与HIV蛋白酶抑制剂奈非那韦联合治疗可显著增加耐药KBV20C癌细胞的晚期凋亡，且与P-糖蛋白抑制无关。

Co-treatment With HIV Protease Inhibitor Nelfinavir Greatly Increases Late-phase Apoptosis of Drug-resistant KBV20C Cancer Cells Independently of P-Glycoprotein Inhibition.

作者信息

Kim Ji Yeong, Park Yoo Jung, Lee Byung-Mu, Yoon Sungpil

机构信息

School of Pharmacy, Sungkyunkwan University, Suwon, Republic of Korea.

School of Pharmacy, Sungkyunkwan University, Suwon, Republic of Korea

出版信息

Anticancer Res. 2019 Jul;39(7):3757-3765. doi: 10.21873/anticanres.13524.

DOI:10.21873/anticanres.13524

PMID:31262902

Abstract

BACKGROUND/AIM: The study focused on identifying the mechanisms or drugs that might sensitize resistant KBV20C human oral squamous carcinoma cells overexpressing P-glycoprotein (P-gp) to antimitotic drug treatment.

MATERIALS AND METHODS

Five HIV protease inhibitors (atazanavir, nelfinavir, darunavir, lopinavir, and ritonavir) were tested to identify drugs that could be used at a relatively low dose for sensitizing antimitotic drug-resistant KBV20C cells. Fluorescence-activated cell sorting, annexin V analyses, and rhodamine uptake tests were performed to further investigate the mechanism of action.

RESULTS

Co-treatment with nelfinavir or lopinavir had a high sensitizing effect on vincristine-treated KBV20C cells. Nelfinavir and lopinavir reduced cell viability, increased G phase arrest, and up-regulated apoptosis when used as a co-treatment with vincristine. We also demonstrated that eribulin co-treatment with nelfinavir and lopinavir similarly increased sensitization of KBV20C cells. Only lopinavir was found to have a high P-gp-inhibitory activity (similar to verapamil). Interestingly, nelfinavir had very low P-gp-inhibitory activity, suggesting that vincristine-nelfinavir sensitization is independent of the P-gp-inhibitory effect of nelfinavir. We also demonstrated this same combination mainly caused sensitization due to late apoptosis in P-gp-overexpressing drug-resistant KBV20C cells.

CONCLUSION

Highly antimitotic drug-resistant KBV20C cells can be sensitized by co-treatment with the repositioned HIV protease inhibitors nelfinavir and lopinavir. In particular, the sensitizing effect of co-treatment with nelfinavir on antimitotic drug-resistant cancer cells was found to be strong and independent of P-gp-inhibitory activity. As P-gp inhibition can be toxic to normal cells, selecting nelfinavir may be safer for normal cells in patients with drug-resistant cancer.

摘要

背景/目的：本研究聚焦于确定可能使过表达P-糖蛋白（P-gp）的耐药KBV20C人口腔鳞状癌细胞对抗有丝分裂药物治疗敏感的机制或药物。

材料与方法

测试了五种HIV蛋白酶抑制剂（阿扎那韦、奈非那韦、达芦那韦、洛匹那韦和利托那韦），以确定可在相对低剂量下用于使抗有丝分裂药物耐药的KBV20C细胞敏感的药物。进行了荧光激活细胞分选、膜联蛋白V分析和罗丹明摄取试验，以进一步研究作用机制。

结果

奈非那韦或洛匹那韦与长春新碱联合处理对KBV20C细胞有高度的增敏作用。奈非那韦和洛匹那韦与长春新碱联合使用时，可降低细胞活力，增加G期阻滞，并上调细胞凋亡。我们还证明，艾日布林与奈非那韦和洛匹那韦联合处理同样增加了KBV20C细胞的敏感性。仅发现洛匹那韦具有较高的P-gp抑制活性（类似于维拉帕米）。有趣的是，奈非那韦的P-gp抑制活性非常低，这表明长春新碱-奈非那韦增敏作用独立于奈非那韦的P-gp抑制作用。我们还证明，这种相同的联合处理主要是由于过表达P-gp的耐药KBV20C细胞中晚期凋亡导致的增敏作用。