幽门螺杆菌诱导的凋亡和抗凋亡信号通路分析
Analysis of apoptotic and antiapoptotic signalling pathways induced by Helicobacter pylori.
作者信息
Maeda S, Yoshida H, Mitsuno Y, Hirata Y, Ogura K, Shiratori Y, Omata M
机构信息
Department of Gastroenterology, University of Tokyo, 7-3-1 Hongo, Bunkyo-ku, Tokyo 113-8655, Japan.
出版信息
Gut. 2002 Jun;50(6):771-8. doi: 10.1136/gut.50.6.771.
BACKGROUND AND AIMS
Although it is reported that Helicobacter pylori induces apoptosis on gastric epithelial cells, the mechanism remains unknown. Antiapoptotic effects generated by H pylori have not yet been evaluated.
METHODS
(1) H pylori strains (type 1 wild, TN2-DeltacagE, TN2-DeltavacA) were cocultured with MKN45, TMK1, and HeLa cells, and cell viability and apoptosis were assessed by trypan blue exclusion and DNA laddering, respectively. (2) Activation of caspases-3, 7, and 8, cytochrome c release from the mitochondria, and Fas, Fas associated death domain protein (FADD), Bax, Bak, and Bcl-X expression were evaluated by immunoblot analysis. (3) To investigate whether nuclear factor kappa B (NFkappaB) activation induced by cag pathogenicity island (PAI) positive H pylori affects antiapoptosis, MKN45 cells stably expressing super-repressor Ikappabetaalpha were cocultured with H pylori, and cell viability and caspase activation were evaluated. NFkappaB regulated gene expression was also evaluated by ribonuclease protection assay.
RESULTS
(1) Wild-type and DeltavacA mutant H pylori induced apoptosis more potently than the DeltacagE mutant. Inhibition of cell contact between H pylori and cancer cells and heat killing H pylori diminished cell death. (2) Caspases-3, 7, and 8 were activated time dependently by H pylori as well as by the agonist anti-Fas. Cytochrome c release from mitochondria was observed and was not inhibited by caspase-8 inhibitor. Although protein expression of Fas, FADD, Bax, Bak, and Bcl-X in the whole cell lysates was not changed by H pylori, Bax was decreased from mitochondria free cytosol suggesting that Bax was translocated into mitochondria. (3) Cell death and the activities of caspases-3 and 8 were promoted in MKN45 cells stably expressing super-repressor Ikappabetaalpha that inhibits NFkappaB activation. Antiapoptotic proteins c-IAP1 and c-IAP2 were upregulated by the wild-type strains.
CONCLUSION
cag PAI positive H pylori is capable of inducing apoptotic effects mainly through the mitochondrial pathway. Antiapoptotic effects mediated by NFkappaB activation were also observed.
背景与目的
尽管有报道称幽门螺杆菌可诱导胃上皮细胞凋亡,但其机制仍不清楚。幽门螺杆菌产生的抗凋亡作用尚未得到评估。
方法
(1)将幽门螺杆菌菌株(1型野生株、TN2 - DeltacagE、TN2 - DeltavacA)与MKN45、TMK1和HeLa细胞共培养,分别通过台盼蓝排斥试验和DNA梯状条带分析评估细胞活力和凋亡情况。(2)通过免疫印迹分析评估半胱天冬酶 - 3、7和8的激活、细胞色素c从线粒体的释放以及Fas、Fas相关死亡结构域蛋白(FADD)、Bax、Bak和Bcl - X的表达。(3)为研究cag致病岛(PAI)阳性幽门螺杆菌诱导的核因子κB(NFκB)激活是否影响抗凋亡作用,将稳定表达超抑制因子IkappaBβα的MKN45细胞与幽门螺杆菌共培养,并评估细胞活力和半胱天冬酶激活情况。还通过核糖核酸酶保护试验评估NFκB调节的基因表达。
结果
(1)野生型和DeltavacA突变型幽门螺杆菌比DeltacagE突变型更有效地诱导凋亡。抑制幽门螺杆菌与癌细胞之间的细胞接触以及热灭活幽门螺杆菌可减少细胞死亡。(a)幽门螺杆菌以及激动剂抗Fas可时间依赖性地激活半胱天冬酶 - 3、7和8。观察到细胞色素c从线粒体释放,且未被半胱天冬酶 - 8抑制剂抑制。尽管幽门螺杆菌未改变全细胞裂解物中Fas、FADD、Bax、Bak和Bcl - X的蛋白表达,但Bax从无线粒体的胞质溶胶中减少,提示Bax易位至线粒体。(3)在稳定表达抑制NFκB激活的超抑制因子IkappaBβα的MKN45细胞中,细胞死亡以及半胱天冬酶 - 3和8的活性增强。野生型菌株上调抗凋亡蛋白c - IAP1和c - IAP2。
结论
cag PAI阳性幽门螺杆菌主要通过线粒体途径诱导凋亡作用。还观察到由NFκB激活介导的抗凋亡作用。
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