Journal article

Identification and characterization of bi-thiazole-2,2′-diamines as kinase inhibitory scaffolds

KRW Ngoei, DCH Ng, PR Gooley, DP Fairlie, MJ Stoermer, MA Bogoyevitch

Biochimica Et Biophysica Acta Proteins and Proteomics | ELSEVIER SCIENCE BV | Published : 2013

DOI: 10.1016/j.bbapap.2013.02.001

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Abstract

Based on bioinformatics interrogation of the genome, > 500 mammalian protein kinases can be clustered within seven different groups. Of these kinases, the mitogen-activated protein kinase (MAPK) family forms part of the CMGC group of serine/threonine kinases that includes extracellular signal regulated kinases (ERKs), cJun N-terminal kinases (JNKs), and p38 MAPKs. With the JNKs considered attractive targets in the treatment of pathologies including diabetes and stroke, efforts have been directed to the discovery of new JNK inhibitory molecules that can be further developed as new therapeutics. Capitalizing on our biochemical understanding of JNK, we performed in silico screens of commerciall..

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University of Melbourne Researchers

Grants

Awarded by Appalachian Regional Commission

Funding Acknowledgements

This work was supported by an ARC Discovery grant (DP0984225 to MAB). KRWN acknowledges the support of a Melbourne International Research Scholarship (MIRS), a Melbourne International Fee Remission Scholarship (MIFRS) and a Melbourne Research Scholarship (MRS). DN is supported by the University of Melbourne CR Roper Bequest Fellowship.

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Keywords

Peptide Inhibitor
31 Biological Sciences
Map
Biophysics
Chemical Inhibitor
Science & Technology
in Silico Screen
Activated Protein-Kinase
C-Jun N-Terminal Kinase
2.1 Biological and Endogenous Factors
N-Terminal Kinase
Drug Discovery
Biotechnology
C-Jun
Kinome
P38 Mapk
Protein Kinase
Jnk
Breast-Cancer
Kinetics
Life Sciences & Biomedicine
Critical Features
Biochemistry & Molecular Biology