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  • About
  • The Global ETD Search service is a free service for researchers to find electronic theses and dissertations. This service is provided by the Networked Digital Library of Theses and Dissertations.
    Our metadata is collected from universities around the world. If you manage a university/consortium/country archive and want to be added, details can be found on the NDLTD website.

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Showing 1 to 6 of 6 (0.044 seconds)

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1

Natural killer cell receptors and their MHC ligand interactions in innate resistance to mouse cytomegalovirus

Kielczewska, Agnieszka. January 2007 (has links)
Le premier but de mon projet de doctorat a ete la caracterisation moleculaire de l'interface entre les recepteurs activateurs des cellules Natural Killer (NK) et de leurs ligands exprimes dans les cellules infectees ainsi que l'implication de cette interaction sur la reponse a l'infection par le cytomegalovirus (MCMV). / J'ai tire un avantage de la variation naturelle au sein des membres lies aux recepteurs Ly49C ainsi que de la disponibilite des structures cristallines des Ly49 afin de comprendre les determinants moleculaires des interactions Ly49H-m157 et egalement identifier les residus des acides amines qui permettent de discriminer entre les recepteurs qui se lient et ceux qui ne se lient pas a m157. Mes decouvertes suggerent que le "site 2" du contact entre le CMH de classe I et Ly49 n'est visiblement pas implique dans la liaison avec m157. Au contraire, les residus localises au niveau de l'interface homodimere-recepteur seraient probablement critiques a la reconnaissance fonctionnelle de la glycoproteine m157. Notre approche fonctionnelle et de modelisation tridimensionnelle suggerent que l'architecture du dimere Ly49H est cruciale pour l'accessibilite de m157 mais non pour les molecules de CMH de classe I et relient la variabilite dans l'homodimerisation des Ly49 a la reconnaissance directe des produits pathogeniques. / Un autre mecanisme de la reponse de l'hote contre MCMV provient de l'etude de la souche de souris MA/My, laquelle, malgre l'absence du gene Ly49h ainsi que la proteine pour laquelle il code, y est hautement resistant. Des etudes anterieures ont demontre qu'une interaction epistatique entre un gene issu du groupe des genes Ly49 sur le chromosome 6 et le CMH (H2) sur le chromosome 17 est associee avec la resistance au virus. Utilisant une methode de co-culture de cellules reportrices NFAT-GFP exprimant les recepteurs activateurs Ly49 et de fibroblastes primaires infectes, j'ai montre que le recepteur activateur Ly49P des cellules NK reconnait specifiquement les cellules infectees par MCMV et que cette reconnaissance depend de la presence de l'haplotype H2k. Ce signal etait bloque par l'utilisation des anticorps anti-H2-D k mais non par anti-H2-Kk. Ces resultats indiquent l'existence d'un nouveau mecanisme des cellules NK implique dans la resistance au MCMV, lequel depend de l'interaction fonctionnelle entre le recepteur Ly49P et la molecule du MHC de classe I, H2-Dk, dans les cellules infectees par MCMV. Comme contribution directe de ce travail, nous avons demontre que la resistance chez MA/My est au moins partiellement dependante des interactions entre le recepteur Ly49P et la molecule H2-Dk modifiee par le virus dans les cellules infectees. Comme MCMV regule negativement l'expression des molecules du CMH de classe I, j'ai confirme la presence de H2-Dk dans les cellules infectees par l'utilisation d'un virus MCMV recombinant portant un gene rapporteur GFP. En permutant la plateforme peptidique de liaison, les domaines transmembranaires et intracellulaires entre les molecules H2-Db et H2-D k, j'ai demontre que la plateforme peptidique de liaison est critique pour la reconnaissance des cellules infectees. Par le criblage d'un panel de mutants MCMV portant des genes impliques dans l'evasion immune, j'ai demontre que l'infection de fibroblastes par le MCMV depourvu du gene m04 (Deltam04) abolit totalement l'activation de Ly49P. (Abstract shortened by UMI.)
Muromegalovirus -- immunology.
Herpesviridae Infections -- immunology.
Killer Cells, Natural -- immunology.
Antigens, Ly -- immunology.
Lectins, C-Type -- immunology.
2

The ligand and function of the RegIII family of bactericidal C-type lectins

Cash, Heather Lynn. January 2006 (has links)
Thesis (Master of Science) -- University of Texas Southwestern Medical Center at Dallas, 2006. / Embargoed. Vita. Bibliography: 147-160.
3

Differential dengue tropism & neutralization : potential mechanisms of pathogenesis /

Martin, Nicole C Couillard, Nicole January 2006 (has links) (PDF)
Thesis (Ph.D.)--Uniformed Services University of the Health Sciences, 2006 / Typescript (photocopy)
4

Natural killer cell receptors and their MHC ligand interactions in innate resistance to mouse cytomegalovirus

Kielczewska, Agnieszka. January 2007 (has links)
No description available.
Antigens, Ly -- immunology.
Muromegalovirus -- immunology.
Killer Cells, Natural -- immunology.
Herpesviridae Infections -- immunology.
Lectins, C-Type -- immunology.
5

Intercellular protein transfer and regulation of inhibitory NK cell receptor accessibility /

Andersson, Katja, January 2007 (has links)
Diss. (sammanfattning) Stockholm : Karolinska institutet, 2007. / Härtill 4 uppsatser.
6

Efeitos renais de miotoxinas e lectinas purificadas dos venenos das serpentes Bothrops jararacussu e Bothrops moojeni. Papel da ciclooxigenase e endotelina / Renal effects promoted by myotoxins and lectins isolated from the snake venoms of Bothrops jararacusu and Bothrops moojeni. The role of cyclooxigenase and endothelin

Paulo SÃrgio Ferreira Barbosa 03 March 2006 (has links)
CoordenaÃÃo de AperfeiÃoamento de Pessoal de NÃvel Superior / A insuficiÃncia renal aguda à uma das complicaÃÃes mais freqÃentes nos envenenamentos ofÃdicos. Contudo, a sua patogÃnese permanece obscura. Em nossos estudos foram avaliados os efeitos renais causados pelas miotoxinas purificadas dos venenos das serpentes Bothrops jararacussu (Bthtx I, Lys 49 e Bthtx II, Asp 49) e Bothrops moojeni (BmTx I, Lys 49), assim como pelas lectinas dos venenos de Bothrops moojeni (BmLec) e Bothrops jararacussu (BJcuL). Tentando avaliar o mecanismo envolvido nos efeitos renais das substÃncias acima mencionadas, foram testados os efeitos da indometacina, um bloqueador inespecÃfico de ciclooxigenase. Adicionalmente, foram avaliados os efeitos inibitÃrios do Tezosentan, um bloqueador de receptor de endotelina, nos efeitos renais causados pela miotoxina I da serpente Bothrops moojeni. Para tanto, as miotoxinas, na dosagem de 5Âg/mL, ou as lectinas, na dosagem de 10Âg/mL foram adicionadas 30 minutos depois do inÃcio dos experimentos. Contudo, a indometacina e o tezosentan foram adicionados no sistema de perfusÃo sempre no inÃcio de cada experimento na dosagem de 10Âg/mL. Os efeitos renais foram comparados com um grupo controle, onde os rins foram perfundidos somente com a soluÃÃo de Krebs-Henseleit modificada. Bthtx I, BthtxII e BmLec aumentaram a pressÃo de perfusÃo (C120= 110,28  3,09, Bthtx I120 = 171,20  6,3 *, Bthtx II120 = 175,50  7,20 * e BmLec120 = 152,50  2,10 *), a resistÃncia vascular renal (C120= 5,46  0,54, Bthtx I120= 8,62  0,37 *, Bthtx II120= 8,90  0,36 * e BmLec120= 7,77  0,30*), o fluxo urinÃrio (C120= 0,143  0,008, Bthtx I120= 0,326  0,048*, e Bthtx II120= 0,373  0,085*, BmLec120= 0,085  0,007* ), o ritmo de filtraÃÃo glomerular (C120= 0,678  0,065, Bthtx I120= 0,855  0,133 *, Bthtx II120= 1,224  0,282*, BmLec120=1,037  0,055*) e a excreÃÃo de sÃdio potÃssio e cloreto (ENa+, EK+, ECl-). PorÃm, diminuÃram os percentuais dos transportes tubulares de sÃdio (C120= 79,76  0,56, Bthtx I120= 62,23  4,12*, Bthtx II120= 70,96  2,93* e BmLec60= 77,25  1,36*) e potÃssio (C60= 66,38  3,31, Bthtx I60= 55,79  5,57 *, Bthtx II60= 50,86  6,16* e BmLec60= 59,78  3,49). A indometacina foi capaz de bloquear os efeitos causados pela miotoxina I da B. jararacussu e lectina da B. moojeni, mas reverteu parcialmente os efeitos causados pelas miotoxinas II e lectina da B. jararacussu e miotoxina I da B. moojeni. O tezosentan, por sua vez, bloqueou os efeitos causados pela miotoxina I da B. moojeni. Foi concluÃdo que prostaglandinas estÃo envolvidas nas alteraÃÃes renais promovidas pelas substÃncias isoladas das serpentes B. jararacussu e B. moojeni, enquanto que endotelina seria o principal mediador nas alteraÃÃes renais causadas pela miotoxina I da B. moojeni. / Acute renal failure is one of the most common systemic complications after snakebite. However, its pathogenesis remains obscure. In this study, we evaluated the renal effects of Bothrops jararacussu myotoxins I and II (Bthtx-I Lys 49 and BthtxII, Asp 49), Bothrops moojeni myotoxin I and the lectins from Bothrops moojeni and Bothrops jararacussu. Attempting to investigate the mechanisms involved in the renal effects of the mentioned toxins, we tested indomethacin, an unespecific cyclooxigenase inhibitor. Additionally, tezosentan, an endothelin receptor blocker, was used to evaluate the role of endothelin in the renal effects of Bothrops moojeni myotoxin I. All myotoxins (5 Âg/mL) and lectins (10Âg /mL) were added to the perfusion system 30 min after the beginning of each perfusion. Indomethacin (10Âg/mL) and tezosentan (10 Âg /mL) were always added 30 minutes before the tested substances. The renal effects were compared against a control group, where kidneys were perfused only with the modified Krebs-Henseleit solution. Myotoxins from Bothrops jararacussu and the lectin from Bothrops moojeni increased the perfusion pressure (C120= 110.28  3.09, Bthtx I120= 171.20  6.3 * ,Bthtx II120= 175.50  7.20 * and BmLec120= 152.50  2.10 *), the renal vascular resistance (C120= 5.46  0.54, Bthtx I120= 8.62  0.37 *, Bthtx II120= 8.90  0.36 * and BmLec120= 7.77  0.30*), the urinary flow (C120= 0.143  0.008, Bthtx I120= 0.326  0.048*, and Bthtx II120= 0.373  0.085* ), the glomerular filtration rate (C120= 0.678  0.065, Bthtx I120= 0.855  0.133 *, Bthtx II120= 1.224  0.282* and BmLec120= 1.037  0.055*) and the sodium, potassium and chloride excretion. On the other hand, the same substances decreased the percent of renal tubular transport of sodium (C120= 79.76  0.56, Bthtx I120= 62.23  4.12*, Bthtx II120= 70.96  2.93* and BmLec60= 77.25  1.36*), potassium (C60= 66.38  3.31, Bthtx I60= 55.79  5.57 *, Bthtx II60= 50.86  6.16* and BmLec60= 59.78  3.49*). Indomethacin inhibited the renal effects induced by Bothrops jararacussu myotoxin I and Bothrops moojeni lectin, but partially blocked the effects promoted by myotoxin II and the lectin of Bothrops jararacussu, and the effects of myotoxin I of Bothrops moojeni. Tezosentan inhibited the renal effects induced by B. moojeni myotoxin I. In conclusion, prostaglandins are involved in the renal alterations induced by myotoxins and lectins purified from the snake venoms of Bothrops jararacussu and Bothrops moojeni. In addition, endothelin is the main mediator of the renal alterations promoted by Bothrops moojeni myotoxin I
Lectinas Tipo C
Fosfolipases A
Bothrops
Rim â patologia
Rim â fisiologia
Venenos de Serpentes - farmacologia
Venenos de Serpentes - toxicidade
Lectins, C-Type
Phospholipases A
Kidney - pathology
Kidney - physiology
Snake Venoms - pharmacology
Snake Venoms - toxicity
FARMACOLOGIA GERAL

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