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唑来膦酸在通过反相微乳液法合成的基于双膦酸盐-金属络合物的纳米颗粒制剂中的体内分布。

In vivo distribution of zoledronic acid in a bisphosphonate-metal complex-based nanoparticle formulation synthesized by a reverse microemulsion method.

作者信息

Li Xu, Naguib Youssef W, Cui Zhengrong

机构信息

The University of Texas at Austin, College of Pharmacy, Division of Molecular Pharmaceutics and Drug Delivery, Austin, TX, United States.

The University of Texas at Austin, College of Pharmacy, Division of Molecular Pharmaceutics and Drug Delivery, Austin, TX, United States; Inner Mongolia Medical University, Inner Mongolia Key Laboratory of Molecular Biology, Hohhot, Inner Mongolia, China.

出版信息

Int J Pharm. 2017 Jun 30;526(1-2):69-76. doi: 10.1016/j.ijpharm.2017.04.053. Epub 2017 Apr 26.

Abstract

Bisphosphonates are used to treat bone diseases such as osteoporosis and cancer-induced bone pain and fractures. It is thought that modifying the pharmacokinetics and biodistribution profiles of bisphosphonates (i.e. rapid renal clearance and extensive bone absorption) will not only reduce their side effects, but also expand their clinical applications to extraskeletal tissues. In the present work, using zoledronic acid (Zol) and calcium as model bisphosphonate and metal molecules, respectively, we prepared DOPA (an anionic lipid)-coated spherical Zol-Ca nanocomposites (Zol-Ca@DOPA) and developed Zol-nanoparticle formulations (i.e. Zol-Ca@bi-lipid NPs) based on the nanocomposites. The influence of the inputted weight ratio of Zol-Ca@DOPA to DSPE-PEG on the properties (e.g. size, size distribution, loading efficiency, encapsulation efficiency, zeta potential, and polydispersity) of Zol-Ca@bi-lipid NPs was investigated, and a type of Zol-Ca@bi-lipid NPs with size around 25nm was selected for further studies. In a mouse model, the Zol-Ca@bi-lipid NPs significantly reduced the bone distribution of Zol, increased the blood circulating time of Zol, and altered the distribution of Zol in major organs, as compared to free Zol. It is expected that similar nanoparticles prepared with bisphosphonate-metal complexes can be explored to expand the applications to bisphosphonates in extraskeletal tissues.

摘要

双膦酸盐用于治疗骨质疏松症、癌症引起的骨痛和骨折等骨疾病。人们认为,改变双膦酸盐的药代动力学和生物分布特征(即快速肾清除和广泛的骨吸收)不仅会减少其副作用,还会将其临床应用扩展到骨骼外组织。在本研究中,我们分别使用唑来膦酸(Zol)和钙作为双膦酸盐和金属分子的模型,制备了多巴胺(一种阴离子脂质)包被的球形Zol-Ca纳米复合材料(Zol-Ca@DOPA),并基于该纳米复合材料开发了Zol纳米颗粒制剂(即Zol-Ca@双脂质纳米颗粒)。研究了Zol-Ca@DOPA与DSPE-PEG的输入重量比对Zol-Ca@双脂质纳米颗粒性质(如尺寸、尺寸分布、负载效率、包封率、zeta电位和多分散性)的影响,并选择了一种尺寸约为25nm的Zol-Ca@双脂质纳米颗粒进行进一步研究。在小鼠模型中,与游离Zol相比,Zol-Ca@双脂质纳米颗粒显著降低了Zol在骨中的分布,延长了Zol的血液循环时间,并改变了Zol在主要器官中的分布。预计可以探索用双膦酸盐-金属络合物制备类似的纳米颗粒,以扩大双膦酸盐在骨骼外组织中的应用。

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