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SarCNU-induced G2/M arrest in hepatoma cells is mediated by a p53-independent phosphorylation of cdc-2 at Tyr15

✍ Scribed by Huynh Hung; Chow Kad Hoe Pierce; Soo Khee Chee; Panasci Lawrence; Nguyen Thanh Hung

Book ID
102314104
Publisher
John Wiley and Sons
Year
2005
Tongue
English
Weight
341 KB
Volume
204
Category
Article
ISSN
0021-9541

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✦ Synopsis

Abstract

Hepatocellular carcinoma (HCC) is a major health problem in the Asia‐Pacific region, with high incidence and mortality rate. There is currently no effective treatment for inoperable cases that represent the vast majority of patients. In the present study, we report that in vitro treatment of primary hepatoma, HepG2 (wild‐type p53), PLC/PRF/5 (p53‐mutant), and Hep3B (p53‐deleted) cells with 2‐chloroethyl‐3‐sarcosinamide‐1‐nitrosourea (SarCNU) resulted in upregulation of p53, p21^Cip1/Waf1^, phosphorylated cdc‐2 at Tyr15 in wild‐type p53 cells and phosphorylation of cdc‐2 at Tyr15 in p53‐mutant or p53‐deleted hepatoma cells. This was accompanied by the reduction in cdc‐2 kinase activity and G~2~/M cell cycle arrest. These findings indicate that SarCNU‐induced G~2~/M growth arrest in hepatoma cells by a p53‐independent phosphorylation of cdc‐2. Our data suggest the potential use of SarCNU in treatment of HCC. © 2005 Wiley‐ Liss, Inc.

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