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Oil components modulate the skin delivery of 5-aminolevulinic acid and its ester prodrug from oil-in-water and water-in-oil nanoemulsions

机译:油成分可调节水基油和油包水纳米乳剂在皮肤中释放的5-氨基乙酰丙酸及其酯前药

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摘要

The study evaluated the potential of nanoemulsions for the topical delivery of 5-aminolevulinic acid (ALA) and methyl ALA (mALA). The drugs were incorporated in oil-in-water (O/W) and water-in-oil (W/O) formulations obtained by using soybean oil or squalene as the oil phase. The droplet size, zeta potential, and environmental polarity of the nanocarriers were assessed as physicochemical properties. The O/W and W/O emulsions showed diameters of 216-256 and 18-125 nm, which, respectively, were within the range of submicron- and nano-sized dispersions. In vitro diffusion experiments using Franz-type cells and porcine skin were performed. Nude mice were used, and skin fluorescence derived from protoporphyrin IX was documented by confocal laser scanning microscopy (CLSM). The loading of ALA or mALA into the emulsions resulted in slower release across cellulose membranes. The release rate and skin flux of topical drug application were adjusted by changing the type of nanocarrier, the soybean oil O/W systems showing the highest skin permeation. This formulation increased ALA flux via porcine skin to 180 nmol/cm(2)/h, which was 2.6-fold that of the aqueous control. The CLSM results showed that soybean oil systems promoted mALA permeation to deeper layers of the skin from ∼100 μm to ∼140 μm, which would be beneficial for treating subepidermal and subcutaneous lesions. Drug permeation from W/O systems did not surpass that from the aqueous solution. An in vivo dermal irritation test indicated that the emulsions were safe for topical administration of ALA and mALA. DOI: 10.2147/IJN.S17524
机译:该研究评估了纳米乳剂局部递送5-氨基乙酰丙酸(ALA)和甲基ALA(mALA)的潜力。将药物掺入通过使用大豆油或角鲨烯作为油相而获得的水包油(O / W)和油包水(W / O)制剂中。纳米载体的液滴尺寸,ζ电势和环境极性被评估为物理化学性质。 O / W和W / O乳剂的直径分别为216-256和18-125 nm,分别在亚微米和纳米尺寸的分散体范围内。进行了使用Franz型细胞和猪皮肤的体外扩散实验。使用裸鼠,并通过共聚焦激光扫描显微镜(CLSM)记录了原卟啉IX产生的皮肤荧光。将ALA或mALA装入乳液中会导致跨纤维素膜的释放较慢。通过改变纳米载体的类型来调节局部药物应用的释放速率和皮肤通量,大豆油O / W系统显示出最高的皮肤渗透性。该配方使通过猪皮肤的ALA通量增加到180 nmol / cm(2)/ h,是水性对照的2.6倍。 CLSM结果表明,大豆油体系可将mALA渗透率从约100μm增至约140μm,渗入皮肤深层,这对于治疗表皮下和皮下病变非常有利。 W / O系统的药物渗透率不超过水溶液。体内皮肤刺激试验表明,该乳剂对于局部给药ALA和mALA是安全的。 DOI:10.2147 / IJN.S17524

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