聚合物胶束递送新型微管稳定剂和 Hedgehog 信号抑制剂治疗化疗耐药前列腺癌。
Polymeric Micellar Delivery of Novel Microtubule Destabilizer and Hedgehog Signaling Inhibitor for Treating Chemoresistant Prostate Cancer.
机构信息
Department of Pharmaceutical Sciences, College of Pharmacy, University of Nebraska Medical Center, Omaha, Nebraska (R.Y., D.G., Y.D., R.I.M.) and Department of Pharmaceutical Sciences, University of Tennessee Health Science Center, Memphis, Tennessee (H.C., D.D.M., W.L.).
Department of Pharmaceutical Sciences, College of Pharmacy, University of Nebraska Medical Center, Omaha, Nebraska (R.Y., D.G., Y.D., R.I.M.) and Department of Pharmaceutical Sciences, University of Tennessee Health Science Center, Memphis, Tennessee (H.C., D.D.M., W.L.)
出版信息
J Pharmacol Exp Ther. 2019 Sep;370(3):864-875. doi: 10.1124/jpet.119.256628. Epub 2019 Apr 17.
Castration-resistant prostate cancer that has become resistant to docetaxel (DTX) represents one of the greatest clinical challenges in the management of this malignancy. There is an urgent need to develop novel therapeutic agents to overcome chemoresistance and improve the overall survival of patients. We have designed a novel microtubule destabilizer (2-(4-hydroxy-1-indol-3-yl)-1-imidazol-4-yl)(3,4,5-trimethoxyphenyl)methanone (QW-296) and combined it with a newly synthesized hedgehog (Hh) signaling pathway inhibitor 2-chloro- -[4-chloro-3-(2-pyridinyl)phenyl]- , - bis(2-pyridinylmethyl)-1,4-benzenedicarboxamide (MDB5) to treat taxane-resistant (TXR) prostate cancer. The combination of QW-296 and MDB5 exhibited stronger anticancer activity toward DU145-TXR and PC3-TXR cells and suppressed tumor colony formation when compared with single-drug treatment. Because these drugs are hydrophobic, we synthesized the mPEG-p(TMC-MBC) [methoxy-poly(ethylene glycol)--poly(trimethylene carbonate--2-methyl-2-benzoxycarbonyl-propylene carbonate)] copolymer, which could self-assemble into micelles with loading capacities of 8.13% ± 0.75% and 9.12% ± 0.69% for QW-296 and MDB5, respectively. Further, these micelles provided controlled the respective drug release of 58% and 42% release of QW-296 and MDB5 within 24 hours when dialyzed against PBS (pH 7.4). We established an orthotopic prostate tumor in nude mice using stably luciferase expressing PC3-TXR cells. There was maximum tumor growth inhibition in the group treated with the combination therapy of QW-296 and MDB5 in micelles compared with their monotherapies or combination therapy formulated in cosolvent. The overall findings suggest that combination therapy with QW-296 and MDB5 has great clinical potential to treat TXR prostate cancer, and copolymer mPEG-p(TMC-MBC) could serve as an effective delivery vehicle to boost therapeutic efficacy in vivo.
已经对多西紫杉醇(DTX)产生耐药的去势抵抗性前列腺癌是该恶性肿瘤治疗中最大的临床挑战之一。迫切需要开发新的治疗药物来克服化疗耐药性并提高患者的总生存率。我们设计了一种新型微管稳定剂(2-(4-羟基-1-吲哚-3-基)-1-咪唑-4-基)(3,4,5-三甲氧基苯基)甲酮(QW-296),并将其与新合成的 Hedgehog(Hh)信号通路抑制剂 2-氯- -[4-氯-3-(2-吡啶基)苯基],-双(2-吡啶基甲基)-1,4-苯二甲酰胺(MDB5)结合,用于治疗紫杉烷耐药(TXR)前列腺癌。QW-296 和 MDB5 的联合用药对 DU145-TXR 和 PC3-TXR 细胞表现出更强的抗癌活性,并抑制肿瘤集落形成,与单药治疗相比。由于这些药物具有疏水性,我们合成了 mPEG-p(TMC-MBC)[甲氧基-聚(乙二醇)-聚(三亚甲基碳酸酯-2-甲基-2-苯甲氧基羰基-丙碳酸酯)]共聚物,它可以自组装成胶束,载药量分别为 8.13%±0.75%和 9.12%±0.69%的 QW-296 和 MDB5。此外,这些胶束在 PBS(pH7.4)透析时分别提供了 58%和 42%的 QW-296 和 MDB5 的控制药物释放。我们使用稳定表达荧光素酶的 PC3-TXR 细胞在裸鼠中建立了原位前列腺肿瘤。与单药治疗或混合溶剂中的联合治疗相比,QW-296 和 MDB5 联合治疗的组中肿瘤生长抑制最大。总体研究结果表明,QW-296 和 MDB5 的联合治疗具有很大的临床潜力,可以治疗 TXR 前列腺癌,共聚物 mPEG-p(TMC-MBC)可以作为一种有效的递送载体,提高体内治疗效果。
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