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Method of histopathology-ultrasound association as a pedagogical strategy for medical students in the identification of the halo signGuillen Astete, Carlos Antonio, Salvador Saenz, Belén, Henriquez Camacho, César, Lores Seijas, Fernando 01 January 2020 (has links)
Introduction: There are no validated strategies in the teaching of ultrasound as a diagnostic tool in undergraduate medicine students. Given the role that ultrasound plays in the diagnostic capacity of any clinician is currently undeniable, a teaching method is proposed based on the demonstration of the association between the histopathology of a large vessel vasculitis and the characteristic ultrasound finding, known as the «halo sign». Methods: The teaching strategy was imparted by means of a 10-minute video presentation. Twenty-one final-year students from a single medical school participated in a concordance study and a validation test, identifying images corresponding to the halo sign in 120 different cases. The overall sensitivity, specificity and likelihood ratio of the students were also determined. Results: The overall concordance test had a kappa coefficient of 0.749 (SD: 0.11). The kappa concordance was 0.76 with dynamic images, and 0.84 with cross-sectional slices. The overall sensitivity was 89.7%, and the positive predictive value was 92.3%. The likelihood ratio achieved was 7.28. Conclusions: It has been shown that the application of this pedagogical method is useful in teaching the identification of an ultrasound sign to medical students. This study also suggests conditions that could be useful to improve between-observer agreement in both teaching scenarios and multiple observer scientific studies. / Revisión por pares
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Risk factors, coronary artery disease and mortality in giant cell arteritis: a population-based studyTómasson, Gunnar 08 April 2016 (has links)
Giant Cell arteritis (GCA) is a systemic inflammatory disease that affects arteries
of medium- and large size. Symptoms of GCA such as headache and fever
usually promptly improve with treatment of glucocorticoids. Apart from advanced
age, female sex and Northern-European descent, risk factors for GCA are
unknown. Most studies have found that life expectancy for patients with GCA is
not reduced compared with the general population and studies on cardiovascular
disease in GCA have provided conflicting results.
Data for the studies of this thesis are drawn from the Reykjavik Study (RS) that is
a general population-based cohort study with continuous surveillance for
coronary heart disease and vital status. Subjects born in 1907–1934 and living in
Reykjavik, Iceland or adjacent communities in 1966 were invited for study visit
from 1967-1994. Information on cardiovascular risk factors were collected at
study visit. Diagnosis of GCA for this study was based on re-examination of all
temporal arteries biopsies (TAB) from members of the RS cohort; however,
information was also obtained from the original pathology report.
Of 19,360 subjects included in the RS, 194 developed GCA during the follow-up
period. Body mass index was inversely associated with the occurrence of GCA.
Among men, but not women, hypertension was associated and smoking
inversely associated with the occurrence of GCA. Among women, but not men,
GCA was associated with coronary heart disease. Subjects with GCA had
approximately 50% increase in mortality risk compared with the general
population. Increase mortality was mainly observed among GCA patients based
on the diagnosis of re-examination of TAB; however, no such an association was
found if diagnosis of GCA was made based on the original pathology report.
Those subjects were likely not clinically diagnosed with GCA, signaling that
treatment for GCA might be beneficial with respect to mortality risk.
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Acute Bilateral Ischemia of Fingers: An Unusual Complication of Temporal ArteritisJithpratuck, Warit, Wason, William M., Elshenawy, Yasmin 01 November 2010 (has links)
We describe the case of a patient with documented temporal arteritis, who presented two years into her course with acute digital ischemia, presumed secondary to small vessel vasculitis. To our knowledge, this complication of temporal arteritis has not been previously reported.
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Cardiovascular Outcomes and In-Hospital Mortality in Giant Cell ArteritisMolloy, Eamonn S. 07 July 2008 (has links)
No description available.
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Etude de la réponse immunitaire T au cours de l'artérite à cellules géantes (Maladie de Horton) / Study of the T-cell immune response in giant cell arteritisSamson, Maxime 23 October 2014 (has links)
Ce travail de thèse a été axé sur l’étude de la réponse immunitaire T chez des patients atteints d’artérite à cellules géantes (ACG) et de pseudo-polyarthrite rhizomélique (PPR). Plusieurs études cliniques successives interrégionales ont permis d’inclure de nombreux patients (57 ACG et 27 PPR) des Centres Hospitaliers (CH) Universitaires et des CH de l’interrégion Est. Les échantillons sanguins ont été étudiés dans le laboratoire de l’unité INSERM U1098. Tout d’abord, nous avons confirmé l’implication des lymphocytes Th17 dans la pathogénie de l’ACG et avons montré pour la première fois leur implication au cours de la PPR. De plus, notre étude des lymphocytes T (LT) CD4+CD161+ a permis de mieux comprendre les mécanismes de plasticité entre les réponses Th1 et Th17 au cours de ces deux pathologies. Nous avons complété ces travaux par l’étude de la réponse T régulatrice en montrant qu’il existe un déficit quantitatif en Treg au cours de l’ACG et la PPR. Dans la suite de ce travail, nous avons mis en évidence, chez des patients atteints de polyarthrite rhumatoïde, que le blocage de la voie de signalisation de l’IL-6 par un anticorps monoclonal dirigé contre le récepteur de l’IL-6 permet de corriger le déséquilibre de la balance Th17/Treg, en diminuant la réponse Th17 et en augmentant simultanément la réponse T régulatrice, à l’inverse des corticoïdes qui diminuent le pourcentage de Th17 sans corriger le déficit en Treg. Enfin, dans la dernière partie de ce travail, nous avons montré pour la première fois que les LT CD8+ étaient également impliqués dans la pathogénie de l’ACG et la PPR. Ces résultats ont permis de progresser dans les connaissances physiopathologiques de l’ACG et la PPR en évoluant d’un modèle articulé autour d’un déséquilibre de la balance Th1/Th2 vers celui d’un déséquilibre de la balance Th17/Treg et permettent de proposer des thérapeutiques mieux ciblées pour l’ACG et la PPR. / The aim of this thesis was to investigate the T-cell immune response in the course of giant-cell arteritis (GCA) and polymyalgia rheumatica (PMR). Several studies conducted by our team allowed us to obtain blood samples from many patients affected by GCA (n=57) and PMR (n=28). Immunological studies were performed in INSERM U1098, University Of Burgundy, Dijon, France. We firstly demonstrated the implication of Th17 and CD4+CD161+ T cells in the pathogenesis of these two diseases, thus extending the knowledge in the plasticity mechanisms arising between Th1 and Th17 cell-immune responses in GCA and PMR. Furthermore, we investigated the regulatory T cell immune response in these two affections, demonstrating that although being functional, the percentage of circulating Treg was decreased in GCA and PMR patients. As interleukin-6 (IL-6) had been shown to control the Th17/Treg balance, we studied Th17 and Treg frequencies in rheumatoid arthritis patients treated with an anti-IL-6 receptor antibody (tocilizumab). We showed that the blockade of the IL-6 pathway was able to correct the Th17/Treg imbalance by decreasing the number of Th17 cells and simultaneously increasing that of Treg. Finally, we demonstrated for the first time the implication of CD8+ T cells in the pathogenesis of GCA and PMR. This thesis allowed us to progress in the knowledge of the pathogenesis of GCA making the pathogenesis model progress from a Th1/Th2 to a Th17/Treg imbalance model. Altogether, these data deciphering the immune response in the pathogenesis of GCA and PMR bring new knowledge which will lead to better targeted therapies.
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Étude du rôle des cellules musculaires lisses vasculaires (CMLV) et des anticorps anti-CMLV dans la pathogénie de l’artérite à cellules géantes (maladie de Horton) / Role of vascular smooth muscle cells (VSMC) and anti-VSMC antibodies in the pathogenesis of giant cell arteritisRégent, Alexis 10 November 2014 (has links)
Rationnel : L’artérite à cellules géantes (ACG) est une vascularite primitive des gros vaisseaux dont le diagnostic repose sur la mise en évidence d’un infiltrat inflammatoire et de cellules géantes à la biopsie d’artère temporale (BAT). On note également un remodelage de la paroi vasculaire lié à une prolifération des cellules musculaires lisses vasculaires (CMLV) pouvant aboutir à une occlusion artérielle. Objectif : Caractériser les auto-anticorps dirigés contre les cellules endothéliales (CE) et les CMLV au cours de l’ACG et préciser le rôle des CMLV dans le remodelage pariétal. Méthodes : La recherche d’auto-anticorps a reposé sur un immunoblot 2D couplé à la spectrométrie de masse. Les protéomes des CMLV d’artère ombilicale, d’artère pulmonaire et d’aorte humaines normales a été comparés par protéomique différentielle (2D-DIGE). Nous avons utilisé la 2D-DIGE et des puces d’expression pan-génomiques pour comparer les CMLV issues de BAT de patients suspects d’ACG (avec un diagnostic final d’ACG ou non), afin d’identifier les mécanismes contribuant à la prolifération des CMLV. Résultats : Chez 15 patients atteints d’ACG, nous avons notamment identifié la lamine, la vinculine et l’annexine A5 comme cible des auto-anticorps anti-CMLV. Les antigènes cibles identifiés sont liés à Grb2, une protéine adaptatrice impliquée dans la prolifération des CMLV. Nous avons mis en évidence des protéomes différents au sein des CMLV humaines normales selon leur origine vasculaire et avons principalement identifié des protéines du cytosquelette et du métabolisme énergétique.A partir des CMLV isolées des BAT et à l’aide d’Ingenuity®, nous avons identifié l’endothéline 1 (ET-1) et la paxilline comme des molécules impliquées dans le remodelage vasculaire. En immunohistochimie et par qPCR, nous avons confirmé l’expression de l’ET-1 et de ses récepteurs ETAR et ETBR au sein des artères temporales de patients atteints d’ACG. Enfin, nous avons inhibé la prolifération des CMLV avec du macitentan, un inhibiteur d’ETAR et en particulier avec son métabolite actif, mais pas avec d’autres inhibiteurs des récepteurs de l’ET-1. Conclusion : Nous avons identifié chez les patients atteints d’ACG des anticorps anti-CMLV dont le rôle pathogéne potentiel reste à définir. Les différences protéiques observées à partir des CMLV humaines normales pourraient correspondre à des phénotypes différents. A partir d’un matériel biologique unique, nous avons pu montrer que la prolifération excessive des CMLV au cours de l’ACG pouvait être inhibée par le macitentan ce qui permet d’envisager un usage thérapeutique de cette molécule. / Background : Giant cell arteritis (GCA) is a large vessel vasculitis and its diagnosis usually relies on the identification of an inflammatory infiltrate made of mononuclear cells and giant cells upon temporal artery biopsy. There is also a remodeling process in the arterial wall due to an excessive proliferation of vascular smooth muscle cells (VSMC) which can sometimes lead to arterial occlusion. Purpose: Identify auto-antibodies targeting either endothelial cells (EC) and/or VSMC during GCA and better understand the role of VSMC in the remodeling process. Methods : Auto-antibodies were detected by a 2-dimensionnal immunoblot and their target antigens were identified by mass spectrometry. Proteoms of umbilical artery, pulmonary artery and aorta VSMC were compared by 2 dimension differential in gel electrophoresis (2D-DIGE). In order to identify mechanisms involved in VSMC proliferation in GCA, we used both 2D-DIGE and pan genomic chips in order to compare VSMC isolated at the time of temporal artery biopsy (TAB) from patients with a final diagnosis of GCA or another diagnosis. Results : In 15 patients with GCA, we identified lamin, vinculin and Annexin A5 as target antigens of anti-VSMC antibodies. Target antigens were linked with Grb2, an adaptator protein involved in VSMC proliferation. Normal VSMC originating from different vascular beds have differ in protein contents with differential expression of cytoskeleton and energy metabolism proteins. We compared VSMC from TAB with Ingenuity software and identified endothelin-1 (ET-1) and paxillin as proteins involved in vessel remodeling. We confirmed by immunohistichemistry and qPCR that ET-1 and its receptor ETAR and ETBR were expressed in temporal arteries from patients with GCA. Last, we reduced VSMC proliferation with Macitentan, an ETAR and ETBR antagonist and significantly inhibited VSMC proliferation with its active metabolite whereas other ET-1 inhibitors had no effect. Conclusion : We identified anti-VSMC auto-antibodies in patients with GCA. Their pathogenic role remains to be determined. Normal VSMC from different vascular locations differ in protein conten which might reflect different phenotypes and different properties. The escessive proliferation of VSMC from patients with GCA was inhibited by Macitentan. This drug might constitute a future therapeutic option.
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Stellenwert der [18F]Fluor-2´-Deoxyglucose ([18F] FDG)-PET bei der diagnostischen Abklärung entzündlicher Prozesse / evaluation of the importance of [18F]FDG-PET in the diagnosis of inflammatory diseasesGürocak, Osman 05 July 2011 (has links)
No description available.
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Klinischer Stellenwert der Time of Flight FDG-PET/CT bei entzündungsspezifischen Fragestellungen / Clinical value of Time of Flight FDG-PET/CT in detecting of infection and inflammationBraune, Isabell 26 January 2017 (has links)
No description available.
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