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基于聚甘油的纳米凝胶的温敏性和柔软性对其经皮渗透和细胞摄取的影响。

Effects of thermoresponsivity and softness on skin penetration and cellular uptake of polyglycerol-based nanogels.

机构信息

Clinical Research Center for Hair and Skin Science, Department of Dermatology and Allergy, Charité-Universitätsmedizin Berlin, Charitéplatz 1, 10117 Berlin, Germany.

Institut für Chemie und Biochemie, Freie Universität Berlin, Takustrasse 3, 14195 Berlin, Germany.

出版信息

J Control Release. 2016 Apr 28;228:159-169. doi: 10.1016/j.jconrel.2016.02.047. Epub 2016 Mar 3.

Abstract

Nanogels are water soluble cross-linked polymer networks with nanometer size dimensions that can be designed to incorporate different types of compounds and are promising carrier systems for drugs and biological molecules. In this study, the interactions of thermoresponsive nanogels (tNGs) with the human skin barrier and underlying epidermis cells were investigated with the aim of using such macromolecules to improve dermal and transdermal drug delivery. The investigated tNGs were made of acrylated dendritic polyglycerol, as water soluble cross-linker, and of oligo ethylene glycol methacrylate (OEGMA) as subunit conferring thermoresponsive properties. tNGs with different polymer transition temperatures were tagged with Rhodamine B (RhdB) and analyzed for their physicochemical properties. We found that tNGs with cloud point temperatures (Tcps) of 38 °C (tNG-RhdB-T38) lost softness (measured by PeakForce quantitative nanomechanics, QNM) and aggregated to bigger sized particles (measured as increase of particle average size by dynamic light scattering, DLS) when temperature changed from 15 to 37 °C. On the contrary, at the same conditions, tNGs with higher Tcps (tNG-RhdB-T55) did not show any significant changes of these characteristics. Applied on excised human skin, both tNGs penetrated deep in the stratum corneum (SC). Small amounts of tNGs were detected also in cells of the viable epidermis. Interestingly, whereas tNG softness correlated with higher penetration in SC, a better cellular uptake was observed for the thermoresponsive tNG-RhdB-T38. We conclude that soft nanocarriers possess a high SC penetration ability and that thermoresponsive nanogels are attractive carrier systems for the targeting of drugs to epidermis cells.

摘要

纳米凝胶是具有纳米尺寸的水溶性交联聚合物网络,可设计用于掺入不同类型的化合物,是药物和生物分子的有前途的载体系统。在这项研究中,研究了温敏纳米凝胶(tNG)与人皮肤屏障和下面的表皮细胞的相互作用,目的是使用此类大分子来改善皮肤和经皮药物传递。研究中使用的 tNG 由丙烯酰化树枝状聚甘油作为水溶性交联剂和聚乙二醇甲基丙烯酸酯(OEGMA)作为赋予温敏特性的亚基制成。具有不同聚合物转变温度的 tNG 用 Rhodamine B(RhdB)标记,并分析其物理化学性质。我们发现,云点温度(Tcps)为 38°C 的 tNG(tNG-RhdB-T38)在温度从 15°C 变为 37°C 时失去柔软性(通过 PeakForce 定量纳米力学 QNM 测量)并聚集形成更大的颗粒(通过动态光散射 DLS 测量的颗粒平均尺寸增加)。相反,在相同条件下,Tcps 更高的 tNG(tNG-RhdB-T55)没有显示出这些特性的任何明显变化。应用于离体人皮肤上时,两种 tNG 都深入渗透到角质层(SC)中。在有活力的表皮细胞中也检测到少量的 tNG。有趣的是,尽管 tNG 的柔软性与 SC 中的更高渗透能力相关,但对热敏 tNG-RhdB-T38 观察到更好的细胞摄取。我们得出的结论是,柔软的纳米载体具有高 SC 渗透能力,而温敏纳米凝胶是将药物靶向表皮细胞的有吸引力的载体系统。

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