An investigation of the affects of typefaces upon reader's perception of the meanings of messages using the semantic differential testing technique /

Hofman, Veronica M.

January 1988

Thesis (M.S.)--Rochester Institute of Technology, 1988. / Typescript. Includes bibliographical references (leaves 74-76).

An alphabetical metamorphosis /

Granfield, Monica.

January 1990

Thesis (M.F.A.)--Rochester Institute of Technology, 1990. / Typescript. Includes bibliographical references (leaves 24-29).

Rôle de l'interleukine-33 dans des modèles expérimentaux d'inflammation chronique / Role of Interleukin-33 in experimental models of chronic inflammation

Khaleghparast Athari, Sara

17 November 2015

La polyarthrite rhumatoïde (PR) est une maladie inflammatoire chronique d’étiologie inconnue. Les mécanismes physiopathologiques de cette maladie mettent en jeu un réseau cellulaire et cytokinique dont l’étude permet de définir des cibles thérapeutiques potentielles. L’IL-33 est une cytokine impliquée dans plusieurs maladies inflammatoires mais son rôle dans l’inflammation chronique comme la PR reste peu étudié. L’objectif de ce travail a été d’étudier le rôle de l’IL-33 et son mode d’action dans deux modèles expérimentaux d’inflammation chronique, l’arthrite au collagène (AEC) et le psoriasis induit par l’imiquimod (IMQ) chez la souris. Nous avons montré pour la première fois que l’administration d’IL-33 recombinante pendant les phases précoce et tardive de l’AEC, permet d’inhiber presque totalement les signes cliniques de la maladie. Cet effet protecteur passe par le déclenchement d’une réponse immunitaire de type 2 y compris l'expansion des ILC2, des éosinophiles et des cellules Th2. En outre, nous avons démontré que l’administration d’IL-33 dans notre modèle induit l’expansion de lymphocytes T régulateurs ST2L+ et une activité suppressive accrue. Dans un second temps, nous avons démontré que malgré l’expression de l’IL-33 dans les articulations ou la peau de souris développant une AEC ou un psoriasis induit par imiquimod, l’IL-33 endogène n’est pas nécessaire pour le développement de ces deux pathologies. En outre, l’absence de cette cytokine ne modifie pas la réponse des lymphocytes T ni dans l’AEC et ni dans le psoriasis. L'ensemble de ces résultats suggère que cette cytokine n’est pas cruciale pour le développement de l'inflammation chronique, et que la mise au point de traitement ciblant l’axe IL-33 / ST2 doit être envisagée avec précautions. / Rheumatoid arthritis (RA) is a chronic inflammatory disease that is associated with severalmediators. The physiopathological mechanisms of this disease involve cellular and cytokinenetworks whose study helps to define potential therapeutic targets. IL-33 is a cytokine involved inmany inflammatory diseases although its role in chronic inflammation such as RA remainsunclear. The aim of this work is to study the role of IL-33 and its mode of action in twoexperimental models of chronic inflammation, collagen induced arthritis (CIA) and imiquimod(IMQ) induced psoriasis. First, we showed for that the administration of recombinant IL-33 duringthe early and late phases of CIA inhibits the clinical signs of the disease in mice C57BL/6. Thisprotective effect is associated with the response type 2 including expansion of ILC2, eosinophilsand Th2 cells. Furthermore, we demonstrated that access of IL-33 in our model induced TregST2L and promotes the acquisition of regulatory phenotypes of Tregs. These Tregs achieve animportant suppressive activity leading inhibition of CIA. Secondly, despite the expression of IL-33 in the joint and skin of mice with CIA and IMQ induced psoriasis, endogenous IL-33 is notnecessary for the development of these two chronic inflammation models. In addition, the absenceof this cytokine does not alter the T cell response in the CIA or psoriasis. [...]

Cellules lymphoïde type 2

Lymphoid cells type 2

Sulfide-poor platinum-group element deposits:a mineralogical approach with case studies and examples from the literature

Kaukonen, R. (Risto)

11 November 2008

Abstract Sulfide-poor deposits of platinum-group elements (PGE) occur in two main types: silicate-type and oxide-type. In the silicate-type mineralization PGE form discrete platinum-group minerals (PGM) that occur as inclusions in various silicate minerals. In the oxide-type mineralization PGM may have different modes of occurrence. They may be associated with silicates or they may occur as inclusions in chromite, magnetite or ilmenite, for example. In some cases they may even be associated with base metal sulfides. The approach chosen in this work is mainly a mineralogical one. PGM parageneses, their modes of occurrence and associations with other minerals were studied from different deposits. These are then compared to some well-recorded examples of PGE deposits. The case studies presented, the Duluth Complex in Minnesota, U.S.A., the Hanumalapur Complex in Karnataka, India, and the Penikat Layered Intrusion in northern Finland, are examples that illustrate the multitude of possibilities regarding PGE mineralization versus the traditional approach where any significant quantities of PGE are supposed to occur only in association with base metal sulfides. As the traditional orthomagmatic and hydrothermal models cannot explain the genesis of some sulfide-poor PGE occurrences, a new theory of PGE mineralization was developed. This “redox theory” is an attempt at explaining the association of PGE with various oxide minerals, most importantly chromite.

PGE

PGM

oxide-type

redox theory

silicate-type

sulfide-poor

Some properties of superconductors

French, Robin A.

January 1966

No description available.

The incidence of executive cognitive dysfunction detected by a bedside executive screening tool (BEST) in a cohort of type 2 diabetes attending a tertiary diabetic clinic

De Wet, Hayley Beryl

24 February 2011

MMed, Internal Medicine, Faculty of Health Sciences,University of the Witwatersrand / Aims: To determine whether impairment of the executive functioning domain of cognition could be detected by a battery of simple bedside cognitive tests of executive function associated with inadequate glycaemic control. Methods: People with type 2 diabetes attending a tertiary referral diabetic clinic who consented to participate in the study underwent a brief battery of cognitive testing (the Bedside Executive Screening Test) designed to detect executive function impairment. Glycaemic control was determined using glycated haemoglobin levels (HbA1c). Inadequate glycaemic control was defined as HbA1c ≥ 7.0%. Results: Executive function impairment was detected in 51 (52%) of the 98 study participants. The presence of executive function impairment was significantly associated with poor glycaemic control (HbA1c ≥ 7.0%) (odds ratio 4.9, 95% confidence interval 1.3 – 18.8, p=0.019). There were no significant differences between patients with and without executive function impairment with regard to age, target organ damage, patient reported adherence, and hypoglycaemic therapy. Patients with a lower level of education were more likely to demonstrate executive impairment when glycaemic control was poor (p=0.013). Conclusion: Executive function impairment is common in a population of people with difficult-to-manage type 2 diabetes. The presence of executive impairment is significantly associated with poor glycaemic control.

type 2 diabetes

type 2 diabetics

cognitive dysfunction

The comparison of periodontal health status and metabolic control in diabetic children and adolescents at Tygerberg hospital

Scholtz-Evans, Lèzaan

January 2021

Magister Chirurgiae Dentium (MChD) / Diabetes Mellitus (DM) is a well-known risk factor for Periodontal disease. Research has established that the prevalence of Periodontal disease is directly related to the glycaemic control of DM in adults and only a few research studies explore this prevalence in diabetic children and adolescents in South Africa. The aim of this study is to determine the periodontal health status of diabetic patients which include children and adolescents attending the Paediatric Diabetic Clinic at Tygerberg Hospital and compare periodontal status with diabetic control. cross-sectional study was employed to determine periodontal status and data relating to the HbA1c% level, the type and duration of DM, the body mass index (BMI) percentile, age, sex, and puberty and treatment regimens were collected from patient records and entered into data collection sheets.

Diabetes mellitus

Diabetic type 2

Diabetic type 1

Puberty

Adolescents

Détection et caractérisation moléculaire des rétrovirus d'origine simienne chez l'Homme : cas du virus foamy et du virus T-lymphotrope de type 4 / Detection and molecular characterization of retroviruses of simian origin in humans : foamy virus and T-lymphotropic virus type 4 cases

Richard, Léa

22 September 2016

Les primates non-humains (PNH) sont un important réservoir de pathogènes et notamment de rétrovirus. Plusieurs agents infectieux ont émergé dans la population humaine à partir de ce réservoir animal, comme par exemple le virus de l’immunodéficience humaine ou le virus T lymphotrope humain (HTLV) de type 1 qui se sont répandus mondialement et causent de graves pathologies. L’émergence de rétrovirus chez l’Homme nécessite plusieurs étapes passant par la transmission primaire du virus du PNH à l’Homme, la persistance du virus dans l’organisme,la transmission secondaire inter-humaine et enfin sa diffusion dans la population. Mes deux projets de thèse ont porté sur l’étude de deux rétrovirus qui ont un potentiel d’émergence chez l’Homme, le virus foamy simien (SFV) et le virus T-lymphotrope de type 4, dans des cohortes d’individus à risque vivant au Cameroun et au Gabon. Les SFV sont des rétrovirus ubiquitaires chez de nombreux PNH. Plus d’une centaine de cas d’infection d’humains par des SFV ont été observés à ce jour, l’origine étant un contact(principalement par morsure) avec un PNH. L’infection est chronique et semble asymptomatique.De plus, aucune transmission secondaire n’a été détectée à ce jour. Le laboratoire a pu isoler, chez deux individus camerounais, deux souches de SFV de gorille et a constaté une forte variabilité génétique au niveau du gène d’enveloppe. Nous avons donc étudié la variabilité du gène d’enveloppe de SFV de gorille mais également de chimpanzé infectant une soixantaine de chasseurs camerounais et gabonais et une trentaine de PNH. Nous avons pu mettre en évidence la co-circulation de souches de SFV présentant des variants moléculaires du gène d’enveloppe différents chez les gorilles et les chimpanzés. Ces mêmes souches peuvent être transmises à l’Homme à l’occasion de morsures, les deux variants pouvant être transmis simultanément. Ces variants diffèrent au niveau d’une région de 753 pb située dans la région codant la glycoprotéine de surface, au niveau du domaine de liaison au récepteur. Ils pourraient ainsi avoir des propriétés fonctionnelles différentes, notamment au niveau de l’élicitation de la réponse immunitaire de l’hôte. Ces variants sont potentiellement issus d’événements de recombinaison.HTLV-4 a été détecté chez un unique individu, un chasseur camerounais, aujourd’hui décédé.En 2014, le réservoir simien a été identifié comme étant les gorilles. Nous avons recherché la présence de HTLV-4 chez 300 individus camerounais et gabonais qui avaient été mordus par un PNH. Nous avons identifié deux chasseurs gabonais infectés par HTLV-4, qui avaient été mordus par des gorilles 9 à 15 ans avant d’être prélevés. Nous confirmons donc la présence de HTLV-4 infectant de manière persistante des humains et étendons sa répartition au Gabon. Nous suggérons très fortement une origine zoonotique de ces infections. L’une des souches isolées est divergente par rapport aux souches déjà connues et permet donc de définir le sous-type B deHTLV-4.Ces travaux confortent la notion que les PNH, et notamment les gorilles, sont une source importante d’agents infectieux pour l’Homme. Des études supplémentaires seront nécessaires pour mieux caractériser l’infection chez l’Homme et notamment l’éventuelle pathogénicité et transmissibilité de ces deux virus. / Non-human primates (NHPs) are an important reservoir of pathogens, including retroviruses. Several retroviruses have emerged in human population from NHP reservoir, like the human immunodeficiency virus and the human T-lymphotropic virus type 1 who have spread globally and are the causative agents of serious pathologies. During my PhD, I interested in two retroviruses who have an emerging potential in human population, the simian foamy virus (SFV) and the human T-lymphotropic virus type 4 (HTLV-4), in cohorts of individuals at risk in Central Africa. SFV are retroviruses ubiquituous in NHPs. A hundred of human infections with SFV are known, originating from contacts with NHP. The infection is chronic, asymptomatic although no secondary transmission has been observed yet. We showed that two envelope molecular variants of SFV are co-circulating in gorilla and chimpanzee populations. These strains can be transmitted to humans through bites. The variants differ in the receptor binding domain on the envelope and could have different functional properties. HTLV-4 had been detected in a single individual (a cameroonese hunter) and the simian reservoir idenfied as gorillas. We have detected two gabonese hunters infected with HTLV-4, who had been bitten by gorillas. Then we confirm the presence of HTLV-4 in humans in Central Africa. One of the strains is divergent and defines the prototype of a new subtype of HTLV-4

Virus T-lymphotrope de type 4

T-lymphotropic virus type 4

Investigating inherent functional differences between human cardiac fibroblasts cultured from non-diabetic and type 2 diabetic donors

Sedgwick, B., Riches-Suman, Kirsten, Bageghni, S.A., O'Regan, D.J., Porter, K.E., Turner, N.A.

26 March 2014

yes / Introduction Type 2 diabetes mellitus (T2DM) promotes adverse myocardial remodeling and increased risk of heart failure; effects that can occur independently of hypertension or coronary artery disease. As cardiac fibroblasts (CFs) are key effectors of myocardial remodeling, we investigated whether inherent phenotypic differences exist in CF derived from T2DM donors compared with cells from nondiabetic (ND) donors. Methods Cell morphology (cell area), proliferation (cell counting over 7-day period), insulin signaling [phospho-Akt and phospho-extracellular signal-regulated kinase (ERK) Western blotting], and mRNA expression of key remodeling genes [real-time reverse transcription-polymerase chain reaction (RT-PCR)] were compared in CF cultured from atrial tissue from 14 ND and 12 T2DM donors undergoing elective coronary artery bypass surgery. Results The major finding was that Type I collagen (COL1A1) mRNA levels were significantly elevated by twofold in cells derived from T2DM donors compared with those from ND donors; changes reflected at the protein level. T2DM cells had similar proliferation rates but a greater variation in cell size and a trend towards increased cell area compared with ND cells. Insulin-induced Akt and ERK phosphorylation were similar in the two cohorts of cells. Conclusion CF from T2DM individuals possess an inherent profibrotic phenotype that may help to explain the augmented cardiac fibrosis observed in diabetic patients.

Association of Glycemia with Cystatin C in Youth with Diabetes

Kanakatti Shankar, Roopa

08 October 2012

No description available.

Surgery

Cystatin C

Type 1 diabetes

Type 2 diabetes

Glycemia