Please use this identifier to cite or link to this item: https://hdl.handle.net/2440/53734
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Type: Journal article
Title: Synthesis, biological evaluation and molecular modelling of N-heterocyclic dipeptide aldehydes as selective calpain inhibitors
Author: Jones, M.
Morton, J.
Coxon, J.
McNabb, S.
Lee, H.
Aitken, S.
Mehrtens, J.
Robertson, L.
Neffe, A.
Miyamoto, S.
Bickerstaffe, R.
Gately, K.
Wood, J.
Abell, A.
Citation: Bioorganic and Medicinal Chemistry, 2008; 16(14):6911-6923
Publisher: Pergamon-Elsevier Science Ltd
Issue Date: 2008
ISSN: 0968-0896
1464-3391
Statement of
Responsibility: 
Matthew A. Jones, James D. Morton, James M. Coxon, Stephen B. McNabb, Hannah Y.-Y. Lee, Steven G. Aitken, Janna M. Mehrtens, Lucinda J.G. Robertson, Axel T. Neffe, Shigeru Miyamoto, Roy Bickerstaffe, Karl Gately, Jacqueline M. Wood and Andrew D. Abell
Abstract: A series of N-heterocyclic dipeptide aldehydes 4–13 have been synthesised and evaluated as inhibitors of ovine calpain 1 (o-CAPN1) and ovine calpain 2 (o-CAPN2). 5-Formyl-pyrrole 9 (IC50 values of 290 and 25 nM against o-CAPN1 and o-CAPN2, respectively) was the most potent and selective o-CAPN2 inhibitor, displaying >11-fold selectivity. The amino acid sequences of o-CAPN1 and o-CAPN2 have been determined. Because of the lack of available structural information on the ovine calpains, in silico homology models of the active site cleft of o-CAPN1 and o-CAPN2 were developed based on human calpain 1 (h-CAPN1) X-ray crystal structure (PDB code 1ZCM). These models were used to rationalise the observed SAR for compounds 4–13 and the selectivity observed for 9. The o-CAPN2 selective inhibitor 9 (CAT0059) was assayed in an in vitro ovine lens culture system and shown to successfully protect the lens from calcium-induced opacification.
Keywords: Animals
Sheep
Humans
Aldehydes
Glycoproteins
Dipeptides
Binding Sites
Structure-Activity Relationship
Models, Molecular
DOI: 10.1016/j.bmc.2008.05.048
Published version: http://dx.doi.org/10.1016/j.bmc.2008.05.048
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Chemistry publications

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