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皮肤硬度控制着年轻和老年人类皮肤的表皮和基底膜的形貌。

Dermal stiffness governs the topography of the epidermis and the underlying basement membrane in young and old human skin.

机构信息

Laboratoire de Biologie Tissulaire et Ingénierie Thérapeutique, CNRS UMR 5305, Université de Lyon, Lyon, France.

Native Laboratoire, Bezons, France.

出版信息

Aging Cell. 2024 Apr;23(4):e14096. doi: 10.1111/acel.14096. Epub 2024 Mar 12.

Abstract

The epidermis is a stratified epithelium that forms the outer layer of the skin. It is composed primarily of keratinocytes and is constantly renewed by the proliferation of stem cells and their progeny that undergo terminal differentiation as they leave the basal layer and migrate to the skin surface. Basal keratinocytes rest on a basement membrane composed of an extracellular matrix that controls their fate via integrin-mediated focal adhesions and hemidesmosomes which are critical elements of the epidermal barrier and promote its regenerative capabilities. The distribution of basal cells with optimal activity provides the basement membrane with its characteristic undulating shape; this configuration disappears with age, leading to epidermal weakness. In this study, we present an in-depth imaging analysis of basal keratinocyte anchorage in samples of human skin from participants across the age spectrum. Our findings reveal that skin aging is associated with the depletion of hemidesmosomes that provide crucial support for stem cell maintenance; their depletion correlates with the loss of the characteristic basement membrane structure. Atomic force microscopy studies of skin and in vitro experiments revealed that the increase in tissue stiffness observed with aging triggers mechanical signals that alter the basement membrane structure and reduce the extent of basal keratinocyte anchorage, forcing them to differentiate. Genomic analysis revealed that epidermal aging was associated with mechanical induction of the transcription factor Krüppel-like factor 4. The altered mechanical properties of tissue being a new hallmark of aging, our work opens new avenues for the development of skin rejuvenation strategies.

摘要

表皮是一种分层上皮组织,形成皮肤的外层。它主要由角质形成细胞组成,通过干细胞的增殖及其后代的终末分化不断更新,这些细胞离开基底层并迁移到皮肤表面。基底层角质形成细胞位于由细胞外基质组成的基底膜上,通过整合素介导的黏附斑和半桥粒控制其命运,这些结构是表皮屏障的关键组成部分,促进其再生能力。具有最佳活性的基底细胞的分布为基底膜提供了其特征性的波浪形形状;这种结构随着年龄的增长而消失,导致表皮脆弱。在这项研究中,我们对来自不同年龄段参与者的皮肤样本中的基底角质形成细胞锚定进行了深入的成像分析。我们的发现表明,皮肤衰老与提供干细胞维持所需的关键支持的半桥粒耗竭有关;它们的耗竭与特征性基底膜结构的丧失相关。皮肤的原子力显微镜研究和体外实验表明,随着年龄的增长,组织硬度的增加会引发机械信号,改变基底膜结构并减少基底角质形成细胞的锚定程度,迫使它们分化。基因组分析表明,表皮衰老与转录因子 Krüppel 样因子 4 的机械诱导有关。组织的机械特性改变是衰老的一个新标志,我们的工作为皮肤年轻化策略的发展开辟了新途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/23ab/11019137/f9d6c477c7bb/ACEL-23-e14096-g002.jpg

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