Theoretical Study of Flavopiridol Binded to Transition Metals
الموضوعات : Journal of Physical & Theoretical Chemistry
M. Monajjemi1
1
(Not mentioned)
H. Passdar
2
(Not mentioned)
L. Saedi
3
(Not mentioned)
R. Ghiasi
4
(Not mentioned)
F. Mollaamin
5
(Not mentionrd)
الکلمات المفتاحية: conformations, comformational analysis, metalated flavopiridol, flavopiridol, transition metal, Ab initio, HF,
ملخص المقالة :
More recently medical chemistry research has been focused on proteins that drive and controlcell cycle progression. Among them, the cyclin dependent kinases (cdk’s) are a group ofserine/threonine kinases, which rule the transition between successive stages of the cell cycle. Theactivity of cdk’s is regulated by multiple mechanisms, including binding to cyclins, which is a broadclass of positive regulatory cdk-binding proteins. Among the chemical agents that act selectively ascdk inhibitors are flavonoids,flavopiridol is a semisynthetic flavonoid.Theoretical study is performedon flavopiridol using quantum chemical calculations. Interactions between flavopiridol withtransition metals were studied at HF/6-31G*, and HF/6-311G** levels of theory.Method: Ab initio method at HF level of theory was used.Results: Conformations, optimized parameters, bond length, were computed for metalated andisolated flavopiridol.Conclusions: Flavopiridol can be Metalated from its binding sites (oxo and hydroxyl groups) and theenergies of these compounds were computed.Abbreviations and notations: HF, Hartree-Fock; Cdk , Cyclin dependent kinases.
