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人皮肤成纤维细胞亚群对可见光和近红外光的不同反应:光生物调节在治疗皮肤疾病方面的潜力。

Differential response of human dermal fibroblast subpopulations to visible and near-infrared light: Potential of photobiomodulation for addressing cutaneous conditions.

作者信息

Mignon Charles, Uzunbajakava Natallia E, Castellano-Pellicena Irene, Botchkareva Natalia V, Tobin Desmond J

机构信息

Centre for Skin Sciences, University of Bradford, BD71DP, Bradford, United-Kingdom.

Philips Research, High Tech Campus, Eindhoven, Netherlands.

出版信息

Lasers Surg Med. 2018 Oct;50(8):859-882. doi: 10.1002/lsm.22823. Epub 2018 Apr 17.

Abstract

BACKGROUND OBJECTIVES

The past decade has witnessed a rapid expansion of photobiomodulation (PBM), demonstrating encouraging results for the treatment of cutaneous disorders. Confidence in this approach, however, is impaired not only by a lack of understanding of the light-triggered molecular cascades but also by the significant inconsistency in published experimental outcomes, design of the studies and applied optical parameters. This study aimed at characterizing the response of human dermal fibroblast subpopulations to visible and near-infrared (NIR) light in an attempt to identify the optical treatment parameters with high potential to address deficits in aging skin and non-healing chronic wounds.

MATERIALS AND METHODS

Primary human reticular and papillary dermal fibroblasts (DF) were isolated from the surplus of post-surgery human facial skin. An in-house developed LED-based device was used to irradiate cell cultures using six discrete wavelengths (450, 490, 550, 590, 650, and 850 nm). Light dose-response at a standard oxygen concentration (20%) at all six wavelengths was evaluated in terms of cell metabolic activity. This was followed by an analysis of the transcriptome and procollagen I production at a protein level, where cells were cultured in conditions closer to in vivo at 2% environmental oxygen and 2% serum. Furthermore, the production of reactive oxygen species (ROS) was accessed using real-time fluorescence confocal microscopy imaging. Here, production of ROS in the presence or absence of antioxidants, as well as the cellular localization of ROS, was evaluated.

RESULTS

In terms of metabolic activity, consecutive irradiation with short-wavelength light (⇐530 nm) exerted an inhibitory effect on DF, while longer wavelengths (>=590 nm) had essentially a neutral effect. Cell behavior following treatment with 450 nm was biphasic with two distinct states: inhibitory at low- to mid- dose levels (<=30 J/cm ), and cytotoxic at higher dose levels (>30 J/cm ). Cell response to blue light was accompanied by a dose-dependent release of ROS that was localized in the perinuclear area close to mitochondria, which was attenuated by an antioxidant. Overall, reticular DFs exhibited a greater sensitivity to light treatment at the level of gene expression than did papillary DFs, with more genes significantly up- or down- regulated. At the intra-cellular signaling pathway level, the up- or down- regulation of vital pathways was observed only for reticular DF, after treatment with 30 J/cm of blue light. At the cellular level, short visible wavelengths exerted a greater inhibitory effect on reticular DF. Several genes involved in the TGF-β signaling pathway were also affected. In addition, procollagen I production was inhibited. By contrast, 850 nm near-infrared (NIR) light (20 J/cm ) exerted a stimulatory metabolic effect in these cells, with no detectable intracellular ROS formation. Here too, reticular DF were more responsive than papillary DF. This stimulatory effect was only observed under in vivo-like low oxygen conditions, corresponding to normal dermal tissue oxygen levels (approximately 2%).

CONCLUSION

This study highlights a differential impact of light on human skin cells with upregulation of metabolic activity with NIR light, and inhibition of pro-collagen production and proliferation in response to blue light. These findings open-up new avenues for developing therapies for different cutaneous conditions (e.g., treatment of keloids and fibrosis) or differential therapy at distinct stages of wound healing. Lasers Surg. Med. 50:859-882, 2018. © 2018 Wiley Periodicals, Inc.

摘要

背景目的

在过去十年中,光生物调节(PBM)迅速发展,在治疗皮肤疾病方面取得了令人鼓舞的成果。然而,人们对这种方法的信心不仅受到对光触发分子级联反应缺乏了解的影响,还受到已发表实验结果、研究设计和应用光学参数显著不一致的影响。本研究旨在表征人真皮成纤维细胞亚群对可见光和近红外(NIR)光的反应,以试图确定具有高潜力的光学治疗参数,以解决衰老皮肤和不愈合慢性伤口的缺陷。

材料和方法

从手术后人面部皮肤剩余组织中分离出原代人网状和乳头层真皮成纤维细胞(DF)。使用内部开发的基于发光二极管(LED)的设备,以六个离散波长(450、490、550、590、650和850nm)照射细胞培养物。根据细胞代谢活性评估在标准氧浓度(20%)下所有六个波长的光剂量反应。随后在蛋白质水平上分析转录组和I型前胶原的产生,细胞在更接近体内的条件下培养,环境氧浓度为2%,血清浓度为2%。此外,使用实时荧光共聚焦显微镜成像检测活性氧(ROS)的产生。在此,评估了在有或没有抗氧化剂存在的情况下ROS的产生以及ROS在细胞内的定位。

结果

就代谢活性而言,用短波长光(≤530nm)连续照射对DF有抑制作用,而较长波长(≥590nm)基本上具有中性作用。用450nm光处理后的细胞行为呈双相性,有两种不同状态:在低至中等剂量水平(≤30J/cm²)时具有抑制作用,在较高剂量水平(>30J/cm²)时具有细胞毒性。细胞对蓝光的反应伴随着剂量依赖性的ROS释放,其定位在线粒体附近的核周区域,抗氧化剂可使其减弱。总体而言,在基因表达水平上,网状DF比乳头层DF对光治疗表现出更高的敏感性,有更多基因显著上调或下调。在细胞内信号通路水平上,在用30J/cm²蓝光处理后,仅在网状DF中观察到重要通路的上调或下调。在细胞水平上,短可见光波长对网状DF具有更大的抑制作用。参与转化生长因子-β(TGF-β)信号通路中的几个基因也受到影响。此外,I型前胶原的产生受到抑制。相比之下,850nm近红外(NIR)光(20J/cm²)对这些细胞具有刺激代谢作用,未检测到细胞内ROS形成。在此,网状DF也比乳头层DF反应更敏感。这种刺激作用仅在类似体内的低氧条件下观察到,对应于正常真皮组织氧水平(约2%)。

结论

本研究强调了光对人皮肤细胞的不同影响,近红外光上调代谢活性,而蓝光抑制前胶原产生和增殖。这些发现为开发针对不同皮肤状况(如瘢痕疙瘩和纤维化的治疗)或伤口愈合不同阶段的差异疗法开辟了新途径。《激光外科与医学》50:859 - 882,2018年。©2018威利期刊公司

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