Your search keyword '"Brigitte Kerfelec"' showing total 3 results

1. The Lipase C-terminal Domain

Author

Catherine Chapus, Laurence Ayvazian, Simone Granon, Brigitte Kerfelec, Isabelle Crenon, Edith Foglizzo, and Christophe Dubois

Subjects

chemistry.chemical_classification, Lipoprotein lipase, biology, Chemistry, Cell Biology, Colipase, Biochemistry, Micelle, Enzyme, In vivo, biology.protein, Lipase, Binding site, Molecular Biology, Ternary complex

Abstract

In vertebrates, dietary fat digestion mainly results from the combined effect of pancreatic lipase, colipase, and bile. It has been proposed that in vivo lipase adsorption on oil-water emulsion is mediated by a preformed lipase-colipase-mixed micelle complex. The main lipase-colipase binding site is located on the C-terminal domain of the enzyme. We report here that in vitro the isolated C-terminal domain behaves as a potent noncovalent inhibitor of lipase and that the inhibitory effect is triggered by the presence of micelles. Lipase inhibition results from the formation of a nonproductive C-terminal domain-colipase-micelle ternary complex, which competes for colipase with the active lipase-colipase-micelle ternary complex, thus diverting colipase from its lipase-anchoring function. The formation of such a complex has been evidenced by molecular sieving experiments. This nonproductive complex lowers the amount of active lipase thus reducing lipolysis. Preliminary experiments performed in rats show that the C-terminal domain also behaves as an inhibitor in vivo and thus could be considered a potential new tool for specifically reducing intestinal lipolysis.

Published

2001

2. Lipase Activation by Nonionic Detergents

Author

David Pignol, Isabelle Crenon, Brigitte Kerfelec, Catherine Chapus, Juan C. Fontecilla-Camps, and Juan A. Hermoso

Subjects

biology, Active site, Ether, Cell Biology, Crystal structure, Substrate analog, Colipase, Biochemistry, Micelle, Crystallography, chemistry.chemical_compound, chemistry, biology.protein, Organic chemistry, Lipase, Molecular Biology, Ethylene glycol

Abstract

The crystal structure of the ternary porcine lipase-colipase-tetra ethylene glycol monooctyl ether (TGME) complex has been determined at 2.8 A resolution. The crystals belong to the cubic space group F23 with a = 289.1 A and display a strong pseudo-symmetry corresponding to a P23 lattice. Unexpectedly, the crystalline two-domain lipase is found in its open configuration. This indicates that in the presence of colipase, pure micelles of the nonionic detergent TGME are able to activate the enzyme; a process that includes the movement of an N-terminal domain loop (the flap). The effects of TGME and colipase have been confirmed by chemical modification of the active site serine residue using diisopropyl p-nitrophenylphosphate (E600). In addition, the presence of a TGME molecule tightly bound to the active site pocket shows that TGME acts as a substrate analog, thus possibly explaining the inhibitory effect of this nonionic detergent on emulsified substrate hydrolysis at submicellar concentrations. A comparison of the lipase-colipase interactions between our porcine complex and the human-porcine complex (van Tilbeurgh, H., Egloff, M.-P., Martinez, C., Rugani, N., Verger, R., and Cambillau, C. (1993) Nature 362, 814-820) indicates that except for one salt bridge interaction, they are conserved. Analysis of the superimposed complexes shows a 5.4° rotation on the relative position of the N-terminal domains excepting the flap that moves in a concerted fashion with the C-terminal domain. This flexibility may be important for the binding of the complex to the water-lipid interface.

Published

1996

3. Binding of terbium and of an elastase inhibitor to bovine pancreatic subunit III, an inactive protease E

Author

J L Dimicoli, Catherine Chapus, and Brigitte Kerfelec

Subjects

Magnetic Resonance Spectroscopy, Serine Proteinase Inhibitors, Macromolecular Substances, Stereochemistry, medicine.medical_treatment, Protein subunit, Molecular Sequence Data, Biochemistry, Serine, Sequence Homology, Nucleic Acid, medicine, Animals, Humans, Anilides, Amino Acid Sequence, Binding site, Terbium, Pancreas, Molecular Biology, Binding Sites, Protease, Pancreatic Elastase, biology, Chemistry, Serine Endopeptidases, Elastase, Cell Biology, Endopeptidase, Kinetics, Elastase inhibitor, Spectrometry, Fluorescence, Enzyme inhibitor, biology.protein, Cattle, Protein Binding

Abstract

Using the Tb3+ luminescence technique, we showed that bovine subunit III, a defective pancreatic serine endopeptidase-like protease, possessed a single metal ion binding site able to bind Tb3+ with a high affinity comparable to that of porcine elastase. The topology of the metal ion binding site in subunit III is predicted from sequence homologies and modeling experiments based on the known crystallographic three-dimensional structures of the equivalent sites in porcine elastase 1 and bovine beta-trypsin. Moreover, the Tb3+ luminescence technique in parallel to a 19F NMR investigation, allowed us to measure the binding of a very potent specific inhibitor of porcine elastase (trifluoroacetyl-L-lysyl-alanyl p-trifluoromethylphenylanilide) to bovine subunit III. These results confirm that, although devoid of any specific activity, subunit III might possess a conformation close to that of an active enzyme and further support the analogy between subunit III and an elastase-like family.

Published

1990