramming, which has important implications in regenerative medicine.

摘要

在衰老过程中,成纤维细胞失去收缩性,导致结缔组织硬度降低。成纤维细胞重编程替换是一种有前途的功能性结缔组织再生治疗途径,但仍存在重大障碍。为此,我们最近证明,成纤维细胞在微图案化基底上的横向受限生长诱导出类似于干细胞的球体。在这项研究中,我们将这些部分重编程的球体嵌入到不同密度的胶原-I 基质中,模拟不同的三维 (3D) 组织约束。为了响应这种基质约束,这些球体恢复了它们的成纤维细胞特性,并发芽形成 3D 结缔组织网络。有趣的是,我们发现这些分化的成纤维细胞表现出减少的 DNA 损伤、增强的细胞骨架基因表达和肌动球蛋白收缩性。此外,与亲本成纤维细胞组织网络相比,再生活性化的成纤维细胞显示出增加的基质蛋白(纤连蛋白和层粘连蛋白)沉积和胶原重塑。此外,我们表明部分重编程的细胞具有相对开放的染色质压缩状态,并且可能更容易在 3D-胶原基质中重新分化为收缩性成纤维细胞。总之,我们的结果强调了通过横向受限重编程实现有效的成纤维细胞年轻化,这在再生医学中具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/52f9/7229653/9e307eab62af/pnas.1911497117fig01.jpg

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