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首页> 外文期刊>International Journal of Pharmaceutics >The risk of hydroquinone and sunscreen over-absorption via photodamaged skin is not greater in senescent skin as compared to young skin: Nude mouse as an animal model
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The risk of hydroquinone and sunscreen over-absorption via photodamaged skin is not greater in senescent skin as compared to young skin: Nude mouse as an animal model

机译:与年轻皮肤相比,衰老皮肤中光损伤性皮肤对苯二酚和防晒霜过度吸收的风险不大:裸鼠作为动物模型

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摘要

Intrinsic aging and photoaging modify skin structure and components, which subsequently change percutaneous absorption of topically applied permeants. The purpose of this study was to systematically evaluate drug/sunscreen permeation via young and senescent skin irradiated by ultraviolet (UV) light. Both young and senescent nude mice were subjected to UVA (10 J/cm(2)) and/or UVB radiation (175 mJ/cm(2)). Physiological parameters, immunohistology, and immunoblotting were employed to examine the aged skin. Hydroquinone and sunscreen permeation was determined by in vitro Franz cell. In vivo skin absorption was documented using a hydrophilic dye, rhodamine 123 (log P = -0.4), as a permeant. UVA exposure induced cyclooxygenase (COX)-2 and terminal deoxynucleotidyl transferase dUTP nick end labeling (TUNEL) upregulation. Epidermal tight junction (TJ) were degraded by UVA. UVB increased transepidermal water loss (TEWL) from 13 to 24 g/m(2)/h. Hyperplasia and inflammation, but not loss of TJ, were also observed in UVB-treated skin. UVA + UVB-and UVA-irradiated skin demonstrated similar changes in histology and biomarkers. UVA + UVB or UVA exposure increased hydroquinone flux five-fold. A negligible alteration of hydroquinone permeation was shown with UVB exposure. Hydroquinone exhibited a lower penetration through senescent skin than young skin. Both UVA and UVB produced enhancement of oxybenzone flux and skin uptake. However, the amount of increase was less than that of hydroquinone delivery. Photoaging did not augment skin absorption of sunscreens with higher lipophilicity, including avobenzone and ZnO. Exposure to UVA generally increased follicular entrance of these permeants, which showed two-to three-fold greater follicular uptake compared to the untreated group. Photoaging had less impact on drug/sunscreen absorption with more lipophilic permeants. Percutaneous absorption did not increase in skin subjected to both intrinsic and extrinsic aging. (C) 2014 Elsevier B.V. All rights reserved.
机译:内在的老化和光老化会改变皮肤的结构和成分,从而改变局部应用的渗透剂的经皮吸收。这项研究的目的是系统地评估通过紫外线(UV)照射的年轻和衰老皮肤的药物/防晒霜渗透性。年轻和衰老的裸鼠均接受UVA(10 J / cm(2))和/或UVB辐射(175 mJ / cm(2))。使用生理参数,免疫组织学和免疫印迹检查老化的皮肤。通过体外Franz细胞测定对苯二酚和防晒剂的渗透率。使用亲水性染料若丹明123(log P = -0.4)作为渗透剂记录了体内皮肤吸收。 UVA暴露诱导的环氧合酶(COX)-2和末端脱氧核苷酸转移酶dUTP缺口末端标记(TUNEL)上调。表皮紧密连接(TJ)被UVA降解。 UVB使经表皮水分流失(TEWL)从13增加到24 g / m(2)/ h。在经UVB处理的皮肤中也观察到增生和炎症,但未见TJ丢失。 UVA + UVB和UVA照射的皮肤在组织学和生物标志物方面表现出相似的变化。 UVA + UVB或UVA暴露使氢醌通量增加了五倍。 UVB暴露显示对苯二酚渗透的变化可忽略不计。对苯二酚对衰老皮肤的渗透性低于年轻皮肤。 UVA和UVB均可增强氧苯甲通量和皮肤吸收。但是,增加量小于对苯二酚的递送量。光老化不会增加亲脂性较高的防晒霜(包括阿伏苯宗和ZnO)的皮肤吸收。暴露于UVA通常会增加这些渗透物的卵泡进入,与未治疗组相比,卵泡吸收显示高出2到3倍。光老化对脂类/防晒霜的吸收影响较小,亲脂性渗透剂较多。在经历内在和外在衰老的皮肤中,经皮吸收均没有增加。 (C)2014 Elsevier B.V.保留所有权利。

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