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山梨醇酐单油酸酯稳定的 Cubosomes 和 Hexosomes 作为生物相容性的纳米平台用于对抗皮肤转移性人黑色素瘤。

Cubosomes and hexosomes stabilized by sorbitan monooleate as biocompatible nanoplatforms against skin metastatic human melanoma.

机构信息

Department of Chemistry, Lund University, SE-22100 Lund, Sweden.

Department of Chemical and Geological Sciences, University of Cagliari, s.s. 554 bivio Sestu, I-09042 Monserrato, CA, Italy; Department of Physical and Quantum Chemistry, Faculty of Chemistry, Wroclaw University, University of Science and Technology, Wyb. Wyspianskiego 27, 50-370 Wroclaw, Poland; CSGI, Consorzio Interuniversitario per lo Sviluppo dei Sistemi a Grande Interfase, 50019 Sesto Fiorentino, FI, Italy.

出版信息

J Colloid Interface Sci. 2025 Jan;677(Pt B):842-852. doi: 10.1016/j.jcis.2024.08.126. Epub 2024 Aug 16.

Abstract

Nanoparticles have become versatile assets in the medical field, providing notable benefits across diverse medical arenas including controlled drug delivery, imaging, and immunological assays. Among these, non-lamellar lipid nanoparticles, notably cubosomes and hexosomes, showcase remarkable biocompatibility and stability, rendering them as optimal choices for theranostic applications. Particularly, incorporating edge activators like sodium taurocholate enhances the potential of these nanoparticles for dermal and transdermal drug delivery, overcoming the stratum corneum, a first line of defense in our skin. This study reports on the formulation of monoolein-based cubosomes and hexosomes incorporating taurocholate and stabilized by Span 80 and co-encapsulating Chlorin e6 and coenzyme QH for photodynamic therapy in skin metastatic melanoma. The formulations were optimized using small-angle X-ray scattering, and cryo-transmission electron microscopy confirmed the presence of cubosomes or hexosomes, depending on the ratio between taurocholate and Span 80. Furthermore, the co-loaded nanoparticles exhibited high encapsulation efficiencies for both Ce6 and the coenzyme QH. In vitro studies on human melanoma cells (Me45) demonstrated the biocompatibility and photodynamic activity of the loaded formulations. These findings show the possibility of formulating more biocompatible cubosomes and hexosomes for photodynamic therapy in skin cancer treatment.

摘要

纳米粒子已成为医学领域的多功能资产,在包括药物控制释放、成像和免疫分析在内的多个医学领域提供显著的益处。在这些纳米粒子中,非层状脂质纳米粒子,特别是立方脂质体和六方脂质体,表现出显著的生物相容性和稳定性,使其成为治疗学应用的理想选择。特别是,加入胆汁酸钠等边缘活性剂可以增强这些纳米粒子用于皮肤和透皮药物输送的潜力,克服了我们皮肤的第一道防线——角质层。本研究报告了基于单油酸甘油酯的立方脂质体和六方脂质体的配方,其中包含胆汁酸钠,并由 Span 80 稳定,并共包封氯己定和辅酶 QH 用于皮肤转移性黑色素瘤的光动力治疗。使用小角 X 射线散射对配方进行了优化,而冷冻传输电子显微镜证实了立方脂质体或六方脂质体的存在,这取决于胆汁酸钠和 Span 80 之间的比例。此外,负载的纳米粒子对 Ce6 和辅酶 QH 均表现出高包封效率。对人黑色素瘤细胞(Me45)的体外研究表明了负载配方的生物相容性和光动力活性。这些发现表明有可能为皮肤癌治疗的光动力疗法制定更具生物相容性的立方脂质体和六方脂质体。

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