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Structure-Based Drug Design of Novel Aurora Kinase A Inhibitors: Structural Basis for Potency and Specificity

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dc.contributor.author Shukla, Paritosh
dc.date.accessioned 2021-11-11T10:53:59Z
dc.date.available 2021-11-11T10:53:59Z
dc.date.issued 2009-01-13
dc.identifier.uri https://pubs.acs.org/doi/10.1021/jm801270e
dc.identifier.uri http://dspace.bits-pilani.ac.in:8080/xmlui/handle/123456789/3290
dc.description.abstract Aurora kinases have emerged as attractive targets for the design of anticancer drugs. Through structure-based virtual screening, novel pyrazole hit 8a was identified as Aurora kinase A inhibitor (IC50 = 15.1 μM). X-ray cocrystal structure of 8a in complex with Aurora A protein revealed the C-4 position ethyl carboxylate side chain as a possible modification site for improving the potency. On the basis of this insight, bioisosteric replacement of the ester with amide linkage and changing the ethyl substituent to hydrophobic 3-acetamidophenyl ring led to the identification of 12w with a ∼450-fold improved Aurora kinase A inhibition potency (IC50 = 33 nM), compared to 8a. Compound 12w showed selective inhibition of Aurora A kinase over Aurora B/C, which might be due to the presence of a unique H-bond interaction between the 3-acetamido group and the Aurora A nonconserved Thr217 residue, which in Aurora B/C is Glu and found to sterically clash with the 3-acetamido group in modeling studies. en_US
dc.language.iso en en_US
dc.publisher ACS en_US
dc.subject Chemistry en_US
dc.subject X-rays en_US
dc.subject Peptides and proteins en_US
dc.subject Chemical structure en_US
dc.title Structure-Based Drug Design of Novel Aurora Kinase A Inhibitors: Structural Basis for Potency and Specificity en_US
dc.type Article en_US


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