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局部应用α-三联噻吩与紫外线A辐射诱导的皮肤光毒性的特征

Characterization of cutaneous phototoxicity induced by topical alpha-terthienyl and ultraviolet A radiation.

作者信息

Rampone W M, McCullough J L, Weinstein G D, Towers G H, Berns M W, Abeysekera B

出版信息

J Invest Dermatol. 1986 Sep;87(3):354-7. doi: 10.1111/1523-1747.ep12524490.

DOI:10.1111/1523-1747.ep12524490
PMID:3734487
Abstract

Alpha-terthienyl (alpha-T), a phototoxic thiophene compound isolated from marigolds (Tagetes species), affects cell membranes and does not appear to induce cytogenetic damage. This study was undertaken to investigate topical delivery of alpha-T and characterize its cutaneous phototoxicity in combination with long-wave UV radiation (UVA) in comparison with locally (intradermal) administered alpha-T. Percutaneous penetration (PC) of 0.1% and 1% alpha-T in a 3% Azone gel vehicle was studied in guinea pig skin in vitro and quantitated by UV fluorescence microscopy. Dose-dependent PC of epidermis, adnexae, and superficial dermis was demonstrated in vitro. Alpha-terthienyl (0.1% and 1%) in this vehicle was applied topically in vivo and irradiated with 30 J/cm2 UVA at intervals of 10 min-24 h. Maximum sensitization was achieved with irradiation 1 h following drug application. The clinical response was dose-dependent consisting of erythema, edema, crusting, erosion, and inhibition of hair growth and was observed 72 h to 7 days postirradiation. A comparable dose-dependent phototoxic response was observed when 5-500 micrograms alpha-T were injected intradermally and irradiated with UVA. These results indicated that low-dose topical alpha-T in a nonirritating vehicle can rapidly produce cutaneous photosensitization. Topical alpha-T/UVA may provide a selective and safer alternative approach for the photochemotherapy of psoriasis and other cutaneous diseases.

摘要

α-三联噻吩(α-T)是一种从万寿菊(万寿菊属植物)中分离出的光毒性噻吩化合物,它会影响细胞膜,似乎不会诱导细胞遗传损伤。本研究旨在研究α-T的局部给药,并与局部(皮内)给药的α-T相比,表征其与长波紫外线辐射(UVA)联合时的皮肤光毒性。在体外研究了0.1%和1%α-T在3%氮酮凝胶载体中的经皮渗透(PC),并通过紫外荧光显微镜进行定量。体外证明了表皮、附属器和浅表真皮的剂量依赖性PC。将该载体中的α-三联噻吩(0.1%和1%)局部应用于体内,并每隔10分钟至24小时用30 J/cm2 UVA照射。给药后1小时照射可实现最大致敏。临床反应呈剂量依赖性,包括红斑、水肿、结痂、糜烂和毛发生长抑制,在照射后72小时至7天观察到。当皮内注射5-500微克α-T并用UVA照射时,观察到类似的剂量依赖性光毒性反应。这些结果表明,低剂量局部应用于无刺激性载体中的α-T可迅速产生皮肤光敏作用。局部应用α-T/UVA可能为银屑病和其他皮肤病的光化学疗法提供一种选择性和更安全的替代方法。

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