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与来自人类包皮的角质形成细胞、黑素细胞和成纤维细胞相比,真皮干细胞作为黑素细胞前体的 UVB 损伤反应。

UVB damage response of dermal stem cells as melanocyte precursors compared to keratinocytes, melanocytes, and fibroblasts from human foreskin.

机构信息

Skin Cancer Center, Division of Molecular Cell Biology, Elbe Klinikum Buxtehude, 21614 Buxtehude, Germany.

Pediatric Practice, 22587 Hamburg, Germany.

出版信息

J Photochem Photobiol B. 2021 Jul;220:112216. doi: 10.1016/j.jphotobiol.2021.112216. Epub 2021 May 17.

Abstract

Ultraviolet B (UVB) radiation induces mutagenic DNA photolesions in skin cells especially in form of cyclobutane pyrimidine dimers (CPDs). Protection mechanisms as DNA repair and apoptosis are of great importance in order to prevent skin carcinogenesis. In human skin, neural crest-derived precursors of melanocytes, the dermal stem cells (DSCs), are discussed to be at the origin of melanoma. Although they are constantly exposed to solar UV radiation, it is still not investigated how DSCs cope with UV-induced DNA damage. Here, we report a comparative study of the DNA damage response after irradiation with a physiological relevant UVB dose in DSCs in comparison to fibroblasts, melanocytes and keratinocytes isolated from human foreskin. Within our experimental settings, DSCs were able to repair DNA photolesions as efficient as the other skin cell types with solely keratinocytes repairing significantly faster. Interestingly, only fibroblasts showed significant alterations in cell cycle distribution in terms of a transient S phase arrest following irradiation. Moreover, with the applied UVB dose none of the examined cell types was prone to UVB-induced apoptosis. This may cause persistent genomic alterations and in case of DSCs it may have severe consequences for their daughter cells, the differentiated melanocytes. Altogether, this is the first study demonstrating a similar UV response in dermal stem cells compared to differentiated skin cells.

摘要

紫外线 B(UVB)辐射会在皮肤细胞中引起诱变 DNA 光损伤,尤其是形成环丁烷嘧啶二聚体(CPDs)。为了防止皮肤癌变,DNA 修复和细胞凋亡等保护机制非常重要。在人类皮肤中,黑素细胞的神经嵴前体,即真皮干细胞(DSCs),被认为是黑色素瘤的起源。尽管它们经常暴露在太阳紫外线辐射下,但仍不清楚 DSCs 如何应对紫外线诱导的 DNA 损伤。在这里,我们报告了一项比较研究,即在与来自人包皮的成纤维细胞、黑素细胞和角质形成细胞相比,用生理相关的 UVB 剂量照射 DSCs 后,对 DNA 损伤反应的研究。在我们的实验设置中,DSCs 能够像其他皮肤细胞类型一样有效地修复 DNA 光损伤,而只有角质形成细胞的修复速度明显更快。有趣的是,只有成纤维细胞在照射后细胞周期分布方面表现出明显的变化,表现为短暂的 S 期阻滞。此外,在所应用的 UVB 剂量下,没有一种被检查的细胞类型容易受到 UVB 诱导的凋亡。这可能导致持续的基因组改变,如果发生在 DSCs 中,可能会对其分化的黑素细胞后代产生严重后果。总的来说,这是第一项研究表明真皮干细胞与分化的皮肤细胞相比具有相似的紫外线反应。

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