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采用 AF4/MALLS 和 DLS 评估人工肠液中的共存胶体相:对胆酸盐和(溶)磷脂混合物的系统研究,纳入塞来昔布作为模型药物。

Co-existing colloidal phases in artificial intestinal fluids assessed by AF4/MALLS and DLS: A systematic study into cholate & (lyso-) phospholipid blends, incorporating celecoxib as a model drug.

机构信息

Drug Transport & Delivery Group, Department of Physics, Chemistry & Pharmacy, University of Southern Denmark, Odense, Denmark.

Drug Transport & Delivery Group, Department of Physics, Chemistry & Pharmacy, University of Southern Denmark, Odense, Denmark.

出版信息

Eur J Pharm Sci. 2018 Jul 30;120:61-72. doi: 10.1016/j.ejps.2018.04.031. Epub 2018 Apr 26.

Abstract

Colloidal phases (self-assemblies) in aqueous dispersions of selected binary bile salt/phospholipid blends were studied utilizing the combined analytical approach of asymmetrical flow field-flow fractionation (AF4) and multi-angle laser light scattering (MALLS) in order to resolve the co-existence of different colloidal assemblies. The binary blends were prepared by freeze-drying from tert-butanol/water co-solvent solutions. The blends contained one of two bile salts (sodium taurocholate (TC) or sodium glycodeoxycholate (GDX)) and a mono- or di-acyl phospholipid (lyso-phosphatidylcholine (L-PC) and phosphatidylcholine (PC), respectively). Bile salt and phospholipid (PL) concentrations and their respective ratios were varied systematically within the physiological range found in human intestinal fluids. Furthermore, the BCS class II drug Celecoxib was incorporated in selected blends to assess its potential impact on colloidal phases. To further investigate the smallest self-assemblies observed in AF4/MALLS analysis, dispersions of TC and GDX, respectively, were prepared and analyzed by dynamic light scattering (DLS). AF4/MALLS analysis revealed that binary bile-salt/phospholipid blends form three distinct particle fractions, when the concentration of bile-salt was sufficiently high (≥3.5 mM). Those fractions were assumed to be very small pure bile-salt dimeric/oligomeric self-assemblies (Ø ≈ 2-3 nm), mid-sized mixed micelles (Ø ≈ 10-50 nm) and large liposomes/aggregates (Ø ≈ 150-280 nm). If present, Celecoxib was found solubilized within the structures, but at the lowest TC concentration triggered the formation of an additional (vesicular) phase.

摘要

利用不对称流场流分离(AF4)和多角度激光光散射(MALLS)相结合的分析方法,研究了选定的二元胆汁盐/磷脂混合物在水基分散体中的胶体相(自组装体),以解决不同胶体组装体共存的问题。二元混合物通过从叔丁醇/水共溶剂溶液中冷冻干燥制备。混合物包含两种胆汁盐(牛磺胆酸钠(TC)或甘氨胆酸钠(GDX))中的一种和单或双酰基磷脂(分别为溶磷脂酰胆碱(L-PC)和磷脂酰胆碱(PC))。胆汁盐和磷脂(PL)浓度及其各自的比例在人类肠液中发现的生理范围内系统地变化。此外,将 BCS 类 II 药物塞来昔布掺入选定的混合物中,以评估其对胶体相的潜在影响。为了进一步研究在 AF4/MALLS 分析中观察到的最小自组装体,分别制备并通过动态光散射(DLS)分析 TC 和 GDX 的分散体。AF4/MALLS 分析表明,当胆汁盐浓度足够高(≥3.5mM)时,二元胆汁盐/磷脂混合物形成三种不同的颗粒级分。这些级分被认为是非常小的纯胆汁盐二聚体/低聚物自组装体(Ø≈2-3nm)、中等大小的混合胶束(Ø≈10-50nm)和大的脂质体/聚集体(Ø≈150-280nm)。如果存在,塞来昔布被发现溶解在结构中,但在最低 TC 浓度下触发了另一种(囊泡)相的形成。

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