Resveratrol analog, 3,4,5,4'-tetrahydroxystilbene, differentially induces pro-apoptotic p53/Bax gene expression and inhibits the growth of transformed cells but not their normal counterparts

doi:10.1093/carcin/22.2.321

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Carcinogenesis, Vol. 22, No. 2, 321-328, February 2001
© 2001 Oxford University Press

MOLECULAR EPIDEMIOLOGY AND CANCER PREVENTION

Resveratrol analog, 3,4,5,4'-tetrahydroxystilbene, differentially induces pro-apoptotic p53/Bax gene expression and inhibits the growth of transformed cells but not their normal counterparts

Jiebo Lu, Chi-Tang Ho, Geetha Ghai and Kuang Yu Chen^,^,^,

¹ Department of Chemistry,
² Center for Advanced Food Technology, Rutgers, The State University of New Jersey, Piscataway, NJ 08854-8087, USA and
³ New Jersey Cancer Institute, New Brunswick, NJ 08901, USA

Resveratrol, a trihydroxystilbene found in grapes and otherplants, has been shown to be active in inhibiting multistagecarcinogenesis. Using resveratrol as a prototype, we have synthesizeda number of polyhydroxy- and polymethoxy-stilbenes and testedtheir anti-proliferative effect in normal and transformed humancells. Here we show that one of the resveratrol analogs, 3,4,5,4'-tetrahydroxystilbene(R-4), specifically inhibited the growth of SV40 virally transformedWI38 cells (WI38VA) at 10 µM, but had no effect on normalWI38 cells at even higher concentrations. R-4 also prominentlyinduced apoptosis in WI38VA cells, but not in WI38 cells. RNaseprotection assay showed that R-4 significantly induced the expressionof p53, GADD45 and Bax genes and concomitantly suppressed theexpression of bcl-2 gene in WI38VA, but not in WI38 cells. Alarge increase in p53 DNA binding activity and the presenceof p53 in the Bax promoter binding complex suggested that p53was responsible for the Bax gene expression induced by R-4 intransformed cells. Within 4 h of treatment with R-4, the Baxto bcl-2 protein ratio in WI38 and WI38VA cells was, respectively,0.1 and 105, a difference of three orders of magnitude. WhileR-4 prominently induced the p53/Bax pro-apoptotic genes, italso concomitantly suppressed the expression of Cox-2 in WI38VAcells. Taken together, our study suggests that the inductionof p53 gene by R-4 in transformed cells may play a key rolein the differential growth inhibition and apoptosis of transformedcells.

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