Two synthetic approaches to boehmeriasin A are described. A gram scale racemic preparation is accompanied by an efficient preparation of both the pure enantiomers using the conformationally stable 2-piperidin-2-yl acetaldehyde as starting material. The anti-proliferative activity in three cancer cell lines (CEM, HeLa and L1210) and two endothelial cell lines (HMEC-1, BAEC) indicates promising activity at the nanomolar range. Topoisomerases and SIRT2 are identified as biological targets and the experimental data has been supported by docking studies.

Boehmeriasin A as new lead compound for the inhibition of topoisomerases and SIRT2

BROGGINI, GIANLUIGI;Gazzola, Silvia;
2015-01-01

Abstract

Two synthetic approaches to boehmeriasin A are described. A gram scale racemic preparation is accompanied by an efficient preparation of both the pure enantiomers using the conformationally stable 2-piperidin-2-yl acetaldehyde as starting material. The anti-proliferative activity in three cancer cell lines (CEM, HeLa and L1210) and two endothelial cell lines (HMEC-1, BAEC) indicates promising activity at the nanomolar range. Topoisomerases and SIRT2 are identified as biological targets and the experimental data has been supported by docking studies.
2015
92
766
775
10
Esperti anonimi
Inglese
Boehmeriasin A; Sirtuins inhibition; Topoisomerases inhibition; Total synthesis
262
Christodoulou, Michael S.; Calogero, Francesco; Baumann, Marcus; García Argáez, Aída Nelly; Pieraccini, Stefano; Sironi, Maurizio; Dapiaggi, Federico;...espandi
none
Articoli su Riviste::Articolo su Rivista
19
info:eu-repo/semantics/article
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11383/2019522
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