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A Prodrug Approach to the Use of Coumarins as Potential Therapeutics for Superficial Mycoses

机译:使用香豆素作为浅表真菌病的潜在治疗药物的前药方法

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摘要

Superficial mycoses are fungal infections of the outer layers of the skin, hair and nails that affect 20–25% of the world's population, with increasing incidence. Treatment of superficial mycoses, predominantly caused by dermatophytes, is by topical and/or oral regimens. New therapeutic options with improved efficacy and/or safety profiles are desirable. There is renewed interest in natural product-based antimicrobials as alternatives to conventional treatments, including the treatment of superficial mycoses. We investigated the potential of coumarins as dermatophyte-specific antifungal agents and describe for the first time their potential utility as topical antifungals for superficial mycoses using a prodrug approach. Here we demonstrate that an inactive coumarin glycone, esculin, is hydrolysed to the antifungal coumarin aglycone, esculetin by dermatophytes. Esculin is hydrolysed to esculetin β-glucosidases. We demonstrate that β-glucosidases are produced by dermatophytes as well as members of the dermal microbiota, and that this activity is sufficient to hydrolyse esculin to esculetin with concomitant antifungal activity. A β-glucosidase inhibitor (conduritol B epoxide), inhibited antifungal activity by preventing esculin hydrolysis. Esculin demonstrates good aqueous solubility (<6 g/l) and could be readily formulated and delivered topically as an inactive prodrug in a water-based gel or cream. This work demonstrates proof-of-principle for a therapeutic application of glycosylated coumarins as inactive prodrugs that could be converted to an active antifungal in situ. It is anticipated that this approach will be applicable to other coumarin glycones.
机译:浅表霉菌病是皮肤,头发和指甲外层的真菌感染,影响全世界20%至25%的人口,且发病率不断上升。主要由皮肤癣菌引起的浅表霉菌病的治疗是通过局部和/或口服方案。期望具有改善的功效和/或安全性概况的新的治疗选择。人们对基于天然产物的抗菌剂产生了新的兴趣,这些抗菌剂可以替代常规疗法,包括治疗浅表真菌病。我们研究了香豆素作为皮肤真菌特异性抗真菌剂的潜力,并首次使用前药方法描述了它们作为浅表霉菌的局部抗真菌剂的潜在效用。在这里,我们证明了一种无活性的香豆素香豆素,七叶皂甙被皮肤真菌水解为抗真菌的香豆素糖苷,七叶皂素。 Esculin水解为七叶皂苷β-葡萄糖苷酶。我们证明了β-葡糖苷酶是由皮肤真菌以及皮肤微生物群的成员产生的,并且这种活性足以将七叶皂苷水解为七叶亭,同时具有抗真菌活性。 β-葡萄糖苷酶抑制剂(conduritol B环氧化物)可通过防止七叶皂苷水解来抑制抗真菌活性。 Esculin具有良好的水溶性(<6 g / l),可以很容易地配制成非活性前药,并在水性凝胶或乳膏中局部给药。这项工作证明了糖基化香豆素作为无活性前药的治疗应用的原理证明,该药物可以原位转化为活性抗真菌药。预期该方法将适用于其他香豆素糖苷。

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