Teses / dissertações sobre o tema "Cell death"
Crie uma referência precisa em APA, MLA, Chicago, Harvard, e outros estilos
Veja os 50 melhores trabalhos (teses / dissertações) para estudos sobre o assunto "Cell death".
Ao lado de cada fonte na lista de referências, há um botão "Adicionar à bibliografia". Clique e geraremos automaticamente a citação bibliográfica do trabalho escolhido no estilo de citação de que você precisa: APA, MLA, Harvard, Chicago, Vancouver, etc.
Você também pode baixar o texto completo da publicação científica em formato .pdf e ler o resumo do trabalho online se estiver presente nos metadados.
Veja as teses / dissertações das mais diversas áreas científicas e compile uma bibliografia correta.
Pat, Sze Wa. "Cell metabolism in cell death and cell growth". HKBU Institutional Repository, 2007. http://repository.hkbu.edu.hk/etd_ra/775.
Texto completo da fonteCrisby, Milita. "Cell death in atherosclerosis /". Stockholm, 1998. http://diss.kib.ki.se/1998/91-628-3191-7/.
Texto completo da fonteEllison, David William. "Cell proliferation, cell death, and differentiation in gliomas". Thesis, University of Southampton, 1995. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.295912.
Texto completo da fonteUppington, Kay Marie. "Cell death in prion disease". Thesis, University of Bath, 2008. https://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.488879.
Texto completo da fonteBeeharry, Neil. "Cell death in insulin-containing cells : induction and prevention". Thesis, University of Brighton, 2004. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.401600.
Texto completo da fonteGorak-Stolinska, Patricia. "Activation induced cell death in human T cell subsets". Thesis, King's College London (University of London), 2002. http://kclpure.kcl.ac.uk/portal/en/theses/activation-induced-cell-death-in-human-t-cell-subsets(eb708e24-eccb-42fc-8930-d62ddf6794c1).html.
Texto completo da fonteCheng, Jade. "Regulation of cell division and cell death by GRASP65". Thesis, University of Bristol, 2011. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.544414.
Texto completo da fonteRUNYAN, CHRISTOPHER MICHAEL. "The Role of Cell Death in Germ Cell Migration". University of Cincinnati / OhioLINK, 2008. http://rave.ohiolink.edu/etdc/view?acc_num=ucin1210732680.
Texto completo da fonteCourtois-Moreau, Charleen Laetitia. "Programmed Cell Death in Xylem Development". Doctoral thesis, Umeå universitet, Umeå Plant Science Centre, 2008. http://urn.kb.se/resolve?urn=urn:nbn:se:umu:diva-1831.
Texto completo da fonteOron för klimatförändringar och brist på fossila bränslen har ökat påtagligt under de senaste åren. De enorma möjligheter som skogsråvaran erbjuder som alternativ källa för förnyelsebar energi och råmaterial har väckt ett stort intresse också för den biologiska processen bakom vedbildning i träd. Denna avhandling fokuserar på en viktig process i vedbildning: programmerad celldöd (PCD) i xylemet. Xylemcellernas livstid påverkar bildningen av sekundära cellväggar, vilket i sin tur påverkar vedens kvalitativa egenskaperna, så som veddensitet. Trots dess betydelse för viktiga egenskaper hos vedråvaran existerar fortfarande väldigt lite information om xylem PCD på cellulär eller molekylär nivå. I den här avhandlingen belyses de anatomiska, morfologiska och genetiska aspekterna av PCD i xylemutveckling i både stam av hybridasp, Populus tremula (L.) x tremuloides (Michx.) och hypokotyl av det örtartade modellsystemet Arabidopsis thaliana (L. Heynh.). Xylemet i både Populus och Arabidopsis består av två olika celltyper; de vattentransporterade kärlen och de stödjande fibrerna. Det är känt att celldöd i kärlen pågår mycket snabbt efter att den centrala vakuolen brister och de hydrolytiska enzymer släpps in i cytoplasman. I den här avhandlingen ligger fokus på fibrerna i Populus xylemet. Med hjälp av mikroskopianalyser av cellmorfologin (elektronmikroskopi) och DNA-fragmentering i cellkärnan (TUNEL- och Comet-analyser) kunde vi konstatera att till skillnad från kärlen så uppvisar fibrerna en långsam och progressiv nedbrytning av organellerna och cellkärnans DNA före vakuolbristning. Dessutom har kandidatgener för reglering av fibercelldöd identifierats antingen från ett Populus EST bibliotek från vedartade vävnader som genomgår fibercelldöd eller från mikroarray experiment i Populus stam. Dessa kandidatgener är antingen potentiella nya regulatorer av fibercelldöd eller medlemmar av tidigare beskrivna familjer av celldödsrelaterade gener. Bland de sistnämnda finns autofagi-relaterade gener, vilket stöder funktionen av autofagi i samband med autolys av cellinnehållet i xylemfibrerna. Dessa studier pekar därför på en typ av PCD som har inte tidigare beskrivits för xylemet. Arabidopsis är ett alternativt växtmodellsystem för studier av vissa aspekter av vedbildningen, såsom karakteriseringen av negativa regulatorer av PCD. Därför har också hypokotylanatomin analyserats, och ACAULIS5 (ACL5) genen, som kodar för ett enzym i biosyntesen av polyaminer, har visats vara en viktig regulator av xylemspecifikation genom dess negativa effekt på kärlens celldöd. Sammantaget visar denna avhandling att PCD i xylemutvecklingen verkar involvera unika morfologiska och molekylära mekanismer. Vi visar dessutom att komplexiteten hos de vedartade vävnaderna leder till ett behov av bättre anpassade verktyg för att djupare kunna bedöma PCD och liknande fenomen i veden.
Även med namnet Moreau-Courtois, Charleen L. samt Moreau, Charleen.
Klassen, Shaun Scott. "Nitric oxide-induced cardiomyocyte cell death". Thesis, University of British Columbia, 2006. http://hdl.handle.net/2429/31539.
Texto completo da fonteMedicine, Faculty of
Medicine, Department of
Experimental Medicine, Division of
Graduate
Martinez, Bermudez Ana Katherine. "Isoprostanes in brain endothelial cell death". Thesis, National Library of Canada = Bibliothèque nationale du Canada, 1999. http://www.collectionscanada.ca/obj/s4/f2/dsk1/tape9/PQDD_0025/MQ50832.pdf.
Texto completo da fonteMaianski, Nikolai. "Neutrophil cell death: mechanisms and regulation". [S.l. : Amsterdam : s.n.] ; Universiteit van Amsterdam [Host], 2004. http://dare.uva.nl/document/88280.
Texto completo da fonteMartinez, Bermudez Ana Katherine. "Isoprostanes in brain endothelial cell death". Thesis, McGill University, 1998. http://digitool.Library.McGill.CA:80/R/?func=dbin-jump-full&object_id=21605.
Texto completo da fonte8-Iso-PGF2alpha (1--10 nM) induced 20--25% cell death in endothelial cultures after 24 h coincident with similar increase in the number of cells that become permeable to PI. On the contrary, 8-iso-PGE 2 did not affect endothelial cell survival. Approximately 9% of the cells suffered apoptosis. This percentage remained unchanged regardless the treatment. Several observations indicate a role for thromboxane A2 to mediate 8-iso-PGF2alpha-induced death: (1) the levels of thromboxane A2 increased dramatically in endothelial cultures after 8-iso-PGF2alpha-treatment; (2) inhibitors of thromboxane synthase, CGS12970 and U6355A and Ibuprofen, a non-selective inhibitor of cyclooxygenases, reverted the effect of the isoprostane; (3) analogs of thromboxane A2 U46619 and IBOP, reproduce the effect of 8-iso-PGF 2alpha after 24 h. 8-Iso-PGF2alpha also decreased endothelial viability on isolated brain microvessels. These results suggest, that 8-iso-PGF2alpha, might be a direct contributor to ischemia/reperfusion injury.
Spanos, Sophia. "Cell death during preimplantation embryo development". Thesis, Imperial College London, 2003. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.398228.
Texto completo da fonteŚwidziński, Jodi A. "Programmed cell death in Arabidopsis thaliana". Thesis, University of Oxford, 2003. http://ora.ox.ac.uk/objects/uuid:6e2580fc-8873-4722-89f7-b206d4be2a5f.
Texto completo da fonteCox, Orla T. "Vascular cell death in diabetic retinopathy". Thesis, Queen's University Belfast, 2000. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.343079.
Texto completo da fonteSharma, Pundrique Radheyshyam. "Programmed cell death during heart development". Thesis, University College London (University of London), 2002. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.272255.
Texto completo da fonteFitzgerald, Julia. "Monoamine oxidase in neuronal cell death". Thesis, Nottingham Trent University, 2008. http://irep.ntu.ac.uk/id/eprint/51/.
Texto completo da fonteRamos, Paulina Joanna. "Fibronectin Enhances Carfilzomib Mediated Cell Death". Thesis, The University of Arizona, 2015. http://hdl.handle.net/10150/579327.
Texto completo da fonteJanson, Veronica. "Cisplatin-resistance and cell death in malignant pleural mesothelioma cells". Doctoral thesis, Umeå universitet, Medicinsk biovetenskap, 2008. http://urn.kb.se/resolve?urn=urn:nbn:se:umu:diva-1680.
Texto completo da fonteMcComb, Scott. "The Paradoxical Roles of Cell Death Pathways in Immune Cells". Thèse, Université d'Ottawa / University of Ottawa, 2013. http://hdl.handle.net/10393/24331.
Texto completo da fonteKaul, Aparna. "Mechanisms of Non-Conventional Cell Death in Brain Tumor Cells". University of Toledo Health Science Campus / OhioLINK, 2009. http://rave.ohiolink.edu/etdc/view?acc_num=mco1243364096.
Texto completo da fonteKoterba, Kristen L. "Regulation of Autophagy and Cell Death in Breast Carcinoma Cells". University of Toledo Health Science Campus / OhioLINK, 2010. http://rave.ohiolink.edu/etdc/view?acc_num=mco1276005638.
Texto completo da fonteStuckey, Crystal Elaine. "Oxidative Stress and Cell Death in Osmotically Swollen Glial Cells". Wright State University / OhioLINK, 2008. http://rave.ohiolink.edu/etdc/view?acc_num=wright1208492663.
Texto completo da fontePrise, Kevin M. "Cell death and DNA damage in methotrexate-treated HeLa cells". Thesis, University of Aberdeen, 1985. http://digitool.abdn.ac.uk/R?func=search-advanced-go&find_code1=WSN&request1=AAIU362655.
Texto completo da fonteStuart, Lynda Maria. "Cell death, dendritic cells and downregulation of the immune response". Thesis, University of Edinburgh, 2003. http://hdl.handle.net/1842/23214.
Texto completo da fonteAhmed, Yasser Abdel Galil. "Analysis of physiological death in equine chondrocytes /". Connect to thesis, 2007. http://eprints.unimelb.edu.au/archive/00003656.
Texto completo da fonteJahnke, Ulrike. "Cell cycle de-regulation and cell death in leukaemia chemotherapy". Thesis, Queen Mary, University of London, 2006. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.439424.
Texto completo da fonteWatson, Andrea. "Heat shock proteins in leukaemia cell differentiation and cell death". Thesis, Aston University, 1990. http://publications.aston.ac.uk/12533/.
Texto completo da fonteSciacovelli, Marco. "Cell death regulation by mitochondrial chaperones in tumor cell models". Doctoral thesis, Università degli studi di Padova, 2011. http://hdl.handle.net/11577/3421645.
Texto completo da fonteLe cellule tumorali sono caratterizzate dalla capacità di evadere il normale signale apoptotico, così come mostrano una iper-attivazione costitutiva delle vie di signale kinasico. L’integrazione degli stimoli di sopravvivenza e morte si concentra nei mitocondri, dove molti di questi segnali convergono nella regolazione di un canale chiamato poro della transizione di permeabilità (PTP). L’apertura del PTP porta le cellule alla morte ed è regolata da una varietà di fattori e fra questi gli chaperoni giocano un ruolo fondamentale. Nel mio lavoro di tesi ho studiato come gli chaperoni mitochondriali si integrano nelle vie di trasduzione del segnale , modulando il PTP e più in generale la bioenergetica mitocondriale e come questi network regolatori controllano la vitalità cellualre. Nella prima parte del mio lavoro ho studiato una possibile connessione fra la via del segnale Ras/ERK, la cui attivazione costitutiva caratterizza molti tumori favorendo la loro crescita e sopravvivenza, e la ciclofilina D (CyP-D), uno chaperone mitocondriale che regola il PTP. Una frazione di ERK attivo è stato trovato nei mitocondri delle cellule RWPE-2, ottenute tramite trasformazione con v-ki-Ras a partire da cellule dell’epitelio prostatico RWPE-1; in cellule metastatiche di tumore prostatico DU145; e in cellule di osteosarcoma SAOS-2. Tutte queste cellule tumorali mostrano una marcata resistenza alla morte indotta da stimoli pro-apoptotici come l’acido arachidonico e il BH3 mimetico EM20-25, i quali inducono la morte cellulare attraverso il PTP mitocondriale. L’inibizione del PTP e la conseguente resistenza alla morte cellulare indotta da acido arachidonico o EM-20-25 può essere abolita dall’inibizione di ERK con il farmaco PD98059 o con un peptide selettivo inibitorio di ERK. L’inibizione di ERK aumenta la fosforilazione GSK-3 dipendente della CyP-D, mentre l’inibizione di GSK3 protegge dall’apertura del poro. Ne ERK attivo nei mitocondri, ne desensibilizzazione del poro è stata osservata in cellule non trasformate RWPE-1. In conclusione, nelle cellule tumorali l’attivazione dell’ERK mitocondriale desensibilizza il PTP attraverso un asse di segnale che coinvolge GSK3 e Cyp-D. Nella seconda parte del mio lavoro di tesi, ho studiato l’attività di un secondo chaperone mitocondriale, TRAP1/HSP75, fortemente espresso nelle cellule tumorali e che è stato proposto essere coinvolto nella regolazione del poro. Ho dimostrato che TRAP1 interagisce con la CyP-D ed ho caratterizzato la sua funzione di pro-sopravvivenza nei confronti di un vasto spettro di stimoli di morte, incluso lo stress ossidativo, la diamide, il TNFα, e la deplezione di glucosio. Inoltre ho trovato che il knocking-down dei livelli di espressione di TRAP1 attraverso la tecnica dell’RNA interference in cellule di osteosarcoma SAOS-2 facilita l’apertura del PTP, abbassando la soglia per portare le cellule alla morte. TRAP1 modula inoltre il metabolismo cellulare probabilmente la risposta allo stress ossidativo e l’attività della del complesso I della catena respiratoria, con il quale TRAP1 interagisce direttamente sia in cellule che campioni tumorali. La down- regolazione di TRAP1 abolisce il potere tumori genico delle cellule SAOS-2 sia in vitro che in vivo. Tutti insieme questi dati indicano che gli chaperoni mitocondriali come CyP-D e TRAP! Giocano un ruolo importante nella progressione tumorale e costituiscono un possibile target di nuove terapie antineoplastiche.
Tamm, Christoffer. "Apoptotic cell death in neural stem cells exposed to toxic stimuli /". Stockholm : Karolinska institutet, 2007. http://diss.kib.ki.se/2007/978-91-7357-301-6/.
Texto completo da fonteAjabnoor, Ghada. "Mechanism of cell death in drug resistant human breast cancer cells". Thesis, University of Surrey, 2010. http://epubs.surrey.ac.uk/842867/.
Texto completo da fonteJaligam, Vanaja. "Developmental cell death in the midline glia cells of Drosophila embryo". College Park, Md. : University of Maryland, 2004. http://hdl.handle.net/1903/1467.
Texto completo da fonteThesis research directed by: Dept. of Cell Biology and Molecular Genetics. Title from t.p. of PDF. Includes bibliographical references. Published by UMI Dissertation Services, Ann Arbor, Mich. Also available in paper.
Wilkie, Alexander David. "Evasion of Cell Death in Burkitt’s Lymphoma and Pancreatic Cancer Cells". Thesis, Griffith University, 2016. http://hdl.handle.net/10072/367897.
Texto completo da fonteThesis (PhD Doctorate)
Doctor of Philosophy (PhD)
School of Natural Sciences
Science, Environment, Engineering and Technology
Full Text
Latif, Lubna Salah Eldin Abdel. "Assessment of Cell Death Parameters in Bovine Parvovirus-Infected EBTr Cells". BYU ScholarsArchive, 2005. https://scholarsarchive.byu.edu/etd/445.
Texto completo da fonteMai, Thi Trang. "Cell death mechanisms of Marmycin A and Salinomycin in cancer cells". Thesis, Université Paris-Saclay (ComUE), 2016. http://www.theses.fr/2016SACLS014.
Texto completo da fonteA natural product Salinomycin (SAL) is widely used as an anticoccidial drug now being increasingly recognized as an agent for reducing the proportion of CD44⁺/CD24⁻ breast cancer stem cell which is perceived as important factor for breast tumor relapse. We first time report that not ionophoric action but the proton “sponge” of SAL is responsible for distinguishingly targeting cancer stem cell population. In addition, one SAL-analog alkyne-amine performed the similar action with SAL on CD44⁺/CD24⁻ population but at much lower concentration than SAL, at 30 nM compare to 500 nM of SAL. Using click-imaging method we visually observed the colorless compound saturated in lysosomes and autolysosomes. By raising pH of acidic vesicles, SAL and its analogs inhibit cathepsin B, L, D activity preventing the autophagy which plays an important role in cancer stem cell maintain and survival thus lead to cell death via increasing ROS and apoptosis. Our study provides the insight mechanism how SAL actually eradicates cancer stem cells and suggests sharpened strategies for treating resistant cancers
Giampazolias, Evangelos. "Investigating non-apoptotic cell death in cancer". Thesis, University of Glasgow, 2017. http://theses.gla.ac.uk/8056/.
Texto completo da fonteRijal, Dikchha. "Cell Death Signaling Complexes During Macrophage Differentiation". Thesis, Université d'Ottawa / University of Ottawa, 2017. http://hdl.handle.net/10393/36455.
Texto completo da fonteO'Hare, Michael J. "Cell cycle related signaling in neuronal death". Thesis, University of Ottawa (Canada), 2006. http://hdl.handle.net/10393/29368.
Texto completo da fonteLai, Xin-He. "Francisella tularensis infection induces macrophage cell death". Doctoral thesis, Umeå : Univ, 2004. http://urn.kb.se/resolve?urn=urn:nbn:se:umu:diva-295.
Texto completo da fonteRobey, Thomas Edwin. "Reducing fibrosis and cell death in cardiomyoplasty /". Thesis, Connect to this title online; UW restricted, 2007. http://hdl.handle.net/1773/8031.
Texto completo da fonteMénard, Isabelle. "Exploring the many facets of cell death". Thesis, McGill University, 2007. http://digitool.Library.McGill.CA:80/R/?func=dbin-jump-full&object_id=111878.
Texto completo da fonteIn the second part of the thesis, the role of the RNA-binding protein HuR in cancer cell migration and invasion, as well as in multidrug resistance is determined using RNA interference to knockdown the expression of HuR in HeLa and KB-V1 cells respectively (research performed in the laboratory of Dr. Imed Gallouzi). In this part of the thesis, HuR is shown to promote cancer cell migration and invasion by stabilizing the beta-actin mRNA in a U-rich-dependent manner. Moreover, evidence is shown for the potential involvement of HuR in the phenomenon of multidrug resistance possibly through the post-transcriptional regulation of the multidrug resistance 1 gene.
Palazzo, Francesco Fausto. "Programmed cell death in autoimmune thyroid disease". Thesis, Queen Mary, University of London, 2002. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.270709.
Texto completo da fonteEdwards, Susan N. "Regulation of cell death in sympathetic neurons". Thesis, University of Oxford, 1992. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.316898.
Texto completo da fonteAtkin, Charlotte J. "Developmental cell death in the rat brain". Thesis, University of Oxford, 2001. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.393568.
Texto completo da fonteLoughery, Jayne Eleanor Patricia. "Mismatch repair, DNA methylation and cell death". Thesis, University of Ulster, 2009. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.551565.
Texto completo da fonteParnaik, Rahul. "Cell death and clearance in young animals". Thesis, University College London (University of London), 1997. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.284799.
Texto completo da fonteKreuzaler, Peter Anton. "Cell death modalities in mammary gland involution". Thesis, University of Cambridge, 2011. http://ethos.bl.uk/OrderDetails.do?uin=uk.bl.ethos.609378.
Texto completo da fonteWilkinson, Derek. "Proteases and programmed cell death in fungi". Thesis, University of Exeter, 2011. http://hdl.handle.net/10036/3629.
Texto completo da fonteDhillon, Harsharan. "Mechanisms of Piperlongumine-Induced Cancer Cell Death". Diss., North Dakota State University, 2015. http://hdl.handle.net/10365/25178.
Texto completo da fonteNorth Dakota State University. Department of Biological Sciences
NDSU Graduate School Doctoral Dissertation Fellowship
NDSU Center for Protease Research COBRE (NIH 2P20 RR015566, P30 GM103332-01)
NDSU Development Foundation Centennial
Engebretson Family Research Endowments