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Les IgG et les IgE spécifiques aux isocyanates chez les apprentis en carrosserie automobile à risque de développer de l'asthme professionnelDragos, Mircea Claudiu January 2003 (has links)
Mémoire numérisé par la Direction des bibliothèques de l'Université de Montréal.
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Role of Fyn and Lyn in IgG-mediate immune responsesFalanga, Yves 23 July 2012 (has links)
Anaphylaxis is a rapid, life-threatening hypersensitivity reaction. Until recently, it was mainly attributed to histamine released by mast cells activated by allergen crosslinking (XL) of FcεRI-bound allergen-specific IgE. However, recent reports established that anaphylaxis could also be triggered by basophil, macrophage and neutrophil secretion of platelet activating factor subsequent to FcγR stimulation by IgG/Ag complexes. I have investigated the contribution of Fyn and Lyn tyrosine kinases to FcγRIIb and FcγRIII signaling in the context of IgG-mediated passive systemic anaphylaxis (PSA). I found that mast cell IgG XL induced Fyn, Lyn, Akt, Erk, p38 and JNK phosphorylation. Additionally, IgG XL of mast cells, basophils and macrophages resulted in Fyn- and Lyn-regulated mediator release in vitro. FcγR–mediated activation was enhanced in Lyn-deficient (KO) cells, but decreased in Fyn KO cells, compared to wild type cells. More importantly, Lyn KO mice displayed significantly exacerbated PSA features while no change was observed for Fyn KO mice, compared to wild type littermates. Intriguingly, this work establishes that mast cells account for the majority of serum histamine in IgG-induced PSA. Taken together, these findings establish pivotal roles for Fyn and Lyn in the regulation of PSA and highlight their unsuspected functions in IgG-mediated pathologies.
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Seroprävalenz von Masernvirus-IgG Antikörpern: Untersuchung zum Zusammenhang zwischen Avidität und In-Vitro-NeutralisationsfähigkeitWernecke, Norman 04 October 2016 (has links) (PDF)
Die vorliegende Arbeit hatte das Ziel, die Korrelation zwischen der Avidität der Anti-Masern-IgG-Antikörper und deren In-Vitro-Neutralisationsfähigkeit zu untersuchen, sowie mittels Datenbankanalyse die Seroprävalenz von schützenden Antikörpern gegen Masern und den Impfstatus der Kinder- und Jugendlichen festzustellen. Die lineare Korrelation zwischen Neutralisationsfähigkeit und Avidität war in dieser Stichprobe schwach (ρ=0,240, p=0,006). Für hohe IgG Konzentrationen über 1000 mIU/ml fand sich eine mittlere Korrelation zwischen Avidität und Neutralisationstiter (ρ=0,612; p<0,001).
Bei den untersuchten Jahren von 1997 bis 2013 zur Seroprävalenz (n=8611) wiesen im Durchschnitt 93,4 % der Patienten IgG-Konzentrationen im positiven Bereich (>200 mIU/ml) auf. In allen Jahrgängen lag der Anteil über 90 %.
Zur Ermittlung des Impfstatus wurde eine Stichprobe 2- bis 18-Jähriger aus dem Jahr 2012 untersucht. Insgesamt hatten 81,1 % die erste Masernimpfung erhalten. Die zweite Masernimpfung erhielten noch 59,7 % der Kinder und Jugendlichen.
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Understanding the BED capture enzyme immunoassay (CEIA): measuring HIV-1 incidence in cross-sectional studiesMarinda, Edmore 08 May 2013 (has links)
Thesis (Ph.D.(Public Health))--University of the Witwatersrand, Faculty of Health Sciences, 2012. / Measuring HIV incidence has proved challenging over the years. A number of
serological HIV assays have been proposed, and among these, the BED Capture
Enzyme Immunoassay (CEIA) is one of the more widely used. Although the assay
performs well among known seroconverting panels, it has been shown to classify
some long term infected patients as being recently infected. Information on the
performance of the BED assay among low CD4 cell count patients and those on antiretroviral
therapy is limited. The risk of onwards transmission of HIV has been
reported to be elevated around the seroconversion period compared to the chronic
stage of infection. RNA viral load has been reported as the strongest predictor of HIV
transmission compared to other HIV markers. Understanding how these markers
influence the relationship between the likelihood of being recently infected and the
BED assay might help in understanding some of the shortcomings of the BED assay.
The main aim of this study was to understand the properties of the BED assay. The
performance of the BED assay among advanced HIV disease patients and the
influence of ART on BED levels once patients started treatment was investigated. The
BED assay and CD4 cell count were used to quantify the risk of in utero and intrapartum
transmission to their infants among women believed to have seroconverted
during pregnancy. The influence of viral load, haemoglobin and mid-upper arm
circumference was investigated on the relationship between the probability of being
recently infected and BED ODn levels.
Methods
Cryopreserved plasma samples from HIV patients on the national antiretroviral
treatment (ART) rollout programme at Tygerberg Hospital HIV clinic, South Africa,
iv
were used to investigate the effect of ART on BED ODn levels once patients
commenced treatment. Mixed effect logistic regression models accounting for
multiple readings per patient were used.
To investigate the risk associated with seroconversion during pregnancy HIV
seropositive women who had just given birth were classified into mutually exclusive
groups according to their likelihood of having recently seroconverted using BED and
CD4 cell count levels. Multinomial logistic regression models adjusting for other
factors were used to assess the risk of MTCT in utero and intra-partum infection
comparing these groups.
To investigate the relationship between BED ODn levels and the probability of being
recently infected, BED data from known HIV infected women and women who
seroconverted over a 2 year period was used. Fractional polynomial regression
models that allow for non-linear functions to be fitted were used, and the influence of
viral load, haemoglobin and mid-upper arm circumference was assessed through
multi-variable models. Data from the Zimbabwe Vitamin A for Mothers and Babies
(ZVITAMBO) project, a double blinded treatment-placebo trial was used for these
last two objectives.
Results
Patients with very low CD4 cell counts were more likely to test false recently infected
according to the BED assay than other patients. ART changed BED ODn kinetics
among HIV patients on treatment. Over half of advanced disease stage patients were
likely to be classified as being recently infected according to the BED assay 2 years
into ART treatment.
v
Women who seemed to have seroconverted during pregnancy had elevated risk of
transmitting HIV in-utero compared to chronic HIV patients. BED and CD4 cell
count were not predictive of risk of intra-partum infections attributed to
seroconversion during pregnancy.
The relationship between the probability of being recently infected with HIV and
BED ODn levels was described better using Fractional Polynomial regression models
than using a linear model in BED ODn or a model in which the BED ODn was
categorised. Viral load and haemoglobin were important independent predictors of
incident infections.
Conclusions
If the BED assay is to be used for HIV incidence estimations patients on ART should
be accounted for. The BED assay together with other HIV serological markers can be
used as prognostic tools to assess the risk of HIV transmission.
The risk of in-utero transmission of HIV is higher among women who seroconvert
during pregnancy. Repeat HIV testing among pregnant women may help in
identifying women who seroconvert during pregnancy, and these women will benefit
from Prevention of Mother-to-Child transmission (PMTCT) programmes.
It was found that additional markers such as viral load and haemoglobin did not alter
the relationship between the probability of having been recently infected and BED
ODn.
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Toxoplasmose aguda em gestantes de Araraquara-SP : avaliação da aplicabilidade do teste de avidez de IgG anti-toxoplasma /Isabel, Thais Ferreira. January 2006 (has links)
Resumo: A toxoplasmose na maioria dos casos é assintomática, porém pode causar seqüelas graves no feto, quando transmitida durante a fase aguda da infecção pela gestante. Diante disso, é de fundamental importância o acompanhamento sorológico de gestantes, a fim de definir o momento em que houve a aquisição da infecção por T. gondii, possibilitando assim, o tratamento precoce e diminuindo, portanto, o risco de transmissão congênita. No período de Janeiro a Novembro de 2005, avaliou-se a metodologia sorológica do teste de avidez de IgG anti-Toxoplasma gondii na rotina laboratorial entre as gestantes com teste sorológico negativo para anticorpos IgM anti-Toxoplasma (n = 200) e gestantes com teste sorológico positivo (n = 33) durante o pré-natal, em Araraquara-SP, no Laboratório de Imunologia Clínica e Biologia Molecular NAC-FCF/UNESP. Os resultados foram avaliados, segundo o perfil sorológico das gestantes participantes da pesquisa e a variação do índice de avidez de IgG entre as soropositivas para IgM e sua relação com o tratamento antiparasitário. Baseando-se nos resultados ressaltou-se a importância da adoção de medidas profiláticas para a redução da transmissão congênita. Todos os resultados para anticorpos IgG e IgM devem ser notificados na ficha da paciente, outros testes complementares devem ser realizados e a interpretação utilizada para o teste de avidez de IgG, precisa ser padronizada. Concluiu-se que alguns profissionais de saúde realizaram desnecessariamente o tratamento antiparasitário nas gestantes. Embora as gestantes realizem em sua maioria, o pré-natal no primeiro trimestre de gestação, a prevalência para toxoplasmose entre as gestantes de Araraquara-SP foi elevada, necessitando, portanto, de melhor acompanhamento da gestante e do recém-nascido e conscientização da importância da assistência à saúde pelos serviços de saúde. / Abstract: Toxoplasmosis usually is asymptomatic but can cause serious sequels in the fetus, when transmitted during the acute stage by the pregnant woman. Therefore, the serological screening of pregnant women has fundamental importance, in order to define the moment of contamination by T. gondii, and thus facilitating the precocious treatment and decreasing the risk of congenital transmission. During the period of January to November of 2005, we evaluated the serological methodology of IgG avidity test for toxoplasmosis in the routine laboratory, among pregnant women, with negative serological test for anti-Toxoplasma IgM antibodies (n = 200) and pregnant with serological test positive (n = 33), during the prenatal, in Araraquara-SP, in Immunology Clinic's Laboratory and Molecular Biology NAC-FCF/UNESP. The results in this study were evaluated, according to the serological profile of the pregnant women and the variation of anti-Toxoplasma IgG avidity index among the pregnant women with positive IgM antibodies and its relationship with the antiparasitic treatment. According to our results, we reinforce the importance of use prophylactics measures to reduce congenital transmission. All results for IgG and IgM antibodies must be notified, other complementary tests should be accomplished and the interpretation used for the IgG avidity test should be standardized. We concluded that some professionals realized unnecessary antiparasitic treatment. Although most of pregnant women at Araraquara-SP accomplish the prenatal in the first trimester of gestation, the prevalence for toxoplasmosis are elevated, needing therefore, a better accompaniment of the pregnant women and of the newly born and conscientiousness about the importance of health assistance during pregnancy by health services. / Orientador: Maria Jacira Silva Simões / Coorientador: Paulo Inácio da Costa / Banca: Semíramis Guimarães Ferraz Vianna / Banca: Herminia Yohko Kanamura / Mestre
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Investigation of novel therapeutic strategies in B cell and antibody mediated diseaseBanham, Gemma January 2019 (has links)
Terminally differentiated B cells are responsible for antibody generation, a key component of adaptive immunity. IgG antibodies play an important role in defence against infection but can be pathogenic in some autoimmune diseases and in solid organ transplantation. In addition to antibody generation, there is increasing interest in the antibody-independent functions of B cells, including their ability to regulate immune responses via the production of IL10. In this thesis I firstly explored the therapeutic potential of belimumab, an anti-BLyS antibody, in an experimental medicine study in kidney transplant recipients. The rationale for this study was based on published studies showing that B cells activate alloreactive T cells and secrete human leukocyte antigen (HLA) and non-HLA antibodies that negatively affect graft function and survival, but may also play a protective role by regulating alloimmune responses promoting transplant tolerance. B-Lymphocyte Stimulator (BLyS) is a cytokine that promotes B cell activation and survival. We performed the first randomized controlled trial using belimumab as early maintenance immunosuppression in kidney transplantation. In belimumab-treated subjects, we demonstrate a reduction in naïve and activated memory B cells, plasmablasts, IgG transcripts in peripheral blood and new antibody formation as well as evidence of reduced CD4 T cell activation and of a skewing of the residual B cell compartment towards an IL10-producing regulatory phenotype. This experimental medicine study highlights the potential of belimumab as a novel therapeutic agent in transplantation. In the second part of my project I performed a preclinical study investigating the potential efficacy of bromodomain inhibitors in reducing antibody-mediated immune cell activation. Immune complexed antigen can activate mononuclear phagocytes (MNP), comprising macrophages and dendritic cells (DCs), via ligation of Fc gamma receptors (FcγR), that bind the Fc region of IgG. FcγR-dependent MNP activation results in profound changes in gene expression that mediate antibody effector function in these cells. The resulting inflammatory response can be pathological in the setting of autoimmune diseases, such as systemic lupus erythematosus and in antibody-mediated rejection in transplantation. BET proteins are a family of histone modification 'readers' that bind acetylated lysine residues within histones and function as a scaffold for the assembly of complexes that regulate gene transcription. Bromodomain inhibitors (I-BET) selectively inhibit the transcription of a subset of inflammatory genes in macrophages following toll-like receptor stimulation. Since MNPs make a key contribution to antibody-mediated pathology, we sought to determine the extent to which I-BET inhibits macrophage and DC activation by IgG. We show that I-BET delays phagolysosome maturation associated with build-up of immune complex (IC) whilst selectively inhibiting IC induced cytokine production. I-BET changed MNP morphology, resulting in a less adherent phenotype, prompting an assessment of its impact on DC migration. In vitro, in a three-dimensional collagen matrix, IgG-IC induced augmentation of DC chemotaxis to chemokine (C-C motif) ligand 19 (CCL19) was abrogated by the addition of I-BET. In vivo, two photon imaging showed that systemic I-BET treatment reduced IC-induced dermal DC mobilisation. Tissue DCs and transferred DC also had reduced migration to draining lymph nodes following I-BET treatment. These observations provide mechanistic insight into the potential therapeutic benefit of I-BET in the setting of antibody-associated inflammation.
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Étude de la spécifité des lgA intestinales humaines / Study of human intestinal IgA specificitySterlin, Delphine 30 January 2018 (has links)
Acteur clé de la symbiose hôte-microbiote, les IgA sécrétoires modulent le microbiote et participe à l'homéostasie intestinale. Chez la souris, les IgA sont polyréactives, en reconnaissent diverses bactéries, elles régulent la composition du microbiote et réduisent l'inflammation intestinale. Ces observations ouvrent des perspectives thérapeutiques intéressantes. Cependant, les caractéristiques des IgA et leurs spécificités restent mal connues chez l'homme. L'objectif de ce travail a donc été d'étudier la spécificité de la réponse IgA, en distinguant IgA1 et IgA2. La mise au point d'une technique de production in vitro d'IgA monoclonales 100% humaines issues de l'intestin nous a permis de montrer le profil de polyréactivité des IgA. Chaque IgA interagit avec un spectre large mais défini de bactéries commensales. Par ailleurs, les IgA1 et les IgA2 ciblent la même fraction du microbiote. Les réponses IgA1 et IgA2 convergent aussi au niveau des épitopes polysaccharidiques reconnus. Si les IgA sécrétoires contribuent largement à l’homéostasie intestinale, des IgG sériques anti-microbiote jouent un rôle dans la relation symbiotique hôte-microbiote. Leur présence n’ayant pas encore été démontrée chez l’homme en condition physiologique, ce travail a eu pour objectif secondaire de les explorer. Le développement d’une technique de cytométrie bactérienne nous a permis de détecter des IgG ciblant les bactéries commensales dans le sérum des individus sains. Ces IgG anti-microbiote sont dirigées vers les bactéries déjà reconnues par les IgA sécrétoires, elles présentent des spécificités propres à chaque individu. / IgA, the dominant immunoglobulin produced in the gut, plays diverse roles ranging from toxin neutralization, immune functions regulation, intestinal homeostasis maintenance. It is now well established that polyreactive IgA, which target multiple bacteria, can modulate gut microbiota composition and have promising therapeutic effects. However, IgA features remain elusive in humans. We therefore determined the reactivity profile of native monoclonal antibodies from human colon and compared IgA1 and IgA2. We found that IgA are polyreactive and bind a diverse but restricted subset of gut commensals. Most commensals were dually coated by IgA1 and IgA2, yet IgA2 alone coated a distinct fraction of colonic bacteria. Besides their common microbial targets, IgA1 and IgA2 exhibited overlapping anti-carbohydrate repertoires. An essential link between IgA and IgG responses against microbiota has been recently demonstrated in mice. Nevertheless, it remains unclear whether symbiotic bacteria could induce systemic IgG under homeostatic conditions in humans. Hence, we characterized anti-microbiota IgG in serum of healthy donors by bacterial flow cytometry. We found that each individual harbored a diverse and private panel of anti-commensals IgG that converge with secretory IgA to cover a restricted fraction of the gut microbiota. Patients with IgA deficiency or common variable immunodeficiency (CVID) exhibited a distinct set of anti-commensals IgG suggesting that IgA replacement in addition to polyvalent IgG might be beneficial to treat gastro-intestinal symptoms in these patients.
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Genetische und erworbene thrombophile Gerinnungsstörungen als Quelle chronischer Schmerzsyndrome / Inherited and acquired blood coagulation disorders as a source of chronic pain syndromesSchwab, Marco January 2012 (has links) (PDF)
Anhand einer umfassenden Falldarstellung einer jungen Patientin mit einem lebensbedrohlichen Gesichtsschmerzsyndrom, das nach septischer Thrombose der periorbitalen venösen und arteriellen Gefäße aufgetreten war, wurde die Bedeutung einer medikamentösen Antikoagulation für die erfolgreiche Schmerztherapie herausgearbeitet. An diesem Fallbeispiel konnte aber auch gezeigt werden, dass keine sicheren Parameter für die Indikation einer solchen Gerinnungstherapie vorlagen. Die Bedeutung dieses Falls lag unzweifelhaft in der Erkenntnis, dass in einer anhaltenden Aktivierung des Kontaktsystems der Gerinnung ein bislang unterschätztes Potential für die Entstehung und Unterhaltung ungeklärter Schmerzen liegen könnte und nicht zuletzt auch daran, dass sich diese ätiologische Komponente in der Komplexität der Erkrankung diagnostisch nicht eindeutig sichern ließ. Mit der Translokation von LPS aus der intestinalen Mukosa in endothelial vorgeschädigte Gefäßabschnitte wurde eine Hypothese vorgetragen, die neben einer schwer detektierbaren inflammatorischen Komponente auch das prokoagulatorische Potential der Schmerzentstehung erklären könnte. Die prokoagulatorische Komponente dieses hypothetischen Entstehungs-mechanismus chronischer Schmerzen müsste, so die Arbeitshypothese, umso dominanter sein, wenn prokoagulatorisch wirksame genetische Faktoren bei den Patienten hinzukommen. Unter der Annahme, dass eine solche zusätzliche Diathese nicht nur eine Schrittmacherfunktion haben, sondern auch einen diagnostischen Beitrag liefern könnte, wurde dieses diagnostische Pilotprojekt mit der empirisch begründeten Heparintherapie von 97 Schmerzpatienten verbunden. Alle Pa-tienten wurden mit dem niedermolekularen Heparin Enoxaparin behandelt und nach zehn Behandlungstagen in vier verschiedene Respondergruppen (Gruppe 1 bis 4) eingeteilt. Diese Gruppen wurden auf fünf prothrombotische Parameter untersucht. Dazu wurden die Allelprävalenzen des Plasminogen Aktivator Inhibitor-(PAI-1 4G/5G) Polymorphismus, der Faktor V-Leiden-Mutation, der Prothrombin (G20210A) Genmutation sowie die Prävalenzen der Hyperfibrinogenämie und des Protein S-Mangels ermittelt. Mit Hilfe des exakten Fisher Tests wurden jeweils die Allelprävalenzen und Parameter sowohl der Respondergruppen 1 bis 3 mit einem Kollektiv der Allgemeinbevölkerung als auch mit dem Kollektiv der Non-Responder (Gruppe 4) verglichen. Die Prävalenz des Allels A der Faktor V-Leiden-Mutation G1691A war im Enoxaparin-Kollektiv bei den Respondern der Gruppen 1 bis 3 im Vergleich zur Allgemeinbevölkerung und zur Non-Respondergruppe (Gruppe 4) signifikant erhöht. Die Allelprävalenzen und Parameter der übrigen prokoagulatorischen Faktoren unterschieden sich von denen der Kontrollgruppen nicht. Anhand des Kallikrein-Kinin-Systems als möglichem Effektor des Hämosta-sesystems konnten Hinweise auf die kausale Wirksamkeit des nieder-molekularen Heparins Enoxaparin bei der Behandlung chronischer Schmerzen gegeben werden. / We showed that low molecular heparins (enoxaparin) may help as a remedy in chronic pain syndromes. In our findings the inherited disorder Factor V Leiden was significantly higher in patients with chronic pain that had a benefit from enoxaparin in comparison to non-responders and to common population. The effect was proven by the Kallikrein-kinin-system.
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Quantification of Protein Adhesion Strength to Surface Attached Poly (N- isopropylacrylamide) Networks by Hydrodynamic Detachment Shear StressesSanden, Gulnur 04 November 2014 (has links)
Stimuli responsive coatings offer a versatile method by which to manipulate interfacial interactions of proteins in a desired way. However, there exists little guidance as to how the structure of a responsive polymer coating influences adsorption of proteins. In this dissertation, the adsorption behavior of immuglobulin G (IgG) on poly (N-isopropylacryamide) (PNIPAAm) hydrogel coatings was investigated as a function of film thickness. PNIPAAm exhibits a hydrophilic to hydrophobic transition above a critical temperature of ~32°C in aqueous solutions. In this research, through the use of quartz crystal microbalance with dissipation (QCM-D) it was observed that the adsorption was thickness dependent and became non-reversible as the temperature was decreased. Interestingly, QCM-D results also suggested a similar amount of protein adsorption on both hydrated and dehydrated PNIPAAm surfaces. A rigid film analysis using Sauerbrey equation revealed a multi-layer formation on the collapsed PNIPAAm coatings. Although it is allegedly reported that PNIPAAm favors adsorption above the critical temperature due to hydrophobic interactions, there have been several studies that reported adsorption of proteins below the critical temperature. To better understand the QCM-D results, hydrodynamic shear force assays in a spinning disk configuration were performed in order to quickly measure and quantify adhesion of polystyrene (PS) probe spheres (10μm) to the PNIPAAm coatings in both the solvated (hydrophilic) and collapsed (hydrophobic) state. The influence of polymer coating thickness, polymer chain cross-link density, microsphere concentration and adsorption time on the adhesion characteristics of the coatings was investigated in relation with volume phase transition of the polymer coatings.
A series of experiments on quantification of the temperature dependent adhesion of proteins adsorbed on surface attached PNIPAAm coatings of thicknesses was performed as the surface chemistry was switched from hydrophilic to hydrophobic. First, adhesion of polystyrene (PS) microspheres on PNIPAAm coatings was quantified in order to have a guideline for temperature dependent adhesion performance of these coatings. PS particles were subjected to a range of detachment shear stresses through hydrodynamic flow in a spinning disk configuration. These experiments provide an indirect method to determine the force of adhesion since it is proportional to the hydrodynamic force. Model protein, IgG, was then linked to PS microspheres and the mean adhesion strength of the IgG coated PS microspheres were determined through the detachment shear stresses. The influence of PS deposition time, PS bead concentration, PNIPAAm coating thickness and PNIPAAm cross-link density on the adhesion strength were addressed. The results indicated that in the collapsed state, the adhesion of bare hydrophobic PS microspheres depends strongly on coating thickness. For hydrophilic charged PS microspheres the adhesion was always higher on the hydrated PNIPAAm surfaces and appeared not to be strongly affected by the increase in PNIPAAm coating thickness. The adhesion of IgG was higher on the collapsed PNIPAAm surfaces and the adhesion trend did not significantly change as the PNIPAAm film thickness was increased. For PNIPAAm coatings with the cross-link density reduced by factor of 10, the adhesion was again higher on the collapsed PNIPAAm surface and scaled linearly with thickness. Moreover, the influence of thickness became prominent at the higher thickness values (165 nm-185 nm). In addition, the adhesion of carboxylated microspheres on PNIPAAm did not reach equilibrium and increased linearly with microsphere deposition time.
A study on the sensing characteristics of PNIPAAm coatings in response to heavy metal ions was also conducted in this dissertation. The temperature-dependent swelling behavior of poly(N-isopropylacrylamide) and tripeptide Gly-Gly-His/poly(NIPAAm) conjugate hydrogel coatings were investigated using a quartz crystal microbalance with dissipation (QCM-D) while in contact with NaCl, ZnCl2, NiCl2, and CuCl2 solutions. To fabricate the tripeptide conjugated gels, precursor gels of poly(NIPAAm-co-3-aminopropylmethacrylamide[3.5 mole%]) were synthesized via free radical polymerization. The metal binding tripeptide, Gly-Gly-His, was subsequently synthesized in the gel via a Merrifield solid phase peptide synthesis (SPPS) technique, in which the amino group of the copolymer gel provided a functional site to support peptide synthesis. It was found that the logarithm of the transition temperature of the tripeptide Gly-Gly-His/poly(NIPAAm) conjugate hydrogel was proportional to the ionic strength, showing two distinct regions at low and high ionic strengths for the divalent ions. In the low ionic strength regime, the salting out constants were 0.08 M-1, 0.07 M-1, and 0.06 M-1 for Cu2+, Ni2+, and Zn2+, respectively, which follows the known trend for binding of the ions to Gly-Gly-His. In the high ionic strength region, when the metal-ion binding sites in the tripeptide conjugate hydrogel were saturated, the salting out constants were similar to the salting out constants associated with pure poly(NIPAAm).
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Functions of the Cholinergic System in the Morbidities Associated with Alzheimer’s Disease and the Further Evaluation of Tools for the Molecular Imaging of this SystemQuinlivan, Mitchell Owen Jeffrey January 2007 (has links)
Doctor of Philosophy(PhD) / The aims of this project were to contribute to the elucidation of the role of the cholinergic system in attention and memory, two cognitive processes severely compromised in Alzheimer’s disease (AD), and to evaluate and develop tools for the functional molecular imaging of this system with a view to improving knowledge of AD and other neurological disorders. Towards the first aim, the specific anti-cholinergic toxin 192 IgG-saporin (SAP) was administered to female Sprague-Dawley rats via either an intracerebroventricular (icv) or an intracortical route and animals were tested with a vibrissal-stimulation reaction-time task and an object recognition task to evaluate their attentional and mnemonic function, respectively. The second aim was approached in two ways. Firstly, relative neuronal densities from animals with icv lesions were assessed with both ex vivo and in vitro autoradiography with the specific cholinergic radiopharmaceuticals [123I]iodobenzovesamicol (123IBVM) and 125I-A-85380, ligands for the vesicular acetylcholine transporter and the nicotinic acetylcholine receptor, respectively. Secondly, a number of in vivo and in vitro studies were performed on a novel and unique molecular imaging system (TOHR), with which it had been hoped initially to image eventually SAP-lesioned animals, with a view to measuring and ameliorating its performance characteristics and assessing its in-principle suitability for small-animal molecular imaging. The behavioural studies support a critical role for the cholinergic system in normal attentional function. Additionally, in accord with literature evidence, no significant impairment was observed in mnemonic function. It is postulated however that the results observed in the intracortically-lesioned animals support the published hypothesis that cholinergic projections to the perirhinal cortex are critical for object-recognition memory. In autoradiographic studies, SAP-lesioned animals demonstrated reduced uptake of 123IBVM in multiple regions. A reduction of nicotinic receptors was also seen in SAP-lesioned animals, a novel finding supportive of the excellent characteristics of radioiodinated I-A-85380. Examination of the performance characteristics of the TOHR support in principle its utility for targeted small-animal molecular imaging studies.
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