用于治疗肾透明细胞癌的塔卡醇内酯 AJ-羟丙基-β-环糊精包合物的研制。
Development of Taccalonolide AJ-Hydroxypropyl-β-Cyclodextrin Inclusion Complexes for Treatment of Clear Cell Renal-Cell Carcinoma.
机构信息
Jiangsu Key Laboratory for Functional Substance of Chinese Medicine, Jiangsu Collaborative Innovation Center of Chinese Medicinal Resources Industrialization, State Key Laboratory Cultivation Base for TCM Quality and Efficacy, Jiangsu Key Laboratory for Pharmacology and Safety Evaluation of Chinese Materia Medical, Nanjing University of Chinese Medicine, Nanjing 210023, China.
State Key Laboratory of Drug Research, Shanghai Institute of Material Medical, Chinese Academy of Sciences, 501 Haike Road, Shanghai 201203, China.
出版信息
Molecules. 2020 Nov 27;25(23):5586. doi: 10.3390/molecules25235586.
BACKGROUND
Microtubule-targeted drugs are the most effective drugs for adult patients with certain solid tumors. Taccalonolide AJ (AJ) can stabilize tubulin polymerization by covalently binding to β-tubulin, which enables it to play a role in the treatment of tumors. However, its clinical applications are largely limited by low water solubility, chemical instability in water, and a narrow therapeutic window. Clear-cell renal-cell carcinoma (cc RCC) accounts for approximately 70% of RCC cases and is prone to resistance to particularly targeted therapy drugs.
METHODS
we prepared a water-soluble cyclodextrin-based carrier to serve as an effective treatment for cc RCC.
RESULTS
Compared with AJ, taccalonolide AJ-hydroxypropyl-β-cyclodextrin (AJ-HP-β-CD) exhibited superior selectivity and activity toward the cc RCC cell line 786-O vs. normal kidney cells by inducing apoptosis and cell cycle arrest and inhibiting migration and invasion of tumor cells . According to acute toxicity testing, the maximum tolerated dose (MTD) of AJ-HP-β-CD was 10.71 mg/kg, which was 20 times greater than that of AJ. Assessment of weight changes showed that mouse body weight recovered over 7-8 days, and the toxicity could be greatly reduced by adjusting the injections from once every three days to once per week. In addition, we inoculated 786-O cells to generate xenografted mice to evaluate the anti-tumor activity of AJ-HP-β-CD in vivo and found that AJ-HP-β-CD had a better tumor inhibitory effect than that of docetaxel and sunitinib in terms of tumor growth and endpoint tumor weight. These results indicated that cyclodextrin inclusion greatly increased the anti-tumor therapeutic window of AJ.
CONCLUSIONS
the AJ-HP-β-CD complex developed in this study may prove to be a novel tubulin stabilizer for the treatment of cc RCC. In addition, this drug delivery system may broaden the horizon in the translational study of other chemotherapeutic drugs.
背景
微管靶向药物是治疗某些成人实体瘤最有效的药物。Taccalonolide AJ(AJ)可以通过与β-微管蛋白共价结合稳定微管蛋白聚合,从而发挥治疗肿瘤的作用。然而,其临床应用在很大程度上受到低水溶性、水中化学不稳定性和治疗窗口窄的限制。透明细胞肾细胞癌(cc RCC)约占 RCC 病例的 70%,容易对特别靶向治疗药物产生耐药性。
方法
我们制备了一种水溶性环糊精载体,作为治疗 cc RCC 的有效药物。
结果
与 AJ 相比,taccalonolide AJ-羟丙基-β-环糊精(AJ-HP-β-CD)通过诱导细胞凋亡和细胞周期阻滞,抑制肿瘤细胞的迁移和侵袭,对 cc RCC 细胞系 786-O 表现出优于正常肾细胞的选择性和活性。根据急性毒性试验,AJ-HP-β-CD 的最大耐受剂量(MTD)为 10.71mg/kg,是 AJ 的 20 倍。体重变化评估表明,小鼠体重在 7-8 天内恢复,通过将注射频率从每三天一次调整为每周一次,可以大大降低毒性。此外,我们接种 786-O 细胞生成异种移植小鼠,以评估 AJ-HP-β-CD 在体内的抗肿瘤活性,发现 AJ-HP-β-CD 在肿瘤生长和终点肿瘤重量方面比多西他赛和舒尼替尼具有更好的肿瘤抑制作用。这些结果表明,环糊精包合大大增加了 AJ 的抗肿瘤治疗窗口。
结论
本研究开发的 AJ-HP-β-CD 复合物可能成为治疗 cc RCC 的新型微管稳定剂。此外,该药物递送系统可能会拓宽其他化疗药物转化研究的视野。
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