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近红外光触发热敏脂质体的快速、可逆释放

Rapid, Reversible Release from Thermosensitive Liposomes Triggered by Near-Infra-Red Light.

作者信息

Forbes Natalie, Pallaoro Alessia, Reich Norbert O, Zasadzinski Joseph A

机构信息

Department of Chemical Engineering, University of California, Santa Barbara, CA 93106.

Department of Chemistry, University of California, Santa Barbara, CA 93106.

出版信息

Part Part Syst Charact. 2014 Nov;31(11):1158-1167. doi: 10.1002/ppsc.201400035. Epub 2014 Jul 14.

Abstract

We present a novel drug carrier consisting of plasmonic hollow gold nanoshells (HGN) chemically tethered to liposomes made temperature sensitive with lysolipids (LTSL). Continuous-wave irradiation by physiologically friendly near infra-red light at 800 nm for 2.5 minutes at laser intensities an order of magnitude below that known to damage skin generates heating localized to the liposome membrane. The heating increases the liposome permeability in an irradiation dose-dependent, but reversible manner, resulting in rapid release of small molecules such as the self-quenching dye carboxyfluorescein or the chemotherapeutic doxorubicin, without raising the bulk temperature. The local rise in nanoshell temperature under laser irradiation was inferred by comparing dye release rates from the LTSL via bulk heating to that induced by irradiation. Laser-irradiation of LTSL enables precise control of contents release with low temperature gradients confined to areas irradiated by the laser focus. The combined effects of rapid local release and localized hyperthermia provide a synergistic effect as shown by a near doubling of androgen resistant PPC-1 prostate cancer cell toxicity compared to the same concentration of free doxorubicin.

摘要

我们展示了一种新型药物载体,它由与通过溶血脂质(LTSL)制成的温度敏感脂质体化学连接的等离子体中空金纳米壳(HGN)组成。在生理友好的800nm近红外光下以低于已知会损伤皮肤的激光强度一个数量级的强度连续照射2.5分钟,会使脂质体膜局部产生加热。这种加热以辐照剂量依赖但可逆的方式增加脂质体通透性,导致小分子如自猝灭染料羧基荧光素或化疗药物阿霉素快速释放,而不会升高整体温度。通过比较通过整体加热从LTSL释放染料的速率与辐照诱导的速率,推断出激光照射下纳米壳温度的局部升高。对LTSL进行激光照射能够精确控制内容物释放,低温梯度局限于激光焦点照射的区域。快速局部释放和局部热疗的联合作用产生了协同效应,与相同浓度的游离阿霉素相比,雄激素抗性PPC - 1前列腺癌细胞毒性几乎增加了一倍。

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