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Flavaglines: A group of efficient growth inhibitors block cell cycle progression and induce apoptosis in colorectal cancer cells

โœ Scribed by Barbara Hausott; Harald Greger; Brigitte Marian


Publisher
John Wiley and Sons
Year
2004
Tongue
French
Weight
469 KB
Volume
109
Category
Article
ISSN
0020-7136

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โœฆ Synopsis


Abstract

Flavaglines are flavonolโ€“cinnamateโ€derived cyclopenta[b]benzofurans, so far reported only for the genus Aglaia of the plant family Meliaceae. They represent a group of highly bioactive metabolites already known for their strong antileukemic activities. To assess their suitability as chemotherapeutic drugs in colorectal cancer, their cytostatic effects and the underlying mechanisms of action were analyzed in colorectal tumor cell lines. Aglaiastatin was the most active flavagline, inhibiting growth and inducing apoptosis at nanomolar concentrations in SW480 and HT29/HI1 carcinoma cells, while the premalignant adenoma cell lines VACO235 and LT97 as well as the normal intestinal epithelial cell line IEC18 were 1,000 times less sensitive (IC~50~ > 10 ฮผM). In SW480 cells, aglaiastatin caused cell cycle block in early mitosis, demonstrated by a shift of cell cycle distribution 24 and 48 hr after addition of aglaiastatin and by an increased content of cyclin B after 6 hr together with a decreased level of cyclin A as early as 2 hr after exposure. In addition, induction of apoptosis could be shown by the characteristic morphology of apoptotic nuclei, loss of MMP and downmodulation of bcl~xl~. Strong activation of p38 was observed after 2 hr of exposure, indicating that apoptosis may be induced via a p38โ€mediated stress pathway. ยฉ 2004 Wileyโ€Liss, Inc.


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