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Design and evaluation of a photoprotective compound able to release taurine under conditions of oxidative stress / Patrick Lafitte in IFSCC MAGAZINE, Vol. 11, N° 2 (04-05/2008)
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Titre : Design and evaluation of a photoprotective compound able to release taurine under conditions of oxidative stress Type de document : texte imprimé Auteurs : Patrick Lafitte, Auteur ; Lionel Valenti, Auteur ; Lydia Casciani, Auteur ; Thierry Hoarau, Auteur ; Erika Lomonte, Auteur ; Frédéric Maccario, Auteur ; Jean-François Nicolaÿ, Auteur Année de publication : 2008 Article en page(s) : p. 105-112 Note générale : Bibliogr. Langues : Anglais (eng) Tags : Photoprotection Antioxidant 'Electrophilic species scavenging' 'Structure-activity relationship' Taurine Index. décimale : 668.5 Parfums et cosmétiques Résumé : A novel photoprotective ingredient with anti-oxidant and electrophilic scavenging properties was designed. A structure–activity relationship study was conducted in order to optimize its bioavailability, specifically its ability to reach deep layers of the skin that may be affected by ultraviolet radiation-induced oxidative stress. A particular characteristic of this compound is its ability to release taurine upon reaction with some reactive oxygen species. In situ taurine formation may contribute to photoprotection. Preliminary in vitro experiments provide some evidence for effective protection against UVA-induced oxidative stress. Scavenging of the electrophilic species 4-hydroxynonenal, a highly cytotoxic end product of membrane lipid peroxidation, seems to be 2-oxo-1,3-thiazolidine major photoprotective mechanism. Permalink : https://e-campus.itech.fr/pmb/opac_css/index.php?lvl=notice_display&id=10358
in IFSCC MAGAZINE > Vol. 11, N° 2 (04-05/2008) . - p. 105-112[article]Réservation
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Code-barres Cote Support Localisation Section Disponibilité 010540 - Périodique Bibliothèque principale Documentaires Disponible Multicompartmental protection against toxic glycation late products with a "biobetter" dipeptide / Barbara Morand in IFSCC MAGAZINE, Vol. 16, N° 3 (07-08-09/2013)
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Titre : Multicompartmental protection against toxic glycation late products with a "biobetter" dipeptide Type de document : texte imprimé Auteurs : Barbara Morand, Auteur ; Christelle Golebiewski, Auteur ; Jessica Guglielmi, Auteur ; Pascale Prouheze, Auteur ; Mélanie Mollet, Auteur ; Patrick Lafitte, Auteur ; Jean-François Nicolaÿ, Auteur ; Mathilde Fréchet, Auteur Année de publication : 2013 Article en page(s) : p. 177-184 Note générale : Bibliogr. Langues : Anglais (eng) Catégories : Composés carbonylés
Glycation
Vieillissement cutanéIndex. décimale : 668.5 Parfums et cosmétiques Résumé : Dicarbonyl species such as methylglyoxal and glyoxal are toxic late products (but not end products) of the glycation process that readily react with extracellular matrix proteins and also intracellular cytoplasmic or nuclear targets. These reactive species have thus a major impact on cellular metabolism and actively participate in accelerated skin aging. We designed through a structure-activity relationship study a specific scavenger (DAPHIS) and compared the properties of this compound with those of reference dicarbonyl scavengers and the template antiglycation natural dipeptides carnosine and carcinine. DAPHIS is a bioavailable peptide. It protects the highly sensitive extracellular protein fibrillin-1.
Several in vitro tests highlighted the intra-cellular damage provoked by dicarbonyls. We could show that DAPHIS protects proteins, and in particular type I collagen, from extensive crosslinking by glyoxal or methylglyoxal. It was more efficient than aminoguanidine (a gold standard for dicarbonyl scavenging) and its parent peptides carnosine and carcinine. An ex vivo test with human skin expiants showed that DAPHIS deposited on the surface of human skin expiants limits dicarbonylmediated damage in the dermis.
In human fibroblasts, glyoxal induces the formation of large aggregates of a cytosolic protein, vimentin, which results in a decreased contractile capacity of the fibroblasts (decreased traction on extracellular fibrils). DAPHIS prevented vimentin aggregation and preserved the contractile power of fibroblasts in a dermal equivalent model. This clearly indicated that protection of fibroblasts has a direct effect on preservation of skin mechanical properties.
Final& in the nuclear compartment DA-PHIS could protect dicarbonyl-sensitive histone proteins (both glyoxal and methyl-glyoxal), combating crosslinking and nuclear advanced glycation end product formation. It completely prevented histone damage, while the parent dipeptides carnosine and carcinine had no protective effect and reference scavengers were less effective.
Taken together, these results demonstrate that we have designed a superior dicarbonyl scavenger, a "biobetter" pep-tide, that protects preferential targets of these toxic late products of glycation. Clearly, a high efficiency was required for these sensitive targets, and "regular" scavengers were not suitable.Note de contenu : - EXPERIMENTAL : Dicarbonyl scavening assay - eGFP fluorescence assay - eGFP glycation assessment - Collagen crosslinking assay - Ex vivo test on human skin explants exposed to methylglyoxal - Cell proliferation assay - Cytosolic compartment - Nuclear compartment
- RESULTS AND DISCUSSION : Reactivity assessment - Protection of the model protein eGFP - In vitro protection of collagen (extracellular matrix) - Ex vivo protection of extracellular matrix proteins of the dermis - Protection of cutaneous cells - Protection of the intracellular protein vimentin - Protection of nuclear protein histonesPermalink : https://e-campus.itech.fr/pmb/opac_css/index.php?lvl=notice_display&id=19306
in IFSCC MAGAZINE > Vol. 16, N° 3 (07-08-09/2013) . - p. 177-184[article]Réservation
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Code-barres Cote Support Localisation Section Disponibilité 15469 - Périodique Bibliothèque principale Documentaires Disponible