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Pharmacokinetic Evaluation of a DSPE-PEG2000 Micellar Formulation of Ridaforolimus in Rat

机译:Ridaforolimus DSPE-PEG2000胶束配方在大鼠中的药代动力学评估

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摘要

The rapamycin analog, ridaforolimus, has demonstrated potent anti-proliferative effects in cancer treatment, and it currently is being evaluated in a range of clinical cancer studies. Ridaforolimus is an extremely lipophilic compound with limited aqueous solubility, which may benefit from formulation with polymeric micelles. Herein, we report the encapsulation of ridaforolimus in 1,2-distearoyl-sn-glycero-3-phosphoethanolamine-N-methoxy-poly(ethylene glycol 2000) (DSPE-PEG2000) via a solvent extraction technique. Micelle loading greatly improved the solubility of ridaforolimus by approximately 40 times from 200 μg/mL to 8.9 mg/mL. The diameters of the drug-loaded micelles were 33 ± 15 nm indicating they are of appropriate size to accumulate within the tumor site via the enhanced permeability and retention (EPR) effect. The DSPE-PEG2000 micelle formulation was dosed intravenously to rats at 10 mg/kg and compared to a control of ridaforolimus in ethanol/PEG 400. The micelle significantly increased the half-life of ridaforolimus by 170% and decreased the clearance by 58%, which is consistent with improved retention of the drug in the plasma by the micelle formulation.
机译:雷帕霉素类似物ridaforolimus在癌症治疗中已显示出有效的抗增殖作用,目前正在一系列临床癌症研究中对其进行评估。 Ridaforolimus是一种极富亲脂性的化合物,具有有限的水溶性,可能会受益于聚合胶束的配制。在这里,我们报告了通过溶剂萃取技术在1,2-二硬脂酰基-sn-甘油-3-磷酸乙醇胺-N-甲氧基-聚(乙二醇2000)(DSPE-PEG2000)中包裹ridaforolimus的过程。从200μg/ mL到8.9 mg / mL,胶束的装载大大提高了ridaforolimus的溶解度约40倍。载药胶束的直径为33±15 nm,表明它们具有适当的大小,可以通过增强的通透性和保留(EPR)效应积聚在肿瘤部位内。将DSPE-PEG2000胶束制剂以10 mg / kg的剂量静脉内给予大鼠,并与乙醇/ PEG 400中的ridaforolimus对照进行比较。该胶束显着延长了ridaforolimus的半衰期170%,清除率降低了58%,这与通过胶束制剂改善的药物在血浆中的保留相一致。

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