Search
Feedback
About UniCat 
Help
News
| Listing 1 - 10 of 82 | << page >> |
Sort by
|
ISBN: 0444805265 Year: 1984 Publisher: Amsterdam : Elsevier,
Abstract | Keywords | Export | Availability | Bookmark
Loading...Choose an application
- Reference Manager
- EndNote
- RefWorks (Direct export to RefWorks)
ISBN: 0121345505 0323155162 1299481302 9780121345501 Year: 1974 Publisher: New York: Academic press,
Abstract | Keywords | Export | Availability | Bookmark
Loading...Choose an application
- Reference Manager
- EndNote
- RefWorks (Direct export to RefWorks)
Enzymology --- Lipolytic enzymes --- Enzymes --- Lipase --- Phospholipase --- Enzymes. --- Lipase. --- Phospholipases. --- Lecithinase --- Lecithinases --- Acid Lipase --- Acid Lipase A --- Acid Lipase B --- Acid Lipase I --- Acid Lipase II --- Exolipase --- Monoester Lipase --- Triacylglycerol Hydrolase --- Triglyceridase --- Triolean Hydrolase --- Triacylglycerol Lipase --- Tributyrinase --- Triglyceride Lipase --- A, Acid Lipase --- B, Acid Lipase --- Hydrolase, Triacylglycerol --- Hydrolase, Triolean --- I, Acid Lipase --- II, Acid Lipase --- Lipase A, Acid --- Lipase B, Acid --- Lipase I, Acid --- Lipase II, Acid --- Lipase, Acid --- Lipase, Monoester --- Lipase, Triglyceride --- Biocatalysts --- Molecular Mechanisms of Pharmacological Action --- Phospholipases --- Biocatalyst --- Enzyme
Book
Year: 2006 Publisher: Bruxelles: UCL,
Abstract | Keywords | Export | Availability | Bookmark
Loading...Choose an application
- Reference Manager
- EndNote
- RefWorks (Direct export to RefWorks)
These last years, the elucidation of the physiological roles of the anandamide and the 2-arachidonoylglycérol, two endogenous molecules derived from the arachidonic acid, made it possible to highlight a system of neurotransmission called endocannabinoid system. Among the known enzymes of the endocannabinoid system, MonoGlycerol Lipase (MGL) is one of the less characterised. It is a serine hydrolase which is responsible for the degradation of the major endocannabinoid in the central nervous system, the 2-arachidonoylglycerol (2-AG). Several studies highlighted the pharmacological properties of 2-AG, like the inhibition of the proliferation of cancerous cells of breast and prostate, the stimulation of appetite, and a neuroprotector effect following central lesions. To block the MGL would make it possible to increase the rates of 2-AG and by there, to benefit from its pharmacological properties from the therapeutic point of view such as cancer, neuroprotection and anxiety. Nevertheless, few inhibitors of MGL are known to date. My studies consist on the screening of a library of various molecules in a hydrolysis assay of a radiolabelled substrate (2-oleoylglycérol, 2-OG) by the recombining MGL human in order to identify possible inhibitors of MGL and to highlight structure-activity relationships. Secondly, to appreciate the inhibition of active compound discovered by screening, the curves of inhibition have been realized. The pIC50 of several compounds have been determined and vary between 4,46 and 6,45. In a third time, the most potent compound of each groups were tested on intact glioma cells. This last evaluation, has been realized to know if these compound were able to modify the metabolism of 2-OG by intact cells. These different steps performed to identify three groups of chemical structures favourable for the inhibition of MGL: thioamides, phenyl maleimides and disulfides. Ces dernières années, l’élucidation des rôles physiologiques de l’anandamide et du 2-arachidonoylglycérol, deux molécules endogènes dérivées de l’acide arachidonique, a permis de mettre en évidence un système de neurotransmission appelé système endocannabinoïde. Parmi les enzymes connues du système endocannabinoïde, la Monoglycérol Lipase (MGL) est une des moins caractérisées. Il s’agit d’une sérine hydrolase responsable de la dégradation de l’endocannabinoïde majeur dans le système nerveux central, le 2-arachidonoylglycérol (2-AG). Les propriétés pharmacologiques de ce dernier comprennent l’inhibition de la prolifération des cellules cancéreuses du sein et de la prostate, la stimulation de l’appétit et un effet neuroprotecteur suite à des lésions centrales. La MGL dégrade le 2-AG par clivage de son lien ester donnant respectivement le glycérol et l’acide arachidonique. Bloquer la MGL permettrait d’augmenter les taux de 2-AG et par là, profiter de ses propriétés pharmacologiques dans des perspectives thérapeutiques tels que le cancer, la neuroprotection et l’anxiété. Néanmoins, peu d’inhibiteurs de la MGL sont connus à ce jour. C’est dans ce contexte de recherche que s’inscrit mon mémoire. Il consiste au criblage d’une librairie de molécules chimiques dans un test d’hydrolyse d’un substrat radiomarqué (le 2-oléoylglycérol, 2-OG) par la MGL recombinante humaine afin d’identifier d’éventuels inhibiteurs et de tenter de mettre en évidence un lien entre structure et activité. Trois groupes de structures ont été identifiés parmi la large chimiothèque testée. Deuxièmement, afin d’apprécier la puissance des composés les plus actifs, des courbes de détermination d’IC50 ont été réalisées. Les pIC50 de plusieurs composés sont ainsi connus et varient entre 4,46 et 6,45. Dans un troisième temps, les composés les plus puissants de chacun des trois groupes ont été testés sur des cultures de gliomes. Cette dernière évaluation a permis d’évaluer si ces composés étaient capables de modifier le métabolisme du 2-OG par les cellules intactes. Ces différentes étapes ont permis de mettre en évidence trois groupes de molécules présentant un squelette de base propice à l’inhibition de la MGL : les thioamides, les maléimides et les disulfides.
Lipase --- Cannabis --- Hydrolases --- Monoglycerides
Book
Year: 1950 Publisher: Edmonton, Alberta University of Alberta
Abstract | Keywords | Export | Availability | Bookmark
Dissertation
Year: 1986 Publisher: Alblasserdam Kanters
Abstract | Keywords | Export | Availability | Bookmark
Loading...Choose an application
- Reference Manager
- EndNote
- RefWorks (Direct export to RefWorks)
Lipase --- Liver --- metabolism --- enzymology
ISBN: 0121821854 0121821870 9780121821852 9780121821876 Year: 1997 Volume: 286 Publisher: London ; Tokyo ; New York Academic Press
Abstract | Keywords | Export | Availability | Bookmark
Loading...Choose an application
- Reference Manager
- EndNote
- RefWorks (Direct export to RefWorks)
Enzymology --- Lipase --- Biotechnology --- Enzymes --- Lipases
Book
ISBN: 1620813947 9781620813942 1620813661 9781620813669 Year: 2012 Publisher: New York
Abstract | Keywords | Export | Availability | Bookmark
Loading...Choose an application
- Reference Manager
- EndNote
- RefWorks (Direct export to RefWorks)
Lipase --- Hydrolases --- Industrial applications. --- Therapeutic use.
Book
Year: 1950 Publisher: Edmonton, Alberta University of Alberta
Abstract | Keywords | Export | Availability | Bookmark
Loading...Choose an application
- Reference Manager
- EndNote
- RefWorks (Direct export to RefWorks)
Bacteria --- Contamination --- Dairy products --- Lipase --- Measurement
Dissertation
Year: 1982 Publisher: Meppel Repro
Abstract | Keywords | Export | Availability | Bookmark
Loading...Choose an application
- Reference Manager
- EndNote
- RefWorks (Direct export to RefWorks)
Vitamin K --- Lipase --- Liver --- analysis --- metabolism --- enzymology
ISBN: 0521445469 Year: 1994 Publisher: Cambridge : Cambridge university press,
Abstract | Keywords | Export | Availability | Bookmark
Loading...Choose an application
- Reference Manager
- EndNote
- RefWorks (Direct export to RefWorks)
Basic Sciences. Chemistry --- Lipase. --- Biochemistry --- Proteins and Enzymes.
| Listing 1 - 10 of 82 | << page >> |
Sort by
|