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短期慢性紫外线照射期间无毛小鼠皮肤中白细胞介素-1、整合素、cJun和cFos的稳态mRNA水平以及外用维甲酸的作用。

Steady-state mRNA levels of interleukin-1, integrins, cJun, and cFos in hairless mouse skin during short-term chronic UV exposure and the effect of topical tretinoin.

作者信息

Kligman L H, Yang S, Schwartz E

机构信息

Department of Dermatology, University of Pennsylvania School of Medicine, Philadelphia 19104, USA.

出版信息

Photodermatol Photoimmunol Photomed. 1999 Oct;15(5):198-204. doi: 10.1111/j.1600-0781.1999.tb00085.x.

Abstract

We have proposed that UV activation of cytokine and integrin signaling pathways may initiate the photoaging process and that one of the effects of tretinoin treatment may be to alter the cytokine and integrin patterns. In previous results, steady-state mRNA levels of interleukin-1alpha, tumor necrosis factor alpha, transforming growth factor beta, collagenase, stromelysin, collagen, and integrins (alpha1 and alpha2) were increased in the skin of hairless mice that were either UV treated or concurrently treated with UV followed by topical tretinoin for 5 weeks. The aim of this study was to focus on the expression of alpha1, alpha2 and alpha5 integrins, IL-1alpha, IL-1beta, cJun, and cFos at an earlier time point (3 weeks). Animals were UV irradiated thrice weekly for 3 weeks and were treated topically with either 0.05% tretinoin or the vehicle immediately after each exposure. Total RNA was prepared and used in RT-PCR with radiolabeled dCTP and specific primers. UV slightly increased steady-state mRNA levels for alpha1, alpha2 and alpha5 integrins whereas UV + tretinoin increased their expression (3-, 2- and 7-fold respectively). Steady-state mRNA levels for IL-1alpha, IL-1beta and cJun were increased with UV (3-, 12- and 6-fold respectively) and with UV + tretinoin (6-, 7- and 9-fold respectively). In contrast, cFos expression was unchanged. In situ staining for IL-1alpha mRNA was slightly more abundant in mice treated for 3 weeks with UV and UV + tretinoin than in controls whereas 5 weeks of UV + tretinoin treatment gave strongly positive staining. Results are consistent with cytokines and integrins mediating the effects of UV on the skin, with modulation of these effects by tretinoin.

摘要

我们提出,细胞因子和整合素信号通路的紫外线激活可能引发光老化过程,而维甲酸治疗的作用之一可能是改变细胞因子和整合素模式。在先前的结果中,无论是紫外线处理的无毛小鼠皮肤,还是紫外线处理后同时局部使用维甲酸5周的无毛小鼠皮肤,白细胞介素-1α、肿瘤坏死因子α、转化生长因子β、胶原酶、基质金属蛋白酶、胶原蛋白和整合素(α1和α2)的稳态mRNA水平均升高。本研究的目的是在更早的时间点(3周)关注α1、α2和α5整合素、IL-1α、IL-1β、cJun和cFos的表达。动物每周接受3次紫外线照射,共3周,每次照射后立即局部使用0.05%维甲酸或赋形剂。制备总RNA,并与放射性标记的dCTP和特异性引物一起用于逆转录聚合酶链反应(RT-PCR)。紫外线略微增加了α1、α2和α5整合素的稳态mRNA水平,而紫外线+维甲酸则增加了它们的表达(分别为3倍、2倍和7倍)。IL-1α、IL-1β和cJun的稳态mRNA水平在紫外线处理时增加(分别为3倍、12倍和6倍),在紫外线+维甲酸处理时增加(分别为6倍、7倍和9倍)。相比之下,cFos的表达没有变化。用紫外线和紫外线+维甲酸处理3周的小鼠中,IL-1α mRNA的原位染色略比对照组丰富,而紫外线+维甲酸处理5周则产生强阳性染色。结果表明细胞因子和整合素介导紫外线对皮肤的作用,维甲酸可调节这些作用。

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