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皮肤干燥可能与真皮基质改变有关。

The possible involvement of skin dryness on alterations of the dermal matrix.

作者信息

Yokota Mariko, Shimizu Kenji, Kyotani Daiki, Yahagi Shoichi, Hashimoto Satoru, Masaki Hitoshi

机构信息

NIKKOL Group, COSMOS Technical Center Co., Ltd., 3-24-3 Hasune, Itabashi-ku, Tokyo, 174-0046, Japan.

出版信息

Exp Dermatol. 2014 Oct;23 Suppl 1:27-31. doi: 10.1111/exd.12392.

Abstract

Moisturization of the skin plays an important role in maintaining skin homeostasis. Although it is understood that skin dryness initiates the formation of fine wrinkles, there are few objective reports to support that understanding. The purpose of this study was to establish an in vitro dry epidermal model using reconstructed human epidermal equivalents (RHEEs) and to elucidate the relationship between skin dryness and alterations of the dermal matrix which is one of the causes for the formation of wrinkles. An in vitro dry epidermal model was prepared by loading a CaCl2 -filled ampoule on the surface of an RHEE. To evaluate whether the in vitro model reproduced the characteristics of in vivo skin dryness, histological studies and biological assays using a protein array were carried out. Histologically, a distinct fluorescence which originated from carbonylated protein was observed in the stratum corneum. In addition, conditioned medium from RHEEs cultured under dry conditions for 24 h revealed the secretion of several proteins, such as IL-1α, IL-1ra, IL-8, MMP-9, VEGF, M-CSF and IGFBP-2 and IGFBP-3, galectin-1, Cys-C, FGF-6, OPG, Glc and TSP4 compared with normal RHEEs. It has been reported that an increase in IL-1α and the accumulation of carbonylated proteins are observed in the intact stratum corneum in the low humidity winter season. Thus, the in vitro dry epidermal model expresses the features of in vivo skin dryness observed in the winter season. Furthermore, the conditioned medium from RHEEs cultured under dry conditions enhanced MMP-1 secretion by normal human dermal fibroblasts. Taken together, we propose the hypothesis that skin dryness contributes to alterations of the dermal matrix through the elevation of MMP-1 secretion.

摘要

皮肤保湿在维持皮肤内环境稳定中起着重要作用。尽管人们知道皮肤干燥会引发细纹形成,但鲜有客观报告支持这一认知。本研究的目的是利用重建的人表皮替代物(RHEE)建立体外干性表皮模型,并阐明皮肤干燥与真皮基质改变之间的关系,而真皮基质改变是皱纹形成的原因之一。通过将装有氯化钙的安瓿加载到RHEE表面制备体外干性表皮模型。为评估该体外模型是否重现了体内皮肤干燥的特征,进行了组织学研究和使用蛋白质阵列的生物学检测。在组织学上,在角质层中观察到源自羰基化蛋白质的明显荧光。此外,与正常RHEE相比,在干燥条件下培养24小时的RHEE的条件培养基显示出几种蛋白质的分泌,如IL-1α、IL-1ra、IL-8、MMP-9、VEGF、M-CSF和IGFBP-2和IGFBP-3、半乳糖凝集素-1、胱抑素-C、FGF-6、骨保护素、葡萄糖和血小板反应蛋白4。据报道,在低湿度冬季,完整的角质层中观察到IL-1α增加和羰基化蛋白质积累。因此,体外干性表皮模型表达了冬季观察到的体内皮肤干燥的特征。此外,在干燥条件下培养的RHEE的条件培养基增强了正常人真皮成纤维细胞的MMP-1分泌。综上所述,我们提出一个假说,即皮肤干燥通过MMP-1分泌的增加导致真皮基质的改变。

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