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首页> 外文期刊>Journal of Cancer Research and Clinical Oncology >Vitamin K(2) selectively induced apoptosis in ovarian TYK-nu and pancreatic MIA PaCa-2 cells out of eight solid tumor cell lines through a mechanism different from geranylgeraniol.
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Vitamin K(2) selectively induced apoptosis in ovarian TYK-nu and pancreatic MIA PaCa-2 cells out of eight solid tumor cell lines through a mechanism different from geranylgeraniol.

机译:维生素K(2)通过不同于香叶基香叶醇的机制选择性诱导八种实体肿瘤细胞系中的卵巢TYK-nu和胰腺MIA PaCa-2细胞凋亡。

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PURPOSE. In this study, we examined the effects of vitamin K(2) (menaquinone 4), which has a geranylgeranyl side chain, on various lines of cells derived from human solid tumors and compared them with the effects of geranylgeraniol (GGO). METHODS. Cell proliferation was determined with 3'-[1-[(phenylamino)carbonyl]-3,4-tetrazolium- bis (4-methoxy-6-nitro) benzene-sulfonic acid hydrate (XTT), and the induction of apoptosis was analyzed by TUNEL staining and flow cytometry as well as by measurement of DNA fragmentation, released nucleosomes and caspase-3 activity. Levels of Bcl-2, Bax and cytochrome c were determined by immunoblotting. RESULTS. GGO inhibited the growth of all eight cell lines derived from solid tumors, while vitamin K(2) selectively inhibited the proliferation of ovarian TYK-nu and pancreatic MIA PaCa-2 cancer cells, inducing apoptosis in both cell lines. Far more time was required for the induction of apoptosis in these two cell lines by vitamin K(2) than by GGO. Apoptotic signals induced in TYK-nu cells during the first 2 days that followed the addition of vitamin K(2) to the culture medium were reversible, but these signals became irreversible after 3 days of treatment with vitamin K(2). The induction of apoptosis in TYK-nu cells by vitamin K(2) was inhibited by cycloheximide and also by starvation at a low concentration of serum. Neither cycloheximide nor starvation had any effect on the induction of apoptosis by GGO. Cytochrome c was released simultaneously with the initiation of apoptosis on treatment of TYK-nu cells with vitamin K(2) or GGO. However, GGO induced the release of cytochrome c from isolated mitochondria, while vitamin K(2) did not. The amount of Bcl-2 in TYK-nu cells was reduced by vitamin K(2), but not by GGO. CONCLUSIONS. In contrast to GGO, vitamin K(2) induced apoptosis selectively in pancreatic MIA-PaCa 2 and ovarian TYK-nu cancer cells. It is suggested that de novo protein synthesis might be necessary for induction of apoptosis by vitamin K(2) but not by GGO, and thus, that vitamin K(2) and GGO might induce apoptosis by different mechanisms.
机译:目的。在这项研究中,我们检查了具有香叶基香叶基侧链的维生素K(2)(甲萘醌4)对源自人类实体瘤的各种细胞系的影响,并将它们与香叶基香叶醇(GGO)的作用进行了比较。方法。用3'-[1-[([苯基氨基)羰基] -3,4-四唑-双(4-甲氧基-6-硝基)苯磺酸水合物(XTT)测定细胞增殖,并分析其凋亡诱导通过TUNEL染色和流式细胞术以及通过测量DNA片段,释放核小体和caspase-3活性。通过免疫印迹测定Bcl-2,Bax和细胞色素c的水平。结果。 GGO抑制了来自实体瘤的所有8种细胞系的生长,而维生素K(2)选择性抑制了卵巢TYK-nu和胰腺MIA PaCa-2癌细胞的增殖,诱导了这两种细胞系的凋亡。与GGO相比,维生素K(2)诱导这两个细胞系凋亡的时间要长得多。在向培养基中添加维生素K(2)之后的前2天,在TYK-nu细胞中诱导的凋亡信号是可逆的,但是在用维生素K(2)处理3天后,这些信号变得不可逆。维生素K(2)诱导的TYK-nu细胞凋亡被环己酰亚胺抑制,也被低浓度血清饥饿所抑制。环己酰亚胺和饥饿均未对GGO诱导的细胞凋亡产生任何影响。在用维生素K(2)或GGO处理TYK-nu细胞时,细胞色素c的释放与细胞凋亡的启动同时开始。但是,GGO诱导从孤立的线粒体中释放细胞色素c,而维生素K(2)没有。维生素K(2)减少了TYK-nu细胞中Bcl-2的含量,但GGO却没有。结论。与GGO相反,维生素K(2)在胰腺MIA-PaCa 2和卵巢TYK-nu癌细胞中选择性诱导凋亡。提示从头合成蛋白质可能是维生素K(2)诱导凋亡所必需的,而不是GGO诱导的,因此,维生素K(2)和GGO可能通过不同的机制诱导凋亡。

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