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本文引用的文献

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Mechanisms of Light-induced Liposome Permeabilization.光诱导脂质体通透性增加的机制。
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Chemophototherapy: An Emerging Treatment Option for Solid Tumors.化学光动力疗法:实体肿瘤的一种新兴治疗选择。
Adv Sci (Weinh). 2016 May 24;4(1):1600106. doi: 10.1002/advs.201600106. eCollection 2017 Jan.
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Ultrasmall Biocompatible BiSe Nanodots for Multimodal Imaging-Guided Synergistic Radiophotothermal Therapy against Cancer.用于多模态成像引导的协同放化疗的超小生物相容性 BiSe 纳米点。
ACS Nano. 2016 Dec 27;10(12):11145-11155. doi: 10.1021/acsnano.6b06067. Epub 2016 Dec 6.
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Sphingomyelin Liposomes Containing Porphyrin-phospholipid for Irinotecan Chemophototherapy.含卟啉磷脂的鞘磷脂脂质体用于伊立替康化学光动力疗法
Theranostics. 2016 Oct 1;6(13):2329-2336. doi: 10.7150/thno.15701. eCollection 2016.
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Dual-Stimuli Responsive Nanotheranostics for Multimodal Imaging Guided Trimodal Synergistic Therapy.双重刺激响应型纳米诊疗剂用于多模态成像引导的三模态协同治疗
Small. 2017 Feb;13(6). doi: 10.1002/smll.201602580. Epub 2016 Nov 15.
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Black Phosphorus Nanosheets as a Robust Delivery Platform for Cancer Theranostics.黑磷纳米片作为癌症治疗与诊断一体化的稳健递药平台。
Adv Mater. 2017 Jan;29(1). doi: 10.1002/adma.201603276. Epub 2016 Oct 31.
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Design of Hydrated Porphyrin-Phospholipid Bilayers with Enhanced Magnetic Resonance Contrast.水合卟啉磷脂双层的设计具有增强的磁共振对比。
Small. 2017 Jan;13(1). doi: 10.1002/smll.201602505. Epub 2016 Oct 14.
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Chlorin-Based Nanoscale Metal-Organic Framework Systemically Rejects Colorectal Cancers via Synergistic Photodynamic Therapy and Checkpoint Blockade Immunotherapy.基于氯的纳米级金属有机骨架系统地通过协同光动力疗法和检查点封锁免疫疗法来排斥结直肠癌。
J Am Chem Soc. 2016 Sep 28;138(38):12502-10. doi: 10.1021/jacs.6b06663. Epub 2016 Sep 14.
9
Rapid Light-Triggered Drug Release in Liposomes Containing Small Amounts of Unsaturated and Porphyrin-Phospholipids.含少量不饱和及卟啉磷脂的脂质体中光触发的快速药物释放
Small. 2016 Jun;12(22):3039-47. doi: 10.1002/smll.201503966. Epub 2016 Apr 28.
10
Indocyanine Green-Loaded Liposomes for Light-Triggered Drug Release.用于光触发药物释放的载吲哚菁绿脂质体
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多功能脂质体用于图像引导的肿瘤内化疗-光疗。

Multifunctional Liposomes for Image-Guided Intratumoral Chemo-Phototherapy.

机构信息

Department of Biomedical Engineering, University at Buffalo, State University of New York, Buffalo, NY, 14260, USA.

Department of Pharmacology and Therapeutics, Roswell Park Cancer Institute, Buffalo, NY, 14263, USA.

出版信息

Adv Healthc Mater. 2017 Aug;6(16). doi: 10.1002/adhm.201700253. Epub 2017 May 15.

DOI:10.1002/adhm.201700253
PMID:28504409
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5568974/
Abstract

Intratumoral (IT) drug injections reduce systemic toxicity, but delivered volumes and distribution can be inconsistent. To improve IT delivery paradigms, porphyrin-phospholipid (PoP) liposomes are passively loaded with three hydrophilic cargos: sulforhodamine B, a fluorophore; gadolinium-gadopentetic acid, a magnetic resonance (MR) agent; and oxaliplatin, a colorectal cancer chemotherapeutic. Liposome composition is optimized so that cargo is retained in serum and storage, but is released in less than 1 min with exposure to near infrared light. Light-triggered release occurs with PoP-induced photooxidation of unsaturated lipids and all cargos release concurrently. In subcutaneous murine colorectal tumors, drainage of released cargo is delayed when laser treatment occurs 24 h after IT injection, at doses orders of magnitude lower than systemic ones. Delayed light-triggering results in substantial tumor shrinkage relative to controls a week following treatment, although regrowth occurs subsequently. MR imaging reveals that over this time frame, pools of liposomes within the tumor migrate to adjacent regions, possibly leading to altered spatial distribution during triggered drug release. Although further characterization of cargo loading and release is required, this proof-of-principle study suggests that multimodal theranostic IT delivery approaches hold potential to both guide injections and interpret outcomes, in particular when combined with chemo-phototherapy.

摘要

瘤内(IT)药物注射可降低全身毒性,但输送的体积和分布可能不一致。为了改进 IT 输送模式,卟啉 - 磷脂(PoP)脂质体被动加载三种亲水性载药:磺基罗丹明 B,荧光团;钆 - 二乙三胺五乙酸,磁共振(MR)造影剂;奥沙利铂,结直肠癌化疗药物。脂质体的组成经过优化,使载药在血清和储存中保留,但在近红外光照射下不到 1 分钟即可释放。光触发释放发生在 PoP 诱导的不饱和脂质的光氧化和所有载药的同时释放。在皮下结直肠肿瘤的小鼠模型中,当激光治疗在 IT 注射后 24 小时进行时,释放的载药的引流会被延迟,而激光治疗的剂量要低几个数量级。与对照组相比,在治疗后一周,延迟光触发导致肿瘤显著缩小,尽管随后肿瘤会再次生长。MR 成像显示,在这段时间内,肿瘤内的脂质体池迁移到相邻区域,可能导致在触发药物释放时改变空间分布。尽管需要进一步对载药和释放进行特征描述,但这项原理验证研究表明,多模式治疗性 IT 输送方法具有引导注射和解释结果的潜力,特别是当与化疗 - 光疗相结合时。