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Nile Red 和 Rhodamine 标记荧光聚合物胶束共价结合对各自药物传递系统成像改善的影响。

Impact of covalently Nile Red and covalently Rhodamine labeled fluorescent polymer micelles for the improved imaging of the respective drug delivery system.

机构信息

School of Pharmaceutical Sciences, University of Geneva, University of Lausanne, 1 Rue Michel Servet, CH-1206 Geneva, Switzerland.

School of Pharmaceutical Sciences, University of Geneva, University of Lausanne, 1 Rue Michel Servet, CH-1206 Geneva, Switzerland.

出版信息

Eur J Pharm Biopharm. 2019 Sep;142:480-487. doi: 10.1016/j.ejpb.2019.07.020. Epub 2019 Jul 20.

Abstract

Novel fluorescently labeled poly(ethylene glycol)-poly(hydroxyoctanoic acid) (MPEG-PHOA) block-copolymers were synthesized for the improved visualization of the deriving polymeric micelle drug delivery system. Albeit commonly used, one has to be aware that by simple incorporation of Nile Red (hydrophobic) or Rhodamine B (hydrophilic) as fluorescent compounds in nanocarriers (e.g., nanoparticles, liposomes or micelles) for imaging applications, these fluorescent probes can diffuse out of the carrier system and lead to artefacts due to the concomitant fluorescence loss or areal distribution. In order to inhibit such an uncontrolled diffusion, the Nile Red derivative 2-((9-(diethylamino)-5-oxo-5H-benzo[a]phenoxazin-2-yl)oxy)acetic acid was synthesized and covalently attached to the MPEG-PHOA block-copolymer via a mild Mitsunobu reaction to yield the desired MPEG-PHOA-Nile Red polymer for micelle preparations. Rhodamine B was coupled via its native carboxylic acid group with the copolymer MPEG-PHOA under mild conditions using DMAP, EDC, and NHS. For the proof of concept, aqueous solutions of composite micelles made of 0.5% (w/w fluorescence dye) MPEG-PHOA-dye and MPEG-PHOA copolymers were prepared ("spiking" of the non-labeled base MPEG-PHOA micelles) and characterized by transmission electron microscopy (TEM), dialysis and fluorescence spectrometry. The fluorescence intensity of the Nile Red in the solutions was followed up at physiological temperatures and pH values (37 °C, pH = 7.4 PBS buffer 0.01 M) over a period of 8 weeks. The labeled and non-labeled micelle formulations were tested in vitro in cells (Rhodamine-micelle formulations), then in vivo in a case study of an ophthalmic application (Nile Red micelle formulations). Both in vitro and in vivo experiments revealed a significant improvement of fluorescence stability of the MPEG-PHOA-dye formulations, facilitating the investigations on tracing the micelles and their stability. The results clearly demonstrate the value of the novel Nile Red and Rhodamine derivatives, whose simple synthesis and covalent attachment may easily be transferred to other nanosized polymeric drug delivery systems, e.g., MPEGylated or non-MPEGylated PLA/PLGA nanoparticles and be envisioned for novel theranostic systems.

摘要

为了改善衍生的聚合物胶束药物递送系统的可视化效果,合成了新型荧光标记的聚(乙二醇)-聚(羟基辛酸)(MPEG-PHOA)嵌段共聚物。尽管通常使用,但人们必须意识到,通过将尼罗红(疏水性)或罗丹明 B(亲水性)简单地掺入纳米载体(例如纳米粒子、脂质体或胶束)中用于成像应用,这些荧光探针可能会从载体系统中扩散出来,并由于伴随的荧光损失或面积分布而导致伪影。为了抑制这种不受控制的扩散,合成了尼罗红衍生物 2-((9-(二乙氨基)-5-氧代-5H-苯并[a]吩恶嗪-2-基)氧基)乙酸,并通过温和的 Mitsunobu 反应将其共价连接到 MPEG-PHOA 嵌段共聚物上,得到所需的 MPEG-PHOA-尼罗红聚合物用于胶束制备。通过其天然羧酸基团,在温和条件下将罗丹明 B 与共聚物 MPEG-PHOA 偶联,使用 DMAP、EDC 和 NHS。为了验证概念,制备了由 0.5%(w/w 荧光染料)MPEG-PHOA-染料和 MPEG-PHOA 共聚物组成的复合胶束的水溶液(“标记”非标记的基础 MPEG-PHOA 胶束),并通过透射电子显微镜(TEM)、透析和荧光光谱法进行表征。在生理温度和 pH 值(37°C,pH=7.4 PBS 缓冲液 0.01 M)下,在 8 周的时间内跟踪尼罗红在溶液中的荧光强度。标记和未标记的胶束制剂在细胞(罗丹明胶束制剂)中进行了体外测试,然后在眼科应用的案例研究(尼罗红胶束制剂)中进行了体内测试。体外和体内实验均表明,MPEG-PHOA-染料制剂的荧光稳定性得到了显著改善,这有助于研究胶束及其稳定性的追踪。结果清楚地表明了新型尼罗红和罗丹明衍生物的价值,其简单的合成和共价连接可以很容易地转移到其他纳米尺寸的聚合物药物递送系统中,例如 MPEG 化或非 MPEG 化的 PLA/PLGA 纳米粒子,并可用于新型治疗诊断系统。

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