The p53 pathway is synergized by p38 mapk signaling to mediate 11,11 '-dideoxyverticillin-induced g(2)/m arrest | |
Chen, Y; Miao, ZH; Zhao, WM; Ding, J | |
刊名 | Febs letters |
2005-07-04 | |
卷号 | 579期号:17页码:3683-3690 |
关键词 | 11,11 '-dideoxyverticillin G(2)/m arrest P53 P38 mapk Chk2 Anti-tumor Hct-116 cell |
ISSN号 | 0014-5793 |
DOI | 10.1016/j.febslet.2005.05.053 |
通讯作者 | Ding, j() |
英文摘要 | The phytochemical 11,11'-dideoxyverticillin, derived from the fungus shiraia bambusicola, has been shown to possess potent anticancer activity in vitro and in vivo. here, we investigated the effect of 11,11'-dideoxyverticillin on cell cycle progression, and explored the potential mechanisms for this effect. a concentration- and time-dependent cell cycle blockade at g(2)/m phase was observed in human colon cancer cells (hct-116) following 11,11'-dideoxyverticillin treatment and was associated with marked increases in levels of p53, phospho-p53(ser20) and phospho-chk2(thr 68). when wild type p53 expression was specifically inhibited by rna interference, hct-116 cells treated with 11,11'-dideoxyverticillin failed to arrest in g2/m and did not show increased phospho-chk2(thr 68). on the other hand, 11,11'-dideoxyverticillin treatment also elicited p38 map kinase activity and expression of phospho-p38 mapk. treatment with a specific p38 mapk inhibitor (sb203580) successfully inhibited p38 mapk and delayed the onset of g2/m arrest induced by 0.5 mu m 11,11'-dideoxyverticillin after approximately 6h, but did not abolish the induction of g2/m arrest. additionally, sb203580 did not alter the levels of p53, phospho-p53 (ser20), or phospho-chk2 (thr68) proteins in 11,11'-dideoxyverticillin-treated cells. together, these findings indicate that p53-mediated phosphorylation of chk2 maybe plays a vital role in 11, 11-dideoxyverticillin-induced g arrest, and that p38 mapk might accelerate this progression. our work suggests a new possibility of interactions among p53, chk2 and p38 mapk signaling in g(2)/m arrest. (c) 2005 federation of european biochemical societies. published by elsevier b.v. all rights reserved. |
WOS关键词 | CELL-CYCLE CHECKPOINTS ; DNA-DAMAGE CHECKPOINT ; INDUCED PHOSPHORYLATION ; PROTEIN-KINASE ; RADIATION ; CHK2 ; ACTIVATION ; GROWTH ; CANCER ; G(1) |
WOS研究方向 | Biochemistry & Molecular Biology ; Biophysics ; Cell Biology |
WOS类目 | Biochemistry & Molecular Biology ; Biophysics ; Cell Biology |
语种 | 英语 |
出版者 | ELSEVIER SCIENCE BV |
WOS记录号 | WOS:000230335600034 |
内容类型 | 期刊论文 |
URI标识 | http://www.corc.org.cn/handle/1471x/2377289 |
专题 | 中国科学院大学 |
通讯作者 | Ding, J |
作者单位 | 1.Chinese Acad Sci, Shanghai Inst Biol Sci, Shanghai Inst Mat Med, Div Anti Tumor Pharmacol,State Key Lab Drug Res, Shanghai, Peoples R China 2.Chinese Acad Sci, Shanghai Inst Biol Sci, Shanghai Inst Mat Med, Dept Phytochem, Shanghai, Peoples R China 3.Chinese Acad Sci, Grad Sch, Shanghai, Peoples R China |
推荐引用方式 GB/T 7714 | Chen, Y,Miao, ZH,Zhao, WM,et al. The p53 pathway is synergized by p38 mapk signaling to mediate 11,11 '-dideoxyverticillin-induced g(2)/m arrest[J]. Febs letters,2005,579(17):3683-3690. |
APA | Chen, Y,Miao, ZH,Zhao, WM,&Ding, J.(2005).The p53 pathway is synergized by p38 mapk signaling to mediate 11,11 '-dideoxyverticillin-induced g(2)/m arrest.Febs letters,579(17),3683-3690. |
MLA | Chen, Y,et al."The p53 pathway is synergized by p38 mapk signaling to mediate 11,11 '-dideoxyverticillin-induced g(2)/m arrest".Febs letters 579.17(2005):3683-3690. |
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