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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 221 to 230 of 231 (0.035 seconds)
221

Le rôle des vésicules extracellulaires dans la dysfonction lymphatique liée à l’athérosclérose

Farhat, Maya 12 1900 (has links)
Toutes les cellules libèrent plusieurs types de vésicules extracellulaires (VEs) qui transportent protéines, lipides et acides nucléiques. Ces vésicules de petite taille se retrouvent dans tous les fluides biologiques tel que le sang et la lymphe et interagissent avec les cellules environnantes. Le système lymphatique constitue une voie de prédilection pour la mobilisation des accepteurs de cholestérol à partir de la paroi artérielle. Nous avons démontré dans un modèle murin qu’une dysfonction lymphatique précède la formation de la plaque d’athérome et que cette dysfonction touche a priori la capacité de contraction des vaisseaux collecteurs. À la base de toutes ces observations, nous avons émis l’hypothèse que les VEs contribuent à la dysfonction lymphatique liée à l’athérosclérose. Pour répondre à ceci, nous avons mis en place un projet translationnel composé de deux groupes de sujets sains, sans maladie cardiovasculaire, qui se distinguent par la présence d’antécédents familiaux d’accidents cardiovasculaires prématurés chez un parent du premier degré. Nous avons quantifié plusieurs sous-types d’intérêt de VEs en circulation à partir du plasma exempt de plaquettes, par cytométrie en flux ultraspécialisés dans la détection de petites particules (> 100 nm) combiné à d’autres techniques complémentaires standardisées. Ensuite, nous avons évalué la fonction lymphatique grâce à l’imagerie par proche infrarouge après injection du vert indocyanine (ICG). Nos résultats préliminaires sont prometteurs quant aux rôles des VEs et de la dysfonction lymphatique dans le développement de l’athérosclérose et corroborent avec nos observations faites chez la souris. Les sujets avec antécédents familiaux de maladie cardiovasculaire (MCV) présentent des signes de dysfonction lymphatique avant même l’apparition de plaques d’athérome subcliniques. La réponse mécano-sensible de leurs vaisseaux collecteurs paraît défectueuse et est observable de concert avec un profil de VEs qui présument une atteinte lymphatique. Ces résultats restent à être confirmer avec le recrutement de sujets additionnels et l'évaluation de la corrélation avec le score de risque polygénique de développer une MCV, dans l’objectif ultime de faire des VEs et de la fonction lymphatique de nouveaux biomarqueurs dans l’identification précoce des MCV. / All cell types release extracellular vesicles (EVs) that carry different types of cellular cargo, such as proteins, lipids and nucleic acids. These small vesicles are found in all biological fluids including blood and lymph and can interact with neighboring cells. The lymphatic system is a preferred route for the mobilization of cholesterol from the arterial wall. We have demonstrated in a mouse model that lymphatic dysfunction precedes the development of atherosclerosis and that that this dysfunction affects the contraction capacity of the collecting vessels. Based on these observations, we hypothesized that EVs contribute to atherosclerosis-associated lymphatic dysfunction. Therefore, we have initiated a translational study involving two groups of healthy subjects that differ in their risk of cardiovascular disease (CVD). We quantified several subtypes of circulating EVs on platelet-free plasma by ultraspecialized flow cytometry in the detection of small particles (> 100 nm) combined to other state-of-the art complementary techniques. Next, we assessed the lymphatic function using near-infrared imaging and injection of indocyanine green (ICG). Our preliminary results are promising for the role of EVs and lymphatic dysfunction in the development of atherosclerosis and corroborate with our observations made in mice. Individuals at high risk of CVD have signs of lymphatic dysfunction even before the onset of subclinical atherosclerosis. The mechano-sensitive response of their collecting vessels appears to be defective and is observable in concert with a profile of EVs that presume lymphatic damage. These results remain to be confirmed with the recruitment of additional subjects and the assessment of the correlation with the polygenic risk score of developing a CVD, in the hope of making these specific EV subsets and lymphatic function new biomarkers in the early detection of CVD.
Vésicules extracellulaires
Système lymphatique
Athérosclérose
Cytométrie en flux
Maladie cardiovasculaire
Imagerie proche infrarouge
extracellular vesicles
Lymphatic system
Atherosclerosis
Flow cytometry
Cardiovascular diseases
Infrared imaging
222

Transport and lymphatic uptake of monoclonal antibodies after subcutaneous injection

Ehsan Rahimi (11892065) 02 August 2023 (has links)
<p>The subcutaneous injection has emerged as a common approach for self-administration of biotherapeutics due to the patient comfort and cost-effectiveness. However, the available knowledge about transport and absorption of these agents after subcutaneous injection is limited. Here we aim to find drug distribution in the tissue and lymphatic uptake after subcutaneous (SC) injection. In the first part of the study, a mathematical framework to study the subcutaneous drug delivery from injection to lymphatic uptake is presented. A three-dimensional poroelastic model is exploited to find the biomechanical response of the tissue by taking into account tissue deformation during the injection. The results show that including tissue deformability noticeably changes tissue poromechanical response due to the significant dependence of interstitial pressure on tissue deformation. Moreover, the importance of the amount of lymph fluid at the injection site and injection rate on the drug uptake to lymphatic capillaries is highlighted. Finally, the variability of lymphatic uptake due to uncertainty in parameters, including tissue poromechanical and lymphatic absorption parameters, is evaluated. It is found that interstitial pressure due to injection is the major contributing factor in short-term lymphatic absorption, while the amount of lymph fluid at the site of injection determines the long-term absorption of the drug. Finally, it is shown that the lymphatic uptake results are consistent with experimental data available in the literature.</p><p>In the second part, drug transport and distribution in different tissue layers are studied. A single-layer model of the tissue as a base study was first explored. During injection, the difference between the permeability of the solvent and solute results in a higher drug concentration proportional to the inverse of the permeability ratio. Then the effects of layered tissue properties with primary layers, including epidermis, dermis, subcutaneous, and muscle layers, on tissue biomechanical response to injection and drug transport are studied. The drug distributes mainly in the SQ layer due to its lower elastic moduli. Finally, the effect of secondary tissue elements like the deep fascia layer and the network of septa fibers inside the SQ tissue is investigated. The Voronoi algorithm is exploited to create random geometry of the septa network. It is shown how drug molecules accumulate around these tissue components as observed in experimental SC injection. Next, the effect of injection rate on drug concentration is studied. Higher injection rates slightly increase the drug concentration around septa fibers. Finally, it is demonstrated that the concentration-dependent viscosity increases the concentration of biotherapeutics in the direction of septa fibers.</p><p>In the third part of this thesis, a poro-hyperelastic model of the tissue is exploited to find the biomechanical response of the tissue together with a transport model based on an advection-diffusion equation in large-deformation poro-hyperelastic Media. The process of mAbs transport to the lymphatic system is explored. This process has two major parts. First, the initial phase, where mAbs are dispersed in the tissue as a result of momentum exerted by injection. This stage last for only a few minutes after the injection. Then there is the second stage, which can take tens of hours, and as a result, monoclonal antibodies (mAbs) molecules are transported from the subcutaneous layer towards initial lymphatics in the dermis to enter the lymphatic system. In third chapter, both stages are studied. The process of plume formation, interstitial pressure, and velocity development is explored. Then the effect of the injection device, injection site, and sensitivity of long-term lymphatic uptake due to variability in permeability, diffusivity, viscosity, and binding of mAbs are investigated. Then the results are used to find an equivalent lymphatic uptake coefficient that is widely used in pharmacokinetic (PK) models to study the absorption of mAbs. We show that the injection rate is the least, and the injection site is the most important parameter in the uptake of mAbs. Injection depth and mAbs dose also significantly alter lymphatic absorption. Finally, the computational model is validated against experimental studies available in the literature.</p>
Mechanobiology
Bio-fluids
Biomedical fluid mechanics
Drug delivery
Lymphatic absorption.
Drug transport in tissue
Subcutanous administration
poroelastic model of the soft tissue
223

Struktur und Funktion der 20S Proteasomen aus Organen Listeria monocytogenes infizierter Mäuse

Strehl, Britta Katharina 28 June 2005 (has links)
Das Proteasomensystem der Zelle ist für die Degradation von Proteinen verantwortlich und spielt eine zentrale Rolle bei der Generierung von Epitopen, die auf MHC-Klasse-I Molekülen den cytotoxischen T-Lymphozyten (CTLs) präsentiert werden. Die Stimulation von Zellen mit Interferon-gamma (IFNgamma) führt zu der Bildung von Immunoproteasomen, die im Vergleich zu den konstitutiven Proteasomen eine verbesserte Generierung vieler MHC-Klasse-I Epitope aufweisen. In gesunden Mäusen werden Immunoproteasomen vorwiegend in den lymphatischen Geweben exprimiert, wohingegen nicht-lymphatische Gewebe hauptsächlich konstitutive Proteasomen enthalten. In der vorliegenden Arbeit wurde der Einfluss der Listeria monocytogenes Infektion auf die aus der Leber, der Milz, dem Dünndarm und dem Colon stammenden murinen 20S Proteasomen untersucht. Die Struktur der isolierten 20S Proteasomen wurde mittels zweidimensionaler Gelelektrophorese und Westernblot ermittelt, während die Funktion durch in vitro Prozessierung von drei oligomeren Peptidsubstraten analysiert wurde. Die Prozessierungsprodukte wurden mittels HPLC-ESI-Ionenfalle massenspektrometrisch identifiziert sowie quantifiziert. Die vorliegende Arbeit zeigt zum ersten Mal, dass nach einer Infektion die aus den nicht-lymphatischen Organen und Zellen isolierten 20S Proteasomen eine strukturelle und funktionelle Plastizität aufweisen: Nach der Infektion wurde die Bildung von Immunoproteasomen induziert, was mit der gesteigerten Generierung der immunrelevanten Fragmente korreliert werden konnte. Dies verlief unabhängig von der direkten Präsenz von Listeria monocytogenes in den Organen und wurde ausschließlich durch das Cytokin IFNgamma reguliert. Es konnte außerdem eine Zunahme der posttranslationalen Modifikation von Leberproteasomen mit dem Monosaccharid N-Acetylglucosamin nach der Infektion nachgewiesen werden. Des Weiteren wurde eine detaillierte Analyse der massenspektrometrischen Daten hinsichtlich des Schnittverhaltens der konstitutiven und Immunoproteasomen etabliert. Die Auswertung ergab, dass die Immunoproteasomen nach der Infektion durch schnellere und veränderte Nutzung bestehender Spaltstellen an der verbesserten Epitoppräsentation beteiligt sind. / The proteasome system of the cell is responsible for the degradation of proteins and plays a central role in the generation of epitopes which are presented to cytotoxic T-lymphocytes (CTLs) on MHC-class-I molecules. The stimulation of cells by interferon-gamma (IFNgamma) leads to the formation of immunoproteasomes that show an improved generation of many MHC-class-I epitopes compared to constitutive proteasomes. In healthy mice, immunoproteasomes are mainly expressed in the lymphatic tissues, whereas the non-lymphatic organs predominantly contain constitutive proteasomes. In this project the effect of Listeria monocytogenes infection on murine 20S proteasomes derived from the liver, spleen, small intestine and colon were investigated. The structure of the isolated proteasomes was analyzed by two-dimensional gel electrophoresis and western blots while the function was studied by in vitro processing of three oligomeric peptide substrates. Identification and quantification of the processing products was performed by HPLC-ESI-ion trap mass spectrometry. The project showed for the first time, that after infection 20S proteasomes isolated from non-lymphatic organs as well as from non-lymphatic cells displayed structural and functional plasticity: immunoproteasomes were induced post infection which could be correlated with the enhanced generation of immuno-relevant fragments. This was independent of the direct presence of Listeria monocytogenes in the organs and solely controlled by the cytokine IFNgamma. In addition, an increased posttranslational modification with the monosaccharide N-acetylglucosamine could be detected in liver-derived proteasomes after infection. Furthermore, a detailed analysis of the mass spectrometry data was established according to the cleavage site usage of constitutive and immunoproteasomes. The result was that immunoproteasomes are involved in improved generation of the immuno-relevant fragments by the faster cleavage and the changed usage of existing cleavage sites after infection.
20S Proteasom
Immunoproteasom
Listeria monocytogenes
Mausmodell
lymphatische Organe
nicht-lymphatische Organe
IFNgamma
TNFalpha
Antigenprozessierung
MHC-Klasse-I Epitop
Antitop
LLO
Hsp60
pp89
HPLC-ESI-Ionenfalle
Massenspektrometrie
posttranslationale Modifikation
N-Acetylglucosamin
O-GlcNAc
20S proteasome
immunoproteasome
Listeria monocytogenes
mouse model
lymphatic organs
non-lymphatic organs
IFNgamma
TNFalpha
antigen processing
MHC-class-I epitope
antitope
LLO
Hsp60
pp89
HPLC-ESI-ion trap
mass spectrometry
posttranslational modification
N-acetylglucosamine
O-GlcNAc
570 Biowissenschaften, Biologie
32 Biologie
WC 6570
YD 5687
ddc:570
224

"Contribuição ao estudo da influência da radiação ionizante pré-operatória sobre a marcação do linfonodo sentinela do reto com azul patente: estudo experimental em ratos" / Contribution to the study of the influence of preoperative ionizing radiation on the identification of the sentinel lymph node with patent blue : an experimental study in rats

Fernandes, Margareth da Rocha 06 February 2006 (has links)
A radiação ionizante prévia promove alterações actínicas em tecidos peritumorais,o que poderia influenciar a demarcação do linfonodo sentinela.O presente estudo desenvolveu modelo experimental para demarcação do linfonodo sentinela do reto do rato e para definição da dose de radiação (curva de calibração). O objetivo foi avaliar a influência da radiação ionizante pré-operatória sobre a marcação, com corante azul patente, do linfonodo sentinela do reto de ratos. A amostra foi constituída por 40 ratos machos Wistar e dividida em 2 grupos:Grupo 1 (controle não irradiado; n = 20) e Grupo 2 (irradiado com 1200cGy e demarcado 2 dias após; n = 20). Foi observado aumento linear do tempo de coloração do linfonodo no Grupo 2. Concluindo,a irradiação pré-operatória não influiu na demarcação do linfonodo sentinela do reto do rato / Previous ionizing radiation induces actinic alterations in peritumoral tissues and thus might influence the localization of the sentinel lymph node. The present study developed an experimental model for the localization of the sentinel lymph node of the rectum of the rat and for the definition of the dose of radiation (calibration curve). The objective was to evaluate the influence of preoperative ionizing radiation on the staining of a patent blue dye in the sentinel lymph node of the rectum in rats.The sample was composed of 40 male Wistar rats and was divided in two groups: Group 1 (non-irradiated control; n = 20 ) and Group 2(irradiated with 1200cGy and stained 2 days afterwards; n = 20). It was observed a linear increase in the time for the staining of the lymph in Group 2.In conclusion, preoperative irradiation did not influence the staining of the sentinel lymph node of the rectum in rats
Biópsia de linfonodo sentinela/métodos
Dyes/diagnostic use
Linfonodo/cintilografia
Linfonodo/efeitos de radiação
Linfonodo/irrigação sangüínea
Lymph/radionuclide imaging
Lymphatic metastasis/diagnosis
Lymphatic metastasis/radiotherapy
Mapeamento por restrição/métodos
Metástase linfática/diagnóstico
Metástase linfática/radioterapia
Neoplasias retais/radioterapia
Radiação ionizante
Radiation ionizing
Ratos Wistar
Rats Wistar
Rectal neoplasms/blood supply
Rectal neoplasms/radioterapy
Restriction Mapping/methods
Sentinel lymph node biopsy/methods
Tinturas/uso diagnóstico
225

"Contribuição ao estudo da influência da radiação ionizante pré-operatória sobre a marcação do linfonodo sentinela do reto com azul patente: estudo experimental em ratos" / Contribution to the study of the influence of preoperative ionizing radiation on the identification of the sentinel lymph node with patent blue : an experimental study in rats

Margareth da Rocha Fernandes 06 February 2006 (has links)
A radiação ionizante prévia promove alterações actínicas em tecidos peritumorais,o que poderia influenciar a demarcação do linfonodo sentinela.O presente estudo desenvolveu modelo experimental para demarcação do linfonodo sentinela do reto do rato e para definição da dose de radiação (curva de calibração). O objetivo foi avaliar a influência da radiação ionizante pré-operatória sobre a marcação, com corante azul patente, do linfonodo sentinela do reto de ratos. A amostra foi constituída por 40 ratos machos Wistar e dividida em 2 grupos:Grupo 1 (controle não irradiado; n = 20) e Grupo 2 (irradiado com 1200cGy e demarcado 2 dias após; n = 20). Foi observado aumento linear do tempo de coloração do linfonodo no Grupo 2. Concluindo,a irradiação pré-operatória não influiu na demarcação do linfonodo sentinela do reto do rato / Previous ionizing radiation induces actinic alterations in peritumoral tissues and thus might influence the localization of the sentinel lymph node. The present study developed an experimental model for the localization of the sentinel lymph node of the rectum of the rat and for the definition of the dose of radiation (calibration curve). The objective was to evaluate the influence of preoperative ionizing radiation on the staining of a patent blue dye in the sentinel lymph node of the rectum in rats.The sample was composed of 40 male Wistar rats and was divided in two groups: Group 1 (non-irradiated control; n = 20 ) and Group 2(irradiated with 1200cGy and stained 2 days afterwards; n = 20). It was observed a linear increase in the time for the staining of the lymph in Group 2.In conclusion, preoperative irradiation did not influence the staining of the sentinel lymph node of the rectum in rats
Biópsia de linfonodo sentinela/métodos
Linfonodo/cintilografia
Linfonodo/efeitos de radiação
Linfonodo/irrigação sangüínea
Mapeamento por restrição/métodos
Metástase linfática/diagnóstico
Metástase linfática/radioterapia
Neoplasias retais/radioterapia
Radiação ionizante
Ratos Wistar
Tinturas/uso diagnóstico
Dyes/diagnostic use
Lymph/radionuclide imaging
Lymphatic metastasis/diagnosis
Lymphatic metastasis/radiotherapy
Radiation ionizing
Rats Wistar
Rectal neoplasms/blood supply
Rectal neoplasms/radioterapy
Restriction Mapping/methods
Sentinel lymph node biopsy/methods
226

Молекуларна и генска хетерогеност метастаза у аксиларним лимфним чворовима код пацијенткиња са инвазивним карциномом дојке / Molekularna i genska heterogenost metastaza u aksilarnim limfnim čvorovima kod pacijentkinja sa invazivnim karcinomom dojke / Molecular and genetic heterogeneity of axillary lymph node metastases in breast cancer patients

Baroš Ilija 21 June 2019 (has links)
<p>HER2 Gene-Protein Assay (GPA) је посебно погодан за истовремено процењивање експресије HER2 протеина и статуса амплификације HER2 гена на нивоу појединачних ћелија и њихово повезивање са ћелијском морфологијом. Циљ истраживања био је испитати да ли су постојећи критеријуми препоручени од стране ASCO/CAP довољни за дијагностиковање HER2 позитивности код пацијенткиња које показују интратуморску хетерогеност, како у примарним туморима тако и у метастазама у регионалне лимфне чворове, учесталост HER2 хетерогености у макрометастазама лоцираним у лимфним чворовима, те да ли постоји јасна корелација између хетерогености нађене у примарном тумору дојке и припадајућим метастазама у лимфним чворовима. Испитивање је обухватило 41 од планиране 51 пацијенткиње које су испуниле све критеријуме укључивања. Репрезентативни парафински блокови метастатских лимфних чворова одабрани су из архивираног материјала, обојени GPA методом и процењени у складу са критеријумима ASCO/CAP 2013. Анализирано је 120 ћелија у хистолошком резу сваког метастатског лимфног чвора. Статус HER2 се разликовао између примарног тумора и његових метастаза у 13,2% (5/38) случајева. Један случај HER2 позитивног примарног тумора имао је HER2 негативне метастазе, два додатна случаја са HER2 позитивним примарним тумором су имала метастазе са статусом граничне амплификације без прекомерне експресије HER2 протеина и два случаја са HER2 негативним примарним тумором су имала метастазе са статусом граничне амплификације без прекомерне експресије HER2 протеина. У 17.4% (4/23) случајева са HER2 не-амплификованим примарним тумором метастазе су постале граничне у статусу генске амплификације. Једна од четири метастазе HER2 негативног примарног тумора показала је мали фокус HER2 позитивних туморских ћелија (&lt;3% тумора). Микрохетерогеност је анализирана у 108 лимфних чворова код 38 пацијенткиња и уочена у 22 лимфна чвора, тј. код четири пацијенткиње у свим анализираним лимфним чворовима, док је код једне пацијенткиње од 4 анализирана лимфна чвора микрохетерогеност потврђена у једном лимфном чвору. На основу добијених резултата може се закључити да постојећи критеријуми препоручени од стране ASCO/CAP применом прихваћених метода нису довољни за дијагностиковање HER2 позитивности код пацијенткиња које показују интратуморску и интертуморску хетерогеност како у примарним туморима тако и у метастазама, те да постоји статистички високо сигнификантан број макрометастаза лоцираних у лимфним чворовима које показују HER2 хетерогеност и позитивна корелација између хетерогености нађене у примарним туморима и припадајућим метастазама у лимфним чворовима.</p> / <p>HER2 Gene-Protein Assay (GPA) je posebno pogodan za istovremeno procenjivanje ekspresije HER2 proteina i statusa amplifikacije HER2 gena na nivou pojedinačnih ćelija i njihovo povezivanje sa ćelijskom morfologijom. Cilj istraživanja bio je ispitati da li su postojeći kriterijumi preporučeni od strane ASCO/CAP dovoljni za dijagnostikovanje HER2 pozitivnosti kod pacijentkinja koje pokazuju intratumorsku heterogenost, kako u primarnim tumorima tako i u metastazama u regionalne limfne čvorove, učestalost HER2 heterogenosti u makrometastazama lociranim u limfnim čvorovima, te da li postoji jasna korelacija između heterogenosti nađene u primarnom tumoru dojke i pripadajućim metastazama u limfnim čvorovima. Ispitivanje je obuhvatilo 41 od planirane 51 pacijentkinje koje su ispunile sve kriterijume uključivanja. Reprezentativni parafinski blokovi metastatskih limfnih čvorova odabrani su iz arhiviranog materijala, obojeni GPA metodom i procenjeni u skladu sa kriterijumima ASCO/CAP 2013. Analizirano je 120 ćelija u histološkom rezu svakog metastatskog limfnog čvora. Status HER2 se razlikovao između primarnog tumora i njegovih metastaza u 13,2% (5/38) slučajeva. Jedan slučaj HER2 pozitivnog primarnog tumora imao je HER2 negativne metastaze, dva dodatna slučaja sa HER2 pozitivnim primarnim tumorom su imala metastaze sa statusom granične amplifikacije bez prekomerne ekspresije HER2 proteina i dva slučaja sa HER2 negativnim primarnim tumorom su imala metastaze sa statusom granične amplifikacije bez prekomerne ekspresije HER2 proteina. U 17.4% (4/23) slučajeva sa HER2 ne-amplifikovanim primarnim tumorom metastaze su postale granične u statusu genske amplifikacije. Jedna od četiri metastaze HER2 negativnog primarnog tumora pokazala je mali fokus HER2 pozitivnih tumorskih ćelija (&lt;3% tumora). Mikroheterogenost je analizirana u 108 limfnih čvorova kod 38 pacijentkinja i uočena u 22 limfna čvora, tj. kod četiri pacijentkinje u svim analiziranim limfnim čvorovima, dok je kod jedne pacijentkinje od 4 analizirana limfna čvora mikroheterogenost potvrđena u jednom limfnom čvoru. Na osnovu dobijenih rezultata može se zaključiti da postojeći kriterijumi preporučeni od strane ASCO/CAP primenom prihvaćenih metoda nisu dovoljni za dijagnostikovanje HER2 pozitivnosti kod pacijentkinja koje pokazuju intratumorsku i intertumorsku heterogenost kako u primarnim tumorima tako i u metastazama, te da postoji statistički visoko signifikantan broj makrometastaza lociranih u limfnim čvorovima koje pokazuju HER2 heterogenost i pozitivna korelacija između heterogenosti nađene u primarnim tumorima i pripadajućim metastazama u limfnim čvorovima.</p> / <p><!--[if gte mso 9]><xml> <o:DocumentProperties> <o:Author>ilija vogel</o:Author> <o:Version>16.00</o:Version> </o:DocumentProperties> <o:OfficeDocumentSettings> <o:AllowPNG/> </o:OfficeDocumentSettings></xml><![endif]--><!--[if gte mso 9]><xml> <w:WordDocument> <w:View>Normal</w:View> <w:Zoom>0</w:Zoom> <w:TrackMoves/> <w:TrackFormatting/> <w:PunctuationKerning/> <w:ValidateAgainstSchemas/> 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Predição do risco individual de metástase linfática e hematogênica em função da intensidade da linfangiogênese no tumor carcinóide típico broncopulmonar / Individual risk prediction of node and distant metastasis based on lymphangiogenic intensity in typical pulmonary carcinoid tumor

Laloni, Mariana Tosello 05 August 2008 (has links)
Os tumores carcinóides típicos broncopulmonares são proliferações de células neuroendócrinas. Foram consideradas como adenomas e acreditava-se que não tinham potencial para disseminação hematogênica e linfática. Porém, a ocorrência de metástase linfática e hematogênica acontece em um quinto dos indivíduos acometidos por essa patologia. A variação no comportamento clínico dos carcinóides broncopulmonares torna imperativa a realização de pesquisas que visem à melhor compreensão dessa doença. É fundamental determinar a agressividade e o risco individual da ocorrência de metástase linfática e hematogênica para que se possa oferecer um tratamento individualizado para cada binômio doente-doença. A classificação atual divide os tumores carcinóides, conforme o grau histológico de malignidade em típico e atípico, agrupando as neoplasias de acordo com o índice mitótico, relação volumétrica núcleo/citoplasma, presença ou ausência de necrose, pleomorfismo nuclear e invasão vascular. Esta análise, porém, é realizada em espécimes histológicos corados pela hematoxilina-eosina, técnica tradicional consagrada, mas que não permite avaliar processos biomoleculares relacionados ao potencial maligno das células que já podem estar presentes e não serem detectados pelo método. Em tumores carcinóides vários estudos já foram realizados na tentativa de identificar o potencial proliferativo de células que ainda não apresentam figuras de mitose, como PCNA, p53, Ki-67, o processo apoptótico (Bcl-2, Bax e Bak), fibras do sistema colágeno e elástico e angiogênese. Entretanto, a linfangiogênese nunca foi estudada. Na última década várias moléculas funcionais e constitucionais que são expressas especificamente nas células do endotélio ou nos podócitos dos vasos linfáticos foram identificadas, como o VEGF-C, VEGFR-3 e o LYVE-1, possibilitando a melhor compreensão da linfangiogênese. Estudamos a imunomarcação dessas estruturas no carcinóide típico. Pela primeira vez no Brasil, a quantificação de vasos linfáticos foi realizada usando o LYVE1 como marcador. Apesar do uso de vários bloqueios de sítios inespecíficos não foi possível quantificar a expressão do VEGF-C e VEGFR-3 em carcinóides típicos, pois não encontramos controle interno negativo. Houve diferença significante entre as médias da idade em relação ao gênero. Não houve diferença significante entre as médias do diâmetro e número de linfonodos acometidos em relação ao gênero. Em relação ao grupo com e sem metástase encontramos difenca significante em relação ao diâmetro e ao comprometimento da margem. Não houve diferença da mediana do número de vasos linfáticos corados por mil células entre os grupos sem e com metástase linfática. Por regressão logística identificamos o diâmetro do tumor primário como uma variável independente preditiva do risco de metástase hematogênica e o diâmetro do tumor primário e a localização central ou periférica como variáveis independentes preditivas do risco de qualquer metástase (linfática ou hematogênica). O número de vasos linfáticos corados por mil células não foi identificado pelo modelo de regressão logistica como uma variável independente preditiva do risco individual de metástase linfática. Conclui-se que há correlação do diâmetro do tumor com o potencial de metástase hematogênica e há correlação entre diâmetro e localização do tumor primário e a ocorrência de metástase linfática ou hematogênica. A quantificação da imunoexpressão do LYVE-1 não demonstrou correlação. Outras técnicas devem ser estudadas e empregadas para identificar a importância da linfangiogênese no carcinóide típico. / Typical pulmonary carcinoids are neuroendocrine cells proliferations and they were former considered lung adenomas with no hematogenic or lymphatic metastatic potential. However, it is known that up to 20% of patients develop metastatic disease. It is mandatory that new studies be developed due to the variation in clinical presentation of these patients. It is also required that the individual risk of lymphatic and hematogenic metastasis be determined in order to individualize the patients treatment. Pulmonary carcinoids are classified according to hystologic grade. The current classification includes hystologic grade, presence or absence of necrosis, nuclear pleomorphism, and vascular invasion. This classification is based on Hematoxylin and Eosin stain and this technique can not assess biomolecular processes related to malignant potential. Trying to identify the malignant potential of the carcinoid tumors some studies have already been designed to identify some proteins as PCNA, p53, Ki-67, apoptosis proteins (Bcl-2, Bax and Bak), collagen and elastic fibers as well as angiogenic process. However, the lymphangiogenic mechanism has never been evaluated in typical pulmonary carcinoid tumors. Recently some molecules (VEGF-C, VEGFR-3 and LYVE-1) that are specifically expressed in the endothelium of the lymphatic vessels have been identified. These findings have improved the lymphangiogenic mechanism comprehension. This study used the immunohistochemical technique to identify VEGF-C, VEGFR-3 and LYVE-1 in 182 patients submitted to surgical procedures to treat Typical pulmonary carcinoid tumors. Lymphatic metastasis were diagnosed in 23 of 182 patients and 17 of 182 patients were identified with hematogenic metastasis. Futhermore, this study was the first reported one which has tried to quantify the lymphatic vessels using the LYVE-1 as an immunohistochemical marker. This study could not assess VEGF-C and VEGFR-e expression in Typical pulmonary carcinoids since an internal negative control could not be determined. There was a statistical difference between the median age and gender. There was no statistical difference between the median diameter and the number of positive lymph nodes related to the gender. This study demonstrated a statistical difference between the diameter and positive margins related to the group of patients that have developed metastatic disease and the group of patients with no metatastatic disease. There was no difference between the group of patients that have developed metastatic disease and the group of patients with no metatastatic disease according to the median number of lymphatic vessels stained. Based on logistic regression this study demonstrated that there is a predictive risk of developing hematogenic metastasis related to the diameter of the tumor. The predictive risk of the lymphatic metastasis was not improved by the number of the immunohistochemical stained lymphatic vessels, according to the logistic regression model. The immunohistochemical expression of LYVE-1 has not demonstrated statistical correlation between the parameters studied. Other than immnuhistochemical techniques are required to improve the comprehension of the lymphangiogenic mechanism involved in the Typical pulmonary carcinoid tumor
Bronquial neoplasms/classification
Carcinoid tumors/classification
Fatores de risco
Linfagiogênese
Linphangiogeneses
Lymphatic vessel
Metástase neoplásica
Metastasis
Neoplasias brônquicas/classificação
Neuroendocrine carcinoma/classification
Neuroendocrine tumors/classification
Risk factor
Tumor carcinóide/classificação
Tumores neuroendócrinos/classificação
Tumour biomarkers/classification
Vasos linfáticos
228

Randomisierte, kontrollierte Parallelgruppenstudie zur Untersuchung der Wirksamkeit der manuellen Lymphdrainage und klassischen Massage zur Prophylaxe der Migräne mit und ohne Aura / Randomized, controlled, parallel group study to evaluate the efficacy of manual lymph drainage and traditional massage for the prophylaxis of migraine with and without aura

Hamzeh, Minhal 03 January 2012 (has links)
No description available.
Medicine
manuelle Lymphdrainage
klassischen Massage
manual lymphatic drainage
traditional massage
44.00 Medizin: Allgemeines
MED 202: Ausbildung {Medizin}
MED 201: Berufskunde {Medizin}
229

Predição do risco individual de metástase linfática e hematogênica em função da intensidade da linfangiogênese no tumor carcinóide típico broncopulmonar / Individual risk prediction of node and distant metastasis based on lymphangiogenic intensity in typical pulmonary carcinoid tumor

Mariana Tosello Laloni 05 August 2008 (has links)
Os tumores carcinóides típicos broncopulmonares são proliferações de células neuroendócrinas. Foram consideradas como adenomas e acreditava-se que não tinham potencial para disseminação hematogênica e linfática. Porém, a ocorrência de metástase linfática e hematogênica acontece em um quinto dos indivíduos acometidos por essa patologia. A variação no comportamento clínico dos carcinóides broncopulmonares torna imperativa a realização de pesquisas que visem à melhor compreensão dessa doença. É fundamental determinar a agressividade e o risco individual da ocorrência de metástase linfática e hematogênica para que se possa oferecer um tratamento individualizado para cada binômio doente-doença. A classificação atual divide os tumores carcinóides, conforme o grau histológico de malignidade em típico e atípico, agrupando as neoplasias de acordo com o índice mitótico, relação volumétrica núcleo/citoplasma, presença ou ausência de necrose, pleomorfismo nuclear e invasão vascular. Esta análise, porém, é realizada em espécimes histológicos corados pela hematoxilina-eosina, técnica tradicional consagrada, mas que não permite avaliar processos biomoleculares relacionados ao potencial maligno das células que já podem estar presentes e não serem detectados pelo método. Em tumores carcinóides vários estudos já foram realizados na tentativa de identificar o potencial proliferativo de células que ainda não apresentam figuras de mitose, como PCNA, p53, Ki-67, o processo apoptótico (Bcl-2, Bax e Bak), fibras do sistema colágeno e elástico e angiogênese. Entretanto, a linfangiogênese nunca foi estudada. Na última década várias moléculas funcionais e constitucionais que são expressas especificamente nas células do endotélio ou nos podócitos dos vasos linfáticos foram identificadas, como o VEGF-C, VEGFR-3 e o LYVE-1, possibilitando a melhor compreensão da linfangiogênese. Estudamos a imunomarcação dessas estruturas no carcinóide típico. Pela primeira vez no Brasil, a quantificação de vasos linfáticos foi realizada usando o LYVE1 como marcador. Apesar do uso de vários bloqueios de sítios inespecíficos não foi possível quantificar a expressão do VEGF-C e VEGFR-3 em carcinóides típicos, pois não encontramos controle interno negativo. Houve diferença significante entre as médias da idade em relação ao gênero. Não houve diferença significante entre as médias do diâmetro e número de linfonodos acometidos em relação ao gênero. Em relação ao grupo com e sem metástase encontramos difenca significante em relação ao diâmetro e ao comprometimento da margem. Não houve diferença da mediana do número de vasos linfáticos corados por mil células entre os grupos sem e com metástase linfática. Por regressão logística identificamos o diâmetro do tumor primário como uma variável independente preditiva do risco de metástase hematogênica e o diâmetro do tumor primário e a localização central ou periférica como variáveis independentes preditivas do risco de qualquer metástase (linfática ou hematogênica). O número de vasos linfáticos corados por mil células não foi identificado pelo modelo de regressão logistica como uma variável independente preditiva do risco individual de metástase linfática. Conclui-se que há correlação do diâmetro do tumor com o potencial de metástase hematogênica e há correlação entre diâmetro e localização do tumor primário e a ocorrência de metástase linfática ou hematogênica. A quantificação da imunoexpressão do LYVE-1 não demonstrou correlação. Outras técnicas devem ser estudadas e empregadas para identificar a importância da linfangiogênese no carcinóide típico. / Typical pulmonary carcinoids are neuroendocrine cells proliferations and they were former considered lung adenomas with no hematogenic or lymphatic metastatic potential. However, it is known that up to 20% of patients develop metastatic disease. It is mandatory that new studies be developed due to the variation in clinical presentation of these patients. It is also required that the individual risk of lymphatic and hematogenic metastasis be determined in order to individualize the patients treatment. Pulmonary carcinoids are classified according to hystologic grade. The current classification includes hystologic grade, presence or absence of necrosis, nuclear pleomorphism, and vascular invasion. This classification is based on Hematoxylin and Eosin stain and this technique can not assess biomolecular processes related to malignant potential. Trying to identify the malignant potential of the carcinoid tumors some studies have already been designed to identify some proteins as PCNA, p53, Ki-67, apoptosis proteins (Bcl-2, Bax and Bak), collagen and elastic fibers as well as angiogenic process. However, the lymphangiogenic mechanism has never been evaluated in typical pulmonary carcinoid tumors. Recently some molecules (VEGF-C, VEGFR-3 and LYVE-1) that are specifically expressed in the endothelium of the lymphatic vessels have been identified. These findings have improved the lymphangiogenic mechanism comprehension. This study used the immunohistochemical technique to identify VEGF-C, VEGFR-3 and LYVE-1 in 182 patients submitted to surgical procedures to treat Typical pulmonary carcinoid tumors. Lymphatic metastasis were diagnosed in 23 of 182 patients and 17 of 182 patients were identified with hematogenic metastasis. Futhermore, this study was the first reported one which has tried to quantify the lymphatic vessels using the LYVE-1 as an immunohistochemical marker. This study could not assess VEGF-C and VEGFR-e expression in Typical pulmonary carcinoids since an internal negative control could not be determined. There was a statistical difference between the median age and gender. There was no statistical difference between the median diameter and the number of positive lymph nodes related to the gender. This study demonstrated a statistical difference between the diameter and positive margins related to the group of patients that have developed metastatic disease and the group of patients with no metatastatic disease. There was no difference between the group of patients that have developed metastatic disease and the group of patients with no metatastatic disease according to the median number of lymphatic vessels stained. Based on logistic regression this study demonstrated that there is a predictive risk of developing hematogenic metastasis related to the diameter of the tumor. The predictive risk of the lymphatic metastasis was not improved by the number of the immunohistochemical stained lymphatic vessels, according to the logistic regression model. The immunohistochemical expression of LYVE-1 has not demonstrated statistical correlation between the parameters studied. Other than immnuhistochemical techniques are required to improve the comprehension of the lymphangiogenic mechanism involved in the Typical pulmonary carcinoid tumor
Fatores de risco
Linfagiogênese
Metástase neoplásica
Neoplasias brônquicas/classificação
Tumor carcinóide/classificação
Tumores neuroendócrinos/classificação
Vasos linfáticos
Bronquial neoplasms/classification
Carcinoid tumors/classification
Linphangiogeneses
Lymphatic vessel
Metastasis
Neuroendocrine carcinoma/classification
Neuroendocrine tumors/classification
Risk factor
Tumour biomarkers/classification
230

A New Murine Model For Enterohemorrhagic Escherichia coli Infection Reveals That Actin Pedestal Formation Facilitates Mucosal Colonization and Lethal Disease: A Dissertation

Mallick, Emily M. 28 March 2012 (has links)
Enterohemorrhagic Escherichia coli (EHEC) colonizes the intestine and produces the phage-encoded Shiga toxin (Stx) which is absorbed systemically and can lead to hemolytic uremic syndrome (HUS) characterized by hemolytic anemia, thrombocytopenia, and renal failure. EHEC, and two related pathogens, Enteropathogenic E. coli (EPEC), and the murine pathogen, Citrobacter rodentium, are attaching and effacing (AE) pathogens that intimately adhere to enterocytes and form actin “pedestals” beneath bound bacteria. The actin pedestal, because it is a unique characteristic of AE pathogens, has been the subject of intense study for over 20 years. Investigations into the mechanism of pedestal formation have revealed that to generate AE lesions, EHEC injects the type III effector, Tir, into mammalian cells, which functions as a receptor for the bacterial adhesin intimin. Tir-intimin binding then triggers a signaling cascade leading to pedestal formation. In spite of these mechanistic insights, the role of intimin and pedestal formation in EHEC disease remains unclear, in part because of the paucity of murine models for EHEC infection. We found that the pathogenic significance of EHEC Stx, Tir, and intimin, as well as the actin assembly triggered by the interaction of the latter two factors, could be productively assessed during murine infection by recombinant C. rodentium expressing EHEC virulence factors. Here we show that EHEC intimin was able to promote colonization of C. rodentium in conventional mice. Additionally, previous in vitro data indicates that intimin may have also function in a Tir-independent manner, and we revealed this function using streptomycin pre-treated mice. Lastly, using a toxigenic C. rodentium strain, we assessed the function of pedestal formation mediated by Tir-intimin interaction and found that Tir-mediated actin polymerization promoted mucosal colonization and a systemic Stx-mediated disease that shares several key features with human HUS.
Enterohemorrhagic Escherichia coli
Escherichia coli Infections
Hemolytic-Uremic Syndrome
Shiga-Toxigenic Escherichia coli
Shiga Toxin
Citrobacter rodentium
Adhesins
Bacterial
Escherichia coli Proteins
Amino Acids, Peptides, and Proteins
Animal Experimentation and Research
Bacteria
Bacterial Infections and Mycoses
Biological Factors
Enzymes and Coenzymes
Hemic and Lymphatic Diseases
Immunology and Infectious Disease
Male Urogenital Diseases

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