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Key Regulatory Role of Dermal Fibroblasts in Pigmentation as Demonstrated Using a Reconstructed Skin Model: Impact of Photo-Aging

机译:使用重建的皮肤模型证明真皮成纤维细胞在色素沉着中的关键调控作用:光老化的影响

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摘要

To study cutaneous pigmentation in a physiological context, we have previously developed a functional pigmented reconstructed skin model composed of a melanocyte-containing epidermis grown on a dermal equivalent comprising living fibroblasts. The present studies, using the same model, aimed to demonstrate that dermal fibroblasts influence skin pigmentation up to the macroscopic level. The proof of principle was performed with pigmented skins differing only in the fibroblast component. First, the in vitro system was reconstructed with or without fibroblasts in order to test the global influence of the presence of this cell type. We then assessed the impact of the origin of the fibroblast strain on the degree of pigmentation using fetal versus adult fibroblasts. In both experiments, impressive variation in skin pigmentation at the macroscopic level was observed and confirmed by quantitative parameters related to skin color, melanin content and melanocyte numbers. These data confirmed the responsiveness of the model and demonstrated that dermal fibroblasts do indeed impact the degree of skin pigmentation. We then hypothesized that a physiological state associated with pigmentary alterations such as photo-aging could be linked to dermal fibroblasts modifications that accumulate over time. Pigmentation of skin reconstructed using young unexposed fibroblasts (n = 3) was compared to that of tissues containing natural photo-aged fibroblasts (n = 3) which express a senescent phenotype. A stimulation of pigmentation in the presence of the natural photo-aged fibroblasts was revealed by a significant increase in the skin color (decrease in Luminance) and an increase in both epidermal melanin content and melanogenic gene expression, thus confirming our hypothesis. Altogether, these data demonstrate that the level of pigmentation of the skin model is influenced by dermal fibroblasts and that natural photo-aged fibroblasts can contribute to the hyperpigmentation that is associated with photo-aging.
机译:为了在生理环境中研究皮肤色素沉着,我们先前已经开发了一种功能性色素重建皮肤模型,该模型由生长在包含活体成纤维细胞的真皮等同物上的含黑素细胞的表皮组成。本研究使用相同的模型,旨在证明真皮成纤维细胞在宏观水平上影响皮肤色素沉着。用只有在成纤维细胞成分不同的有色皮肤进行原理验证。首先,在有或没有成纤维细胞的情况下重建体外系统,以测试这种细胞类型的存在的整体影响。然后,我们使用胎儿与成人成纤维细胞评估了成纤维细胞株起源对色素沉着程度的影响。在这两个实验中,在宏观水平上观察到皮肤色素沉着的显着变化,并通过与皮肤颜色,黑色素含量和黑色素细胞数量有关的定量参数得到证实。这些数据证实了该模型的响应性,并证明真皮成纤维细胞确实确实影响皮肤色素沉着的程度。然后,我们假设与色素改变(例如光老化)相关的生理状态可能与随着时间累积的皮肤成纤维细胞修饰有关。将使用未暴露的年轻成纤维细胞(n = 3)重建的皮肤的色素沉着与含有自然光衰老成纤维细胞(n = 3)的组织的色素沉着进行了比较,这些表达衰老的表型。皮肤颜色的显着增加(亮度降低)以及表皮黑色素含量和黑色素生成基因表达的增加揭示了在自然光老化的成纤维细胞存在下色素沉着的刺激作用,从而证实了我们的假设。总而言之,这些数据表明皮肤模型的色素沉着水平受到真皮成纤维细胞的影响,并且自然光老化的成纤维细胞可以促进与光老化相关的色素沉着过度。

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