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将一种水油不溶性顺铂衍生物转化为用于癌症治疗的纳米颗粒制剂。

Turning a water and oil insoluble cisplatin derivative into a nanoparticle formulation for cancer therapy.

作者信息

Guo Shutao, Wang Yuhua, Miao Lei, Xu Zhenghong, Lin Ching-Hsuan M, Huang Leaf

机构信息

Division of Molecular Pharmaceutics and Center for Nanotechnology in Drug Delivery, Eshelman School of Pharmacy, University of North Carolina at Chapel Hill, Chapel Hill, NC 27599, USA.

Division of Molecular Pharmaceutics and Center for Nanotechnology in Drug Delivery, Eshelman School of Pharmacy, University of North Carolina at Chapel Hill, Chapel Hill, NC 27599, USA.

出版信息

Biomaterials. 2014 Aug;35(26):7647-53. doi: 10.1016/j.biomaterials.2014.05.045. Epub 2014 Jun 8.

Abstract

The formulation of water insoluble organic compounds into nanoparticles has become a widely established method for enhancing the delivery and efficacy of cancer therapeutics. Therefore, a comparable approach when applied to water insoluble inorganic compounds should also promote similar advantages. Herein, we have successfully formulated insoluble iodinated cisplatin (CDDP-I) into an LPI NPs (lipid-coated iodinated CDDP nanoparticles). Two separate microemulsions were combined, each containing a precursor for the synthesis of CDDP-I. The resulting CDDP-I precipitate was then coated with an anionic lipid and dispersed in water with the help of an additional lipid. This method allows us to effectively encapsulate CDDP-I and was able to achieve a considerable drug loading of 82 wt%. Administered LPI NPs demonstrated high level accumulation in tumor tissues and exhibited an anti-cancer activity comparable to free CDDP in two melanoma xenograft models without inducing nephrotoxicity. The benefits offered through this delivery formulation are not unique to CDDP-I, as this versatile platform may be extended to the formulation of other inorganic compounds that are both water and oil insoluble into nanoparticles for superior anti-cancer efficacy.

摘要

将水不溶性有机化合物制成纳米颗粒已成为一种广泛应用的方法,用于提高癌症治疗药物的递送效率和疗效。因此,将类似方法应用于水不溶性无机化合物时,也应能带来相似的优势。在此,我们成功地将不溶性碘化顺铂(CDDP-I)制成了LPI纳米颗粒(脂质包被碘化顺铂纳米颗粒)。将两种单独的微乳液混合,每种微乳液都含有用于合成CDDP-I的前体。然后,将生成的CDDP-I沉淀物用阴离子脂质包被,并在另一种脂质的帮助下分散于水中。该方法使我们能够有效地包封CDDP-I,并实现了高达82 wt%的可观药物载量。在两种黑色素瘤异种移植模型中,给予的LPI纳米颗粒在肿瘤组织中显示出高水平的蓄积,并且表现出与游离顺铂相当的抗癌活性,同时不会诱导肾毒性。这种递送制剂所带来的益处并非CDDP-I所独有,因为这个通用平台可扩展用于将其他既不溶于水也不溶于油的无机化合物制成纳米颗粒,以实现卓越的抗癌疗效。

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