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姜黄素及其类似物(PGV - 0和PGV - 1)通过抑制HER2和NF - kB的激活来增强耐药性MCF - 7细胞对阿霉素的敏感性。

Curcumin and its analogues (PGV-0 and PGV-1) enhance sensitivity of resistant MCF-7 cells to doxorubicin through inhibition of HER2 and NF-kB activation.

作者信息

Meiyanto Edy, Putri Dyaningtyas Dewi Pamungkas, Susidarti Ratna Asmah, Murwanti Retno, Fitriasari Aditya, Husnaa Ulfatul, Purnomo Hari, Kawaichi Masashi

机构信息

Cancer Chemoprevention Research Center, Faculty of Pharmacy, Universitas Gadjah Mada, Jalan Sekip Utara Yogyakarta, Japan E-mail :

出版信息

Asian Pac J Cancer Prev. 2014;15(1):179-84. doi: 10.7314/apjcp.2014.15.1.179.

DOI:10.7314/apjcp.2014.15.1.179
PMID:24528023
Abstract

Chemoresistance of breast cancer to doxorubicin is mediated mainly through activation of NF-kB and over expression of HER2. Curcumin and its analogues (PGV-0 and PGV-1) exert cytotoxic effects on T47D breast cancer cells. Suppression of NF-kB activation is suggested to contribute to this activity. The present study aimed to explore the effects of curcumin, PGV-0, and PGV-1 singly and in combination with doxorubicin on MCF-7/Dox cells featuring over-expression of HER2. In MTT assays, curcumin, PGV-0, and PGV-1 showed cytotoxicity effects against MCF-7/Dox with IC50 values of 80 μM, 21 μM, and 82 μM respectively. These compounds increased MCF-7/Dox sensitivity to doxorubicin. Cell cycle distribution analysis exhibited that the combination of curcumin and its analogues with Dox increased sub G-1 cell populations. Curcumin and PGV-1 but not PGV-0 decreased localization of p65 into the nucleus induced by Dox, indicating that activation of NF- kB was inhibited. Molecular docking of curcumin, PGV-0, and PGV-1 demonstrated high affinity to HER2 at ATP binding site. This interaction were directly comparable with those of ATP and lapatinib. These findings suggested that curcumin, PGV-0 and PGV-1 enhance the Dox cytotoxicity to MCF-7 cells through inhibition of HER2 activity and NF-kB activation.

摘要

乳腺癌对阿霉素的化疗耐药主要通过核因子-κB(NF-κB)的激活和人表皮生长因子受体2(HER2)的过表达介导。姜黄素及其类似物(PGV-0和PGV-1)对T47D乳腺癌细胞具有细胞毒性作用。抑制NF-κB激活被认为有助于这种活性。本研究旨在探讨姜黄素、PGV-0和PGV-1单独以及与阿霉素联合对具有HER2过表达的MCF-7/Dox细胞的影响。在MTT试验中,姜黄素、PGV-0和PGV-1对MCF-7/Dox显示出细胞毒性作用,IC50值分别为80μM、21μM和82μM。这些化合物增加了MCF-7/Dox对阿霉素的敏感性。细胞周期分布分析表明,姜黄素及其类似物与阿霉素联合增加了亚G-1期细胞群体。姜黄素和PGV-1而非PGV-0降低了阿霉素诱导的p65核定位,表明NF-κB的激活受到抑制。姜黄素、PGV-0和PGV-1的分子对接显示在ATP结合位点对HER2具有高亲和力。这种相互作用与ATP和拉帕替尼的相互作用直接相当。这些发现表明,姜黄素、PGV-0和PGV-1通过抑制HER2活性和NF-κB激活增强了阿霉素对MCF-7细胞的细胞毒性。

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