TPGS 介导的转吸附体通过对变形性和稳定性的影响增强姜黄素的透皮给药。

Teng Guo, Chenming Zhang, Yuling Chen, Yihan Wu, Zhenda Liu, Yongtai Zhang, Nianping Feng
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引用次数: 0

摘要

背景:添加适当的表面活性剂可以提高透硫体的透皮渗透性,同时还能利用其作为功能材料的特性。本研究以 D-α-生育酚酸聚乙二醇琥珀酸酯(TPGS)为边缘活化剂,制备了用于姜黄素(Cur)透皮递送的透硫体:方法:制备并优化了TPGS介导的姜黄素负载透硫体(Cur@TES),并对优化后的制剂进行了形态、粒度、包埋效率(EE)和载药量(DL)的表征。研究了 Cur@TES 的稳定性和变形性,并通过体外透皮试验和荧光成像研究了 Cur@TES 的透皮给药效果。为了确定 Cur@TES.Results 的抗炎效果,对小鼠耳朵肿胀模型进行了研究:Cur@TES呈圆形或椭圆形。优化配方的粒度、EE 和 DL 分别为 131.2 ± 7.2 nm、97.68 ± 2.26% 和 6.58 ± 0.62%。X 射线衍射分析证实,囊泡内核形成了无序结构。此外,与载姜黄素的乙硫体(Cur@ES)相比,Cur@TES 系统表现出更好的稳定性和可变形性。体外透皮实验表明,Cur@TES 能显著增加皮肤中的药物保留量(P<0.05)。荧光成像证实,TPGS 介导的透硫体在皮肤中的分布明显增强。此外,在小鼠耳肿胀模型中,Cur@TES 对炎性肿胀有明显的抑制作用:结论:TPGS 介导的反式硫体具有明显的透皮优势和更强的抗炎效果,为姜黄素的透皮给药提供了新的视角。
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TPGS-mediated Transethosomes Enhance Transdermal Administration of Curcumin via Effects on Deformability and Stability.

Background: Adding a suitable surfactant can enhance the transdermal permeability of transethosomes while also leveraging its functionality as a functional material. In this study, transethosomes were prepared using D-α-tocopherol acid polyethylene glycol succinate (TPGS) as edge activators for transdermal delivery of curcumin (Cur).

Methods: The TPGS-mediated curcumin-loaded transethosomes (Cur@TES) were prepared and formulated optimally, and the optimized formulations were characterized for their morphology, particle size, entrapment efficiency (EE) and drug loading (DL). The stability and deformability of Cur@TES were investigated, while the transdermal delivery of Cur@TES was investigated through in vitro transdermal assays and fluorescence imaging. A mouse ear swelling model was performed to determine the anti-inflammatory effect of Cur@TES.

Results: Cur@TES appeared round or elliptical in shape. The particle size, EE and DL for the optimized formulation were observed as 131.2 ± 7.2 nm, 97.68 ± 2.26%, and 6.58 ± 0.62%, respectively. X-ray diffraction analysis confirmed the formation of disordered structures in the inner core of the vesicles. Moreover, Cur@TES system demonstrated better stability and deformability compared to the curcumin-loaded ethosomes (Cur@ES). In-vitro transdermal experiments demonstrated that Cur@TES significantly increased the amount of drug retained in the skin (P<0.05). Fluorescence imaging confirmed that the skin distribution were distinctly enhanced with the delivery by TPGS mediated transethosomes. In addition, Cur@TES showed a significant inhibitory effect on Inflammatory swelling in the mouse ear-swelling model.

Conclusion: TPGS-mediated transethosomes exhibit significant transdermal advantages and enhanced anti-inflammatory effects, providing a new perspective for the transdermal delivery of curcumin.

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