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盐酸拓扑替康脂质体包封于热敏水凝胶中用于昆明小鼠H22肿瘤的持续高效原位治疗

Topotecan hydrochloride liposomes incorporated into thermosensitive hydrogel for sustained and efficient in situ therapy of H22 tumor in Kunming mice.

作者信息

Xing Jiayu, Qi Xiaole, Jiang Yingchun, Zhu Xuehua, Zhang Ziwei, Qin Xiaoxue, Wu Zhenghong

机构信息

a Key Laboratory of Modern Chinese Medicines , China Pharmaceutical University , Nanjing , PR China , and.

b Yangtze River Pharmaceutical Group , State Key Laboratory for Advanced Formulation Technologies , Taizhou , China.

出版信息

Pharm Dev Technol. 2015 Nov;20(7):812-819. doi: 10.3109/10837450.2014.926918. Epub 2014 Jun 9.

DOI:10.3109/10837450.2014.926918
PMID:24909735
Abstract

Topotecan hydrochloride (TPT) has potential for the treatment of ovarian cancer, but the activity of TPT tends to decrease due to the ring-opening at physiological pH. In this study, we proposed to incorporate TPT liposomes into injectable thermosensitive in situ hydrogel, consisting of chitosan (CS) and β-glycerophosphate (β-GP), for sustained release and preservation of active lactone form of TPT. The rheology studies were carried out to investigate the sol-gel temperature, flow behavior and viscosity of these CS/β-GP systems. The optimized formulation exhibited sol-gel transition at 40.2 ± 0.4 °C, with pseudoplastic flow behavior. The drug release rate of TPT liposomes loaded CS/β-GP hydrogel in phosphate buffer saline (pH = 7.4) was found to be slowed down, and the lactone fraction of TPT in the hydrogel matrix was maintaining 40% after 50 h. In addition, the antitumor efficacy in Kunming mice bearing Hepatoma-22 tumor, after intratumoral injection of TPT liposomes loaded CS/β-GP hydrogel, was higher than that of TPT in saline and TPT in CS/β-GP hydrogel. Those results demonstrated that TPT liposomes loaded CS/β-GP hydrogel could become a potential formulation for improving the antitumor efficacy of TPT and suggested an important technology platform for intratumoral administration of derivative of camptothecin-family drugs.

摘要

盐酸拓扑替康(TPT)具有治疗卵巢癌的潜力,但由于其在生理pH值下会开环,TPT的活性往往会降低。在本研究中,我们建议将TPT脂质体纳入由壳聚糖(CS)和β-甘油磷酸酯(β-GP)组成的可注射热敏原位水凝胶中,以实现TPT活性内酯形式的持续释放和保存。进行了流变学研究,以考察这些CS/β-GP体系的溶胶-凝胶温度、流动行为和粘度。优化后的制剂在40.2±0.4°C表现出溶胶-凝胶转变,具有假塑性流动行为。发现载有TPT脂质体的CS/β-GP水凝胶在磷酸盐缓冲盐水(pH = 7.4)中的药物释放速率减慢,水凝胶基质中TPT的内酯分数在50小时后维持在40%。此外,在昆明荷Hepatoma-22肿瘤小鼠中,瘤内注射载有TPT脂质体的CS/β-GP水凝胶后的抗肿瘤疗效高于TPT生理盐水溶液和TPT CS/β-GP水凝胶。这些结果表明,载有TPT脂质体的CS/β-GP水凝胶可能成为提高TPT抗肿瘤疗效的潜在制剂,并为喜树碱类药物衍生物的瘤内给药提供了一个重要的技术平台。

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