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包封的阿霉素晶体影响溶血磷脂温度敏感脂质体的体外和体内释放及治疗效果。

Encapsulated doxorubicin crystals influence lysolipid temperature-sensitive liposomes release and therapeutic efficacy in vitro and in vivo.

机构信息

School of Pharmacy, Queen's University Belfast, Belfast BT9 7BL, United Kingdom.

Department of Applied Physics, Aalto University School of Science, P.O. Box 15100, FI-00076 Aalto, Finland.

出版信息

J Control Release. 2020 Dec 10;328:665-678. doi: 10.1016/j.jconrel.2020.09.032. Epub 2020 Sep 19.

DOI:10.1016/j.jconrel.2020.09.032
PMID:32961247
Abstract

Doxorubicin (DOX)-loaded lysolipid temperature-sensitive liposomes (LTSLs) are a promising stimuli-responsive drug delivery system that rapidly releases DOX in response to mild hyperthermia (HT). This study investigates the influence of loaded DOX crystals on the thermosensitivity of LTSLs and their therapeutic efficacy in vitro and in vivo. The properties of DOX crystals were manipulated using different remote loading methods (namely (NH)SO, NH-EDTA and MnSO) and varying the lipid:DOX weight ratio during the loading step. Our results demonstrated that (NH)SO or NH-EDTA remote loading methods had a comparable encapsulation efficiency (EE%) into LTSLs in contrast to the low DOX EE% obtained using the metal complexation method. Cryogenic transmission electron microscopy (cryo-TEM) revealed key differences in the nature of DOX crystals formed inside LTSLs based on the loading buffer or/and the lipid:DOX ratio used, resulting in different DOX release profiles in response to mild HT. The in vitro assessment of DOX release/uptake in CT26 and PC-3 cells revealed that the use of a high lipid:DOX ratio exhibited a fast and controlled release profile in combination with mild HT, which correlated well with their cytotoxicity studies. Similarly, in vivo DOX release, tumour growth inhibition and mice survival rates were influenced by the physicochemical properties of LTSLs payload. This study demonstrates, for the first time, that the characteristics of DOX crystals loaded into LTSLs, and their conformational rearrangement during HT, are important factors that impact the TSLs performance in vivo.

摘要

阿霉素(DOX)负载的溶脂温度敏感脂质体(LTSL)是一种很有前途的刺激响应药物输送系统,它可以在温和的热疗(HT)下迅速释放 DOX。本研究探讨了负载 DOX 晶体对 LTSL 热敏感性的影响及其在体外和体内的治疗效果。通过使用不同的远程加载方法(即(NH)SO、NH-EDTA 和 MnSO)和在加载步骤中改变脂质:DOX 重量比来操纵 DOX 晶体的性质。我们的结果表明,(NH)SO 或 NH-EDTA 远程加载方法与使用金属络合方法获得的低 DOX EE%相比,具有相当的 DOX 包封效率(EE%)进入 LTSL。低温透射电子显微镜(cryo-TEM)显示,根据加载缓冲液或/和使用的脂质:DOX 比,形成的 DOX 晶体的性质存在关键差异,导致在温和 HT 下释放曲线不同。在 CT26 和 PC-3 细胞中进行的 DOX 释放/摄取的体外评估表明,高脂质:DOX 比的使用与温和 HT 结合表现出快速和受控的释放曲线,这与其细胞毒性研究密切相关。同样,在体内,DOX 释放、肿瘤生长抑制和小鼠存活率受到 LTSL 有效负载的物理化学性质的影响。本研究首次证明,负载到 LTSL 中的 DOX 晶体的特性及其在 HT 期间的构象重排是影响 TSL 在体内性能的重要因素。

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