Trichostatin A Inhibits Proliferation and Induces Expression of p21WAF and p27 in Human Brain Tumor Cell Lines
10.3321/j.issn:1000-467X.2002.10.014
- VernacularTitle:曲古抑菌素A抑制人脑肿瘤细胞增殖及提高p21和p27蛋白表达
- Author:
Zhi-Min WANG
1
;
Jin HU
;
Dai ZHOU
;
Zhi-Yuan XU
;
C.Panasci LAWRENCE
;
Zhong-Ping CHEN
Author Information
1. the First Affiliated Hospital Suzhou University
- Keywords:
Brain tumor;
Histone deacetylase inhibitor;
p21;
p27
- From:Chinese Journal of Cancer
2002;21(10):1100-1105
- CountryChina
- Language:Chinese
-
Abstract:
Background and Objective: The histone deacetylase inhibitor,trichostatin A(TSA),was shown to induce apoptosis in transformed cells at submicromolar concentrations. However, the effect of TSA on brain tumor cells is still unknown. This study was designed to investigate whether TSA posses antitumor activity and if any, its mechanism. Materials and Methods: A p53 mutant human glioma cell line T98G and a p53 wild type human neuroblastoma cell line SKNSH were exposed to TSA. Cell proliferation was assessed by sulforhodamine B (SRB) cytotoxicity assay. Apoptosis was quantified by flow cytometry and confirmed by apoptotic ladder formation. Expression patterns of accumulation of highly acetylated histone H3,H4; p53 and cell cycle-associated p21waf,p27 which were induced by TSA were determined by using Western blot analysis. Results: TSA inhibited the proliferation of brain tumor cell lines at nanomolar concentrations and induced accumulation of highly acetylased histone moleculars. Treatment with TSA at 0.33μ M for 24h significantly induced cell apoptosis.In addition to the suppression of cell growth, the up regulation of p21waf and p27 expression was observed within 48h after the treatment.p21 protein levels were increased at early time points and reached maximal levels at 8h, while p27 protein levels were increased after 8h. However, there was no significant changes of acetylased p53 and endogenous p53 protein levels were observed. Conclusion:TSA may inhibit brain tumor cell growth in vitro, which is otherwise particularly resistant to chemotherapy. TSA acts as an anti-tumor agent could be through co-operation between p21 and p27 in growth inhibition, irrespective of endogenous p53 status.
