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载有优化纳米结构脂质载体的四卡因的预配方研究。

A pre-formulation study of tetracaine loaded in optimized nanostructured lipid carriers.

机构信息

Department of Biochemistry and Tissue Biology, Institute of Biology, University of Campinas (UNICAMP), Rua Monteiro Lobato 255, Campinas, SP, 13083862, Brazil.

Institute of Biotechnology, Federal University of Uberlandia, Uberlandia, MG, Brazil.

出版信息

Sci Rep. 2021 Nov 2;11(1):21463. doi: 10.1038/s41598-021-99743-6.

Abstract

Tetracaine (TTC) is a local anesthetic broadly used for topical and spinal blockade, despite its systemic toxicity. Encapsulation in nanostructured lipid carriers (NLC) may prolong TTC delivery at the site of injection, reducing such toxicity. This work reports the development of NLC loading 4% TTC. Structural properties and encapsulation efficiency (%EE > 63%) guided the selection of three pre-formulations of different lipid composition, through a 2 factorial design of experiments (DOE). DLS and TEM analyses revealed average sizes (193-220 nm), polydispersity (< 0.2), zeta potential |- 21.8 to - 30.1 mV| and spherical shape of the nanoparticles, while FTIR-ATR, NTA, DSC, XRD and SANS provided details on their structure and physicochemical stability over time. Interestingly, one optimized pre-formulation (CP-TRANS/TTC) showed phase-separation after 4 months, as predicted by Raman imaging that detected lack of miscibility between its solid (cetyl palmitate) and liquid (Transcutol) lipids. SANS analyses identified lamellar arrangements inside such nanoparticles, the thickness of the lamellae been decreased by TTC. As a result of this combined approach (DOE and biophysical techniques) two optimized pre-formulations were rationally selected, both with great potential as drug delivery systems, extending the release of the anesthetic (> 48 h) and reducing TTC cytotoxicity against Balb/c 3T3 cells.

摘要

地卡因(TTC)是一种局部麻醉剂,广泛用于表面和脊髓阻滞,尽管它有全身毒性。将其封装在纳米结构脂质载体(NLC)中可能会延长在注射部位的递送时间,从而降低这种毒性。本工作报告了载有 4%TTC 的 NLC 的开发。结构特性和包封效率(%EE>63%)通过 2 因素实验设计(DOE)指导了三种不同脂质组成的预配方的选择。DLS 和 TEM 分析显示平均粒径(193-220nm)、多分散性(<0.2)、zeta 电位|-21.8 至-30.1mV|和纳米粒子的球形,而 FTIR-ATR、NTA、DSC、XRD 和 SANS 则提供了有关其结构和物理化学稳定性随时间变化的详细信息。有趣的是,一种优化的预配方(CP-TRANS/TTC)在 4 个月后显示出相分离,这正如拉曼成像所预测的那样,该成像检测到其固体(十六烷棕榈酸酯)和液体(Transcutol)脂质之间缺乏混溶性。SANS 分析确定了这些纳米粒子内部的层状排列,TTC 使层状的厚度减小。通过这种组合方法(DOE 和生物物理技术),合理选择了两种优化的预配方,它们都具有作为药物递送系统的巨大潜力,延长了麻醉剂的释放(>48h)并降低了 TTC 对 Balb/c 3T3 细胞的细胞毒性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d8be/8563806/1f7a905c9f6e/41598_2021_99743_Fig1_HTML.jpg

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