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A disulphide bridge allows for site selective binding in liver BABP stabilising the orientation of key amino acid side-chains

Academic Article
Publication Date:
2012
abstract:
The presence of a disulfide bridge in liver bile acid binding protein (L-BABP/S-S) allows for site-selective binding of two bile acids, glycochenodeoxycholic (GCDA) and glycocholic acid (GCA), differing only in the presence of a hydroxyl group. The protein form devoid of the disulfide bridge (L-BABP) binds both bile salts without discriminating ability. We investigate the determinants of the molecular recognition process in the formation of the heterotypic L-BABP/S-S complex with GCA and GCDA located in the superficial and inner protein sites, respectively. The comparison of the NMR spectroscopy structure of heterotypic holo L-BABP/S-S, the first reported for this protein family, with that of the homotypic L-BABP complex demonstrates that the introduction of a SS link between adjacent strands changes the conformation of three key residues, which function as hot-spot mediators of molecular discrimination. The favoured ?1 rotameric states (t, g+ and g- for E99, Q100 and E109 residues, respectively) allow the onset of an extended intramolecular hydrogen-bond network and the consequent stabilisation of the side-chain orientation of a buried histidine, which is capable of anchoring a specific ligand
Iris type:
01.01 Articolo in rivista
Keywords:
NMR; protein
List of contributors:
Cogliati, Clelia; Molinari, Henriette; Pagano, Katiuscia; Ragona, LAURA GIUDITTA; Tomaselli, Simona
Authors of the University:
PAGANO KATIUSCIA
RAGONA LAURA GIUDITTA
TOMASELLI SIMONA
Handle:
https://iris.cnr.it/handle/20.500.14243/30875
Published in:
CHEMISTRY-A EUROPEAN JOURNAL
Journal
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