Synthesis of A83586C analogs with potent anticancer and beta-catenin/ TCF4/osteopontin inhibitory effects and insights into how A83586C modulates E2Fs and pRb.

Karl J Hale Soraya Manaviazar Linos Lazarides Jonathan George Marcus A Walters Jiaqiang Cai Vern M Delisser Gurpreet S Bhatia S Andrew Peak Stephen M Dalby Amandine Lefranc Ying-Nan P Chen Alexander W Wood Paul Crowe Pauline Erwin Mohamed El-Tanani

Org Lett

The School of Chemistry & Chemical Engineering and the Centre for Cancer Research and Cell Biology (CCRCB), Queen's University Belfast (QUB), Stranmillis Road, Belfast BT9 5AG, UK.

Published: February 2009

The synthesis of three potent new antitumor agents is described: the A83586C-citropeptin hybrid (1), the A83586C-GE3 hybrid (2), and l-Pro-A83586C (3). Significantly, compounds 1 and 2 function as highly potent inhibitors of beta-catenin/TCF4 signaling within cancer cells, while simultaneously downregulating osteopontin (Opn) expression. A83586C antitumor cyclodepsipeptides also inhibit E2F-mediated transcription by downregulating E2F1 expression and inducing dephosphorylation of the oncogenic hyperphosphorylated retinoblastoma protein (pRb).

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http://dx.doi.org/10.1021/ol802818f	DOI Listing

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