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A New Approach to Deliver Anti-cancer Nanodrugs with Reduced Off-target Toxicities and Improved Efficiency by Temporarily Blunting the Reticuloendothelial System with Intralipid

机译:通过暂时钝化网状内皮系统和脂质体内来提供降低靶外毒性和提高效率的抗癌纳米药物的新方法

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We have developed a new strategy to temporarily blunt the reticuloendothelial system uptake of nanodrugs, a major challenge for nanodrug delivery and causing off-target toxicities, using an FDA approved nutrition supplement, Intralipid. We have tested our methodology in rats using an experimental platinum-containing anti-cancer nanodrug and three FDA approved nanodrugs, Abraxane, Marqibo, and Onivyde, to determine their toxicities in liver, spleen, and kidney, with and without the addition of Intralipid. Our method illustrates its potentials to deliver nanodrugs with an increase in the bioavailability and a decrease in toxicities. Our study shows that Intralipid treatment exhibits no harmful effect on tumor growing and no negative effect on the anti-tumor efficacy of the platinum-containing nanodrug, as well as animal survival rate in a HT-29 xenograft mouse model. Our methodology could also be a valuable complement/supplement to the “stealth” strategies. Our approach is a general one applicable to any approved and in-development nanodrugs without additional modification of the nanodrugs, thus facilitating its translation to clinical settings.
机译:我们已经开发出一种新的策略,可以使用FDA批准的营养补充剂Intralipid暂时抑制纳米药物对网状内皮系统的吸收,这是纳米药物输送的主要挑战,并且会引起脱靶毒性。我们已经在大鼠中使用实验性的含铂抗癌纳米药物和三种FDA批准的纳米药物Abraxane,Marqibo和Onivyde对我们的方法进行了测试,以确定添加和不添加脂质内药物对肝脏,脾脏和肾脏的毒性。我们的方法说明了其在生物利用度增加和毒性降低的情况下提供纳米药物的潜力。我们的研究表明,在HT-29异种移植小鼠模型中,脂质体内治疗对肿瘤的生长没有有害影响,对含铂纳米药物的抗肿瘤功效以及动物存活率也没有负面影响。我们的方法也可以作为“隐身”策略的宝贵补充/补充。我们的方法是一种通用方法,适用于任何已批准和正在开发的纳米药物,而无需对纳米药物进行额外的修饰,从而有助于将其翻译成临床药物。

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