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二烯丙基三硫化物通过减弱Nrf2/Akt信号通路、激活p38/JNK信号通路来抑制肿瘤生长,并增强顺铂在胃癌治疗中的疗效。

Diallyl trisulfide suppresses tumor growth through the attenuation of Nrf2/Akt and activation of p38/JNK and potentiates cisplatin efficacy in gastric cancer treatment.

作者信息

Jiang Xiao-Yan, Zhu Xiao-Song, Xu Hong-Ya, Zhao Zhong-Xi, Li Si-Ying, Li Shan-Zhong, Cai Jian-Hua, Cao Ji-Min

机构信息

School of Pharmaceutical Sciences, Shandong University, Ji-nan 250012, China.

Shandong Provincial Key Laboratory of Mucosal and Transdermal Drug Delivery Technologies, Shandong Academy of Pharmaceutical Sciences, Ji-nan 250101, China.

出版信息

Acta Pharmacol Sin. 2017 Jul;38(7):1048-1058. doi: 10.1038/aps.2016.176. Epub 2017 Mar 27.

DOI:10.1038/aps.2016.176
PMID:28344324
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5519247/
Abstract

Diallyl trisulfide (DATS), a garlic organosulfide, has shown excellent chemopreventive potential. Cisplatin (DDP) is widely used to treat solid malignant tumors, but causing serious side effects. In the current study, we attempted to elucidate the chemopreventive mechanisms of DATS in human gastric cancer BGC-823 cells in vitro, and to investigate whether DATS could enhance the anti-tumor efficacy of DDP and improve quality of life in BGC-823 xenograft mice in vivo. Treatment with DATS (25-400 μmol/L) dose-dependently inhibited the viability of BGC-823 cells in vitro with an IC of 115.2±4.3 μmol/L after 24 h drug exposure. DATS (50-200 μmol/L) induced cell cycle arrest at G/M phase in BGC-823 cells, which correlated with significant accumulation of cyclin A2 and B1. DATS also induced BGC-823 cell apoptosis, which was accompanied by the modulation of Bcl-2 family members and caspase cascade activation. In BGC-823 xenograft mice, administration of DATS (20-40 mg·kg·d, ip) dose-dependently inhibited tumor growth and markedly reduced the number of Ki-67 positive cells in tumors. Interestingly, combined administration of DATS (30 mg·kg·d, ip) with DDP (5 mg/kg, every 5 d, ip) exhibited enhanced anti-tumor activity with fewer side effects. We showed that treatment of BGC-823 cells with DATS in vitro and in vivo significantly activated kinases such as p38 and JNK/MAPK and attenuated the Nrf2/Akt pathway. This study provides evidence that DATS exerts anticancer effects and enhances the antitumor efficacy of DDP, making it a novel candidate for adjuvant therapy for gastric cancer.

摘要

二烯丙基三硫化物(DATS)是一种大蒜有机硫化物,已显示出优异的化学预防潜力。顺铂(DDP)广泛用于治疗实体恶性肿瘤,但会引起严重的副作用。在当前研究中,我们试图阐明DATS在体外对人胃癌BGC-823细胞的化学预防机制,并研究DATS是否能增强DDP的抗肿瘤疗效并改善BGC-823异种移植小鼠体内的生活质量。用DATS(25 - 400μmol/L)处理在体外剂量依赖性地抑制BGC-823细胞的活力,药物暴露24小时后IC为115.2±4.3μmol/L。DATS(50 - 200μmol/L)诱导BGC-823细胞在G/M期发生细胞周期阻滞,这与细胞周期蛋白A2和B1的显著积累相关。DATS还诱导BGC-823细胞凋亡,这伴随着Bcl-2家族成员的调节和半胱天冬酶级联激活。在BGC-823异种移植小鼠中,给予DATS(20 - 40mg·kg·d,腹腔注射)剂量依赖性地抑制肿瘤生长,并显著减少肿瘤中Ki-67阳性细胞的数量。有趣的是,DATS(30mg·kg·d,腹腔注射)与DDP(5mg/kg,每5天,腹腔注射)联合给药表现出增强的抗肿瘤活性且副作用更少。我们表明,在体外和体内用DATS处理BGC-823细胞可显著激活诸如p38和JNK/MAPK等激酶,并减弱Nrf2/Akt途径。本研究提供了证据表明DATS发挥抗癌作用并增强DDP的抗肿瘤疗效,使其成为胃癌辅助治疗的新候选药物。

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