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重复低剂量可见光照射对浅色和深色皮肤个体的临床和分子变化的影响。

Clinical and molecular change induced by repeated low-dose visible light exposure in both light-skinned and dark-skinned individuals.

机构信息

Department of Dermatology, Johns Hopkins School of Medicine, Baltimore, Maryland, USA.

Department of Dermatology, Soonchunhyang University Seoul Hospital, Seoul, South Korea.

出版信息

Photodermatol Photoimmunol Photomed. 2023 May;39(3):204-212. doi: 10.1111/phpp.12819. Epub 2022 Aug 1.

Abstract

BACKGROUND

Visible light (VL) is known to induce pigmentation in dark-skinned individuals and immediate erythema in light-skinned individuals. However, the effects of accumulated low-dose VL exposure across skin types are not well established.

METHODS

Thirty-one healthy subjects with light (Fitzpatrick skin types [FST] I-II, n = 13) and dark (FST V-VI, n = 18) skin types were enrolled. Subjects' buttocks were exposed daily to VL, wavelength 400-700 nm, with a dose of 120 J/cm at 50 mW/cm , for four consecutive days. Microarray using Affymetrix GeneChip (49,395 genes) was performed followed by qRT-PCR on skin samples.

RESULTS

Repeated low-dose VL irradiation induced immediate pigment darkening and delayed tanning in dark-skinned individuals while no discernable pigmentation and erythema were observed in light-skinned individuals. Top ten upregulated genes by repeated VL exposure in microarray included melanogenic genes such as tyrosinase (TYR), tyrosinase-related protein-1 (TYRP1), dopachrome tautomerase (DCT), premelanosome protein (PMEL), melan-A (MLANA), and solute carrier family 24, member 5 (SLC24A5) and genes involved in inflammation/matrix remodeling/cell signaling including chemokine (C-C motif) ligand 18 (CCL18), BCL2-related protein A1 (BCL2A1), and cartilage oligomeric matrix protein (COMP). In qRT-PCR CCL18 was upregulated in light skin with a greater extent (mean fold change ± SD; 4.03 ± 3.28, p = .04) than in dark-skinned individuals (1.91 ± 1.32, p = .07) while TYR was not significantly upregulated in both skin types.

CONCLUSION

This study highlights the genes upregulated by cumulative VL exposure involved in pigmentation, immune response, oxidation/reduction, and matrix remodeling across skin types providing relevant information on daily solar exposure.

摘要

背景

可见光(VL)已知可诱导深色皮肤个体的色素沉着和浅色皮肤个体的即时红斑。然而,不同类型皮肤累积低剂量 VL 暴露的影响尚未得到很好的确立。

方法

招募了 31 名健康的浅色(Fitzpatrick 皮肤类型 [FST] I-II,n=13)和深色(FST V-VI,n=18)皮肤类型的受试者。将受试者的臀部每天暴露于波长为 400-700nm、剂量为 120J/cm 的 VL,光强为 50mW/cm2,连续照射 4 天。随后对皮肤样本进行 Affymetrix GeneChip 微阵列分析和 qRT-PCR。

结果

重复低剂量 VL 照射诱导深色皮肤个体的即时色素沉着加深和延迟晒黑,而浅色皮肤个体则未观察到明显的色素沉着和红斑。微阵列中重复 VL 暴露上调的前 10 个基因包括黑色素生成基因,如酪氨酸酶(TYR)、酪氨酸酶相关蛋白-1(TYRP1)、多巴色素互变异构酶(DCT)、黑素前体蛋白(PMEL)、黑素-A(MLANA)和溶质载体家族 24 成员 5(SLC24A5)以及参与炎症/基质重塑/细胞信号转导的基因,包括趋化因子(C-C 基元)配体 18(CCL18)、B 细胞淋巴瘤 2 相关蛋白 A1(BCL2A1)和软骨寡聚基质蛋白(COMP)。qRT-PCR 显示 CCL18 在浅色皮肤中的上调程度更大(平均倍数变化±标准差;4.03±3.28,p=0.04),而 TYR 在两种皮肤类型中均未显著上调。

结论

本研究强调了不同类型皮肤累积 VL 暴露所上调的基因,这些基因涉及色素沉着、免疫反应、氧化/还原和基质重塑,为日常太阳暴露提供了相关信息。

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