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Doxorubicin Encapsulated in Stealth Liposomes Conferred with Light-Triggered Drug Release

机译:阿霉素封装在隐伏脂质体中具有轻触发的药物释放作用

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摘要

Stealth liposomes can be used to extend the blood circulation time of encapsulated therapeutics. Inclusion of 2 molar % porphyrin-phospholipid (PoP) imparted optimal near infrared (NIR) light-triggered release of doxorubicin (Dox) from conventional sterically stabilized stealth liposomes. The type and amount of PoP affected drug loading, serum stability and drug release induced by NIR light. Cholesterol and PEGylation were required for Dox loading, but slowed light-triggered release. Dox in stealth PoP liposomes had a long circulation half-life in mice of 21.9 hours and was stable in storage for months. Following intravenous injection and NIR irradiation, Dox deposition increased ~7 fold in treated subcutaneous human pancreatic xenografts. Phototreatment induced mild tumor heating and complex tumor hemodynamics. A single chemophototherapy treatment with Dox-loaded stealth PoP liposomes (at 5–7 mg/kg Dox) eradicated tumors while corresponding chemo- or photodynamic therapies were ineffective. A low dose 3 mg/kg Dox phototreatment with stealth PoP liposomes was more effective than a maximum tolerated dose of free (7 mg/kg) or conventional long-circulating liposomal Dox (21 mg/kg). To our knowledge, Dox-loaded stealth PoP liposomes represent the first reported long-circulating nanoparticle capable of light-triggered drug release.
机译:隐形脂质体可用于延长封装治疗剂的血液循环时间。包含2摩尔%的卟啉磷脂(PoP)可以从传统的空间稳定隐形脂质体中释放出最佳的近红外(NIR)光触发的阿霉素(Dox)释放。 PoP的类型和数量会影响NIR光诱导的载药量,血清稳定性和药物释放。装载Dox需要胆固醇和PEG化,但会降低光触发释放的速度。隐形PoP脂质体中的Dox在小鼠体内的循环半衰期较长,为21.9小时,并且可以稳定保存数月。静脉注射和近红外照射后,经皮下处理的人胰腺异种移植物的Dox沉积增加了约7倍。光疗引起轻度的肿瘤加热和复杂的肿瘤血液动力学。用载有Dox的隐形PoP脂质体(5-7 mg / kg Dox)进行的单一化学光疗可以根除肿瘤,而相应的化学或光动力疗法无效。低剂量3 mg / kg Dox隐形PoP脂质体光疗比最大耐受剂量的游离(7 mg / kg)或常规长循环脂质体Dox(21 mg / kg)更有效。据我们所知,载有Dox的隐形PoP脂质体代表了第一个报道的能够光触发药物释放的长循环纳米颗粒。

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