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Merck

Synthesis of novel anticancer agents through opening of spiroacetal ring of diosgenin.

Steroids (2014-06-15)
A A Hamid, Mohammad Hasanain, Arjun Singh, Balakishan Bhukya, Omprakash, Prema G Vasudev, Jayanta Sarkar, Debabrata Chanda, Feroz Khan, O O Aiyelaagbe, Arvind S Negi
ZUSAMMENFASSUNG

Diosgenin has been modified to furostane derivatives after opening the F-spiroacetal ring. The aldehyde group at C26 in derivative 8 was unexpectedly transformed to the ketone 9. The structure of ketone 9 was confirmed by spectroscopy and finally by X-ray crystallography. Five of the diosgenin derivatives showed significant anticancer activity against human cancer cell lines. The most potent molecule of this series i.e. compound 7, inhibited cellular growth by arresting the population at G0/G1 phase of cell division cycle. Cells undergo apoptosis after exposure to the derivative 7 which was evident by increase in sub G0 population in cell cycle analysis. Docking experiments showed caspase-3 and caspase-9 as possible molecular targets for these compounds. This was further validated by cleavage of PARP, a caspase target in apoptotic pathway. Compound 7 was found non-toxic up to 1000mg/kg dose in acute oral toxicity in Swiss albino mice.

MATERIALIEN
Produktnummer
Marke
Produktbeschreibung

Sigma-Aldrich
Tetramethylsilan, ACS reagent, NMR grade, ≥99.9%
Sigma-Aldrich
Tetramethylsilan, ≥99.0% (GC)
Sigma-Aldrich
Diosgenin, ≥93%
Sigma-Aldrich
Tetramethylsilan, electronic grade, ≥99.99% trace metals basis
Supelco
Tetramethylsilan, analytical standard, for NMR spectroscopy, ACS reagent