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一种亲脂性天然产物补骨脂酚的皮肤递送及生物分布:纳米载体性能比较

Cutaneous delivery and biodistribution of a lipophilic natural product - bakuchiol: Comparing nanocarrier performance.

作者信息

Syafitri Erga, Kalia Yogeshvar N

机构信息

School of Pharmaceutical Sciences, University of Geneva, Geneva, Switzerland; Institute of Pharmaceutical Sciences of Western Switzerland, University of Geneva, Geneva, Switzerland; Department of Pharmacy, Faculty of Science, Institut Teknologi Sumatera, South Lampung, Lampung, Indonesia.

School of Pharmaceutical Sciences, University of Geneva, Geneva, Switzerland; Institute of Pharmaceutical Sciences of Western Switzerland, University of Geneva, Geneva, Switzerland.

出版信息

Int J Pharm. 2025 Aug 20;681:125886. doi: 10.1016/j.ijpharm.2025.125886. Epub 2025 Jun 23.

Abstract

Bakuchiol (BAK) is a natural bioactive agent described as a functional analogue of retinol that acts through the same cellular pathways. Its lipophilicity (log K 6.1) and oily state at ambient temperature pose significant challenges in formulation development. This study investigated the use of different nanocarriers to develop primarily aqueous formulations of BAK and their ability to facilitate its cutaneous delivery. Micelles were prepared using solvent evaporation, microemulsions (ME) were formulated using the water titration method, and nanoemulsions (NE1 and NE2 - with and without oleic acid, respectively) were produced using ultrasonication. Optimized micelles formed using D-α-Tocopherol polyethylene glycol 1000 succinate (TPGS) and Poloxamer 407 demonstrated encapsulation efficiencies of 96.6 ± 3.2 % and 101.5 ± 0.3 %, with particle sizes of 28 nm (PDI 0.21) and 27 nm (PDI 0.092), respectively. NE2 had a higher encapsulation efficiency (106.8 ± 5.7 %) than either NE1 (90.2 ± 2.4 %) or ME (86.3 ± 4.6 %). The micro- and nanoemulsions exhibited larger sizes than the micelles (ME: 108 nm; NE1: 129. nm; NE2: 68 nm). Cutaneous delivery experiments demonstrated that NE1 and NE2 resulted in 3-4 fold higher BAK deposition than either the micelles or microemulsion; thus, oleic acid content was not determining BAK delivery. These findings suggest that the thermodynamic activity and molecular physicochemical properties are more important for skin delivery, than simply considering the size of the nanocarrier; which will not necessarily retain its structure upon contact with skin. Cutaneous biodistribution experiments to determine the spatial distribution of BAK confirmed that nanoemulsions effectively targeted the viable epidermis and dermis - key sites for BAK's biological effects, with concentrations 36-fold higher than the minimum effective concentration.

摘要

补骨脂酚(BAK)是一种天然生物活性剂,被描述为视黄醇的功能类似物,通过相同的细胞途径发挥作用。其亲脂性(log K 6.1)以及在环境温度下的油状状态给制剂开发带来了重大挑战。本研究调查了使用不同的纳米载体来开发主要为水性的BAK制剂及其促进其经皮递送的能力。通过溶剂蒸发制备胶束,使用水滴定法配制微乳液(ME),并使用超声处理制备纳米乳液(NE1和NE2,分别含有和不含油酸)。使用聚乙二醇1000琥珀酸酯-α-生育酚(TPGS)和泊洛沙姆407形成的优化胶束的包封率分别为96.6±3.2%和101.5±0.3%,粒径分别为28nm(PDI 0.21)和27nm(PDI 0.092)。NE2的包封率(106.8±5.7%)高于NE1(90.2±2.4%)或ME(86.3±4.6%)。微乳液和纳米乳液的粒径比胶束大(ME:108nm;NE1:129nm;NE2:68nm)。经皮递送实验表明,NE1和NE2导致的BAK沉积比胶束或微乳液高3至4倍;因此,油酸含量不是决定BAK递送的因素。这些发现表明,对于皮肤递送而言,热力学活性和分子物理化学性质比仅仅考虑纳米载体的大小更为重要;纳米载体与皮肤接触后不一定会保持其结构。确定BAK空间分布的经皮生物分布实验证实,纳米乳液有效地靶向了有活力的表皮和真皮——BAK发挥生物学效应的关键部位,其浓度比最低有效浓度高36倍。

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