Étude de facteurs génétiques prédictifs dans le neuroblastome, en particulier les anomalies du chromosmoe 14q

Arsenault, Marie-Pier

08 1900

Le neuroblastome (NB) représente 8% de tous les cancers pédiatriques et est caractérisé par sa grande hétérogénéité clinique. Afin d’évaluer son pronostic, plusieurs facteurs génétiques sont utilisés : amplification de MYCN, délétion 1p, gain 11q et gain 17q. Les buts de notre travail étaient d’abord de vérifier si l’hybridation in situ en fluorescence (FISH) permet une analyse complète de ces anomalies et ensuite, en utilisant une analyse globale du génome telle le polymorphisme nucléotidique simple (SNP), de vérifier la concordance avec les résultats de la FISH et le pronostic potentiel des anomalies du 14q, en particulier du gène AKT. Nous avons donc établi un panel de sondes pour la FISH qui a été appliqué sur 16 tumeurs non-fixées. Après isolation de l’ADN de 36 tumeurs, nous avons effectué une analyse génotypique par SNP utilisant les puces « Affymetrix Genome-Wide Human SNP Array 6.0 » contenant 945,826 sondes non polymorphiques et 906,000 sondes polymorphiques. Nos résultats ont démontré que la FISH permet l’évaluation complète des anomalies génétiques importantes du NB et que les anomalies déséquilibrées sont détectées très précisément par SNP. Les anomalies du 14q tendent à être associées avec des facteurs cliniques comme le grade et l’évolution, contrairement aux anomalies d’AKT. L’analyse du 14q a révélé trois gènes d’intérêt, MAX, BCL11B et GPHN, qui devraient être analysés sur un plus grand échantillon. Ainsi, l’étude par FISH semble adaptée pour détecter les anomalies génétiques classiques du NB, alors que celles retrouvées en 14q représentent de potentielles cibles thérapeutiques pour cette tumeur. / Neuroblastoma (NB) accounts for 8% of all childhood cancers and is characterized by its clinical heterogeneity. To evaluate its prognostic, many genetic markers are used: MYCN amplification, 1p deletion, 11q gain and 17q gain. Our goals were first to verify if fluorescence in situ hybridization (FISH) allows a complete analysis of these abnormalities and, second, using a global genomic analysis as single nucleotide polymorphism (SNP), to verify the concordance with FISH results and the prognostic potential of 14q abnormalities, especially these of AKT gene. We then established a FISH panel that has been applied on 16 unfixed tumors. After DNA isolation of 36 tumors, we made a genotypic analysis by SNP using « Affymetrix Genome-Wide Human SNP Array 6.0 » containing 945,826 nonpolymorphic probes and 906,000 polymorphic probes. Our results have demonstrated that FISH allows a complete evaluation of the NB’s important genetic abnormalities and that unbalanced abnormalities are detected very precisely by SNP. 14q abnormalities seem to be associated with clinical factors such as tumor grading and evolution, unlike AKT abnormalities. Analysis of 14q abnormalities revealed three genes of interest, MAX, BCL11B and GPHN, which should be analyzed on a larger sample. Thereby, FISH study seems appropriate to detect the NB’s classic genetic abnormalities, while those found in 14q represent potential therapeutic targets for this tumor.

Neuroblastome

Neuroblastoma

FISH

SNP

14q

AKT

Development of Dual-Pathway Inhibitors of Raf/MEK/ERK and PI3K/Akt Signaling Pathways.

Fraser, Sasha

13 December 2011

In the present study, we designed a new chemical template that contains an oxindole moiety as potential dual-pathway inhibitors of the Raf/MEK/ERK and PI3K/Akt signaling pathways. The design hypothesis is to evaluate whether the oxindole ring system will approximately orient functional groups in a similar manner to the thiazolidinedione moiety, and thus maintain biological activity as dual-pathway inhibitors of the Raf/MEK/ERK and PI3K/Akt signaling pathways. Furthermore, the oxindole ring will provide the flexibility to allow the introduction of various substituents on the oxindole moiety, thereby facilitating comprehensive SAR studies to further explore the biological activity.

ras

erk

akt

pi3k

oxindole

mek

raf

Medicine and Health Sciences

Pharmacy and Pharmaceutical Sciences

Divergent Roles of PI3K and Akt in Rapamycin-induced Cardioprotection against Ischemia-Reperfusion Injury

Desai, Shivani Kirit

01 January 2007

Coronary heart disease (CHD) is one of the leading causes of death every year with nearly three-fourths of all deaths caused by the disease. The challenge scientists are facing today is discovering new drugs to protect the heart against cellular damage caused by ischemia-reperfusion injury (I-R injury). Rapamycin is one such drug that has been shown to protect the heart against ischemia-induced cellular injury. Rapamycin(sirolimus) inhibits protein synthesis through inhibition of the mammalian target ofrapamycin (mTOR). This property of rapamycin has led to its current clinical applications in drug-eluting stents and in immunosuppresive treatment to organ transplant patients. The mechanism by which this drug protects against I-R injury is currently unknown. The goal of this study is to elucidate rapamycin's cardioprotective signaling pathway. We hypothesized that upregulation of Akt occurs possibly as part of a positive feedback mechanism following the inhibition of mTOR by rapamycin. Adult male ICRmice were treated with rapamycin (0.25 mg/kg, i.p.), or volume-matched DMSO (solvent for rapamycin), or rapamycin (0.25mg/kg, i.p.) plus wortmannin (WTN, 15µg/kg, i.p.),an inhibitor of phosphatidylinositol 3-kinase, or wortmannin alone (15µg/kg, i.p.). After 30 min of stabilization, the hearts were subjected to 20 minutes of global ischemia and 30 minutes of reperfusion in Langendorff model. In a separate series of experiments mice were either injected with DMSO or rapamycin for 30 minutes, 1 hour, and 2 hours before harvesting the hearts for Western blot analysis of levels of total or phosphorylated Akt at Ser473. Our results showed that rapamycin protected the heart as observed by a reductionin infarct size from 33.8 ± 2.0% in DMSO-treated hearts to 19.3 ± 4.1% in rapamycin-treated hearts; a 43% reduction. This infarct-limiting effect was completely blocked by wortmannin (29.3 ± 4.8%). However, Western blot analysis showed no change in the level of Akt phosphorylation after administration of rapamycin. Our current resultsfurther confirmed rapamycin as a potential cardio-therapeutic drug to limit infarct size,potentially through the PI3K signaling pathway. However, the exact signaling pathway of this protection still remains elusive.

Langendorff isolated heart model

Akt

PI3K

rapamycin

wortmannin

Life Sciences

Physiology

Le rôle de la tyrosine phosphatase Shp-1 dans le maintien de l’homéostasie de l’épithélium intestinal

Leblanc, Caroline

January 2015

Shp-1 (Src homology 2 domain-containing phosphatase 1) est une tyrosine phosphatase retrouvée principalement chez les cellules hématopoïétiques, mais également chez les cellules épithéliales. Bien que Shp-1 soit reconnue comme étant un régulateur négatif de plusieurs voies de signalisation intracellulaire chez les cellules hématopoïétiques, son rôle dans les cellules épithéliales a été jusqu’ici très peu étudié. Afin de mieux comprendre son rôle dans les cellules épithéliales intestinales, nous avons généré un modèle murin de délétion conditionnelle de Shp-1 spécifiquement dans l’épithélium intestinal (Shp-1CEI-KO). De manière intéressante, dès l’âge de 6 semaines, les souris expérimentales présentent une intestinalomégalie associée à une légère augmentation de la prolifération cryptale. La taille des cellules épithéliales est également augmentée, suggérant de l’hypertrophie cellulaire chez les souris invalidées pour Shp-1. Parallèlement, la voie de signalisation PI3K/Akt/mTor est activée dans l’épithélium des souris mutantes. Nous avons également noté une production accrue de cellules caliciformes et de leurs précurseures, les cellules intermédiaires, en absence de Shp-1. Par contre, la maturation des cellules de Paneth semble grandement compromise vu la baisse importante d’expression du lysozyme et des RegIIIβ et RegIIIγ, de même que la faible densité de leurs granules de sécrétion. La comparaison du phénotype intestinal des souris Shp-1CEI-KO avec celui des souris PtenCEI-KO suggère que l’hyperactivation de la voie PI3K/Akt/mTor est responsable en partie des altérations phénotypiques observées chez la souris invalidée pour Shp-1. En conclusion, nos résultats montrent que la tyrosine phosphatase Shp-1 est un régulateur important de l’homéostasie de l’épithélium intestinal en contrôlant notamment la croissance cellulaire et la différenciation des cellules de la lignée sécrétrice.

Shp-1

Tyrosine phosphatase

Cellules de Paneth

Cellules intermédiaires

Wnt/β-caténine

PI3K/Akt/mTor

Právní aspekty spolupráce Evropské unie se zeměmi skupiny AKT / Legal aspects of cooperation between the EU and ACP countries

Pšenka, Lubomír

January 2011

Legal aspects of cooperation between the EU and ACP countries The origins of the EU cooperation with the group of Sub-saharan African, Caribbean and Pacific countries (ACP Group) date back to the very beginnings of the European integration with Part IV of the Treaty of Rome establishing association of the former colonies of the several founding member states to the European Economic Community. After the colonies gained their independence, their association to the EEC was given a basis of the international law by means of the conventions from Yaoundé (1963, 1969) and Lomé (1975, 1980, 1985, 1990 - revised in 1995). The cooperation between the EC/EU and ACP countries has progressively evolved into a comprehensive partnership encompassing the political, development and economic cooperation. The relations between the EU and 78 ACP countries are actually ruled by the Cotonou Partnership Agreement (2000, revised in 2005 and 2010) which is to be in force until 2020. The EU-ACP partnership constitutes a specific system of international law and probably can be described as the most comprehensive relationship between developed and developing countries. In many ways, the cooperation with the ACP countries represents a special case in the field of the EU external relations and, due to a specific historical...

The role of LEF1 and WNT signaling in growth and differentiation of rhabdomyosarcoma

Dräger, Julia

02 February 2017

No description available.

610

Rhabdomyosarcoma

WNT signaling

LEF1/TCF

WNT5A signaling

PI3K/AKT signaling

Biologie (PPN619462639)

Právní aspekty jednostranného prohlášení nezávislosti Kosova / The legal aspects of Kosovo's unilateral declaration of independence

Pecháček, Jakub

January 2010

This thesis focuses on the legal aspects of Kosovo's unilateral declaration of independence. At first I describe the historical and political development in this region. Further follows the explanation of the instruments of international law, such as the definition of a state, the unilateral acts of states and the role of the International Court of Justice. As conclusion I descirbe the role of this instruments on the example of Kosovo and evaluate the impact of the Kosovo indendence on the legal sphere.

The role of Aktin the prevention of Apoptosis in HL-60 cells, A human leukaemic cell line

Drummond, Chantal, Paula

25 October 2006

Faculty of Science School of Molecular Medicine and Haematology Masters Dissertation / Studies on the development of drug resistance in several cancer types, including acute myeloid leukaemia (AML), have implicated the PI3-kinase pathway. This pathway phosphorylates Akt resulting in the activation of proteins involved in cell survival. The aim of this study is to determine the role that Akt plays in urvival and the relationship between Akt, IKK and IkB in HL-60 cells. This study demonstrated that etoposide caused apoptosis in HL-60 cells, which was slightly increased when the PI3-kinase pathway was inhibited by LY294002. Stimulation with PDGF resulted in cell proliferation and increased Akt, IKK and IkB phosphorylation. Although pre-treatment with LY294002 decreased the amount of Phospho-Akt, phosphorylation of IKK and IkB still occurred. Therefore additional pathways must be involved in IkB regulation in HL-60 cells. Akt mRNA transcription was decreased when the cells were pretreated with LY294002 and either PDGF or etoposide. In conclusion, the PI3-kinase pathway plays a minor role in the survival of HL-60 cells and Akt substrates other than IKK are mediating this survival.

drug resistance

acute myeloid leukaemia

AML

phosphorylates

PI3-kinase

Akt

proliferation

Avaliação imunoistoquímica das proteínas metalotioneína, pAKT e NF-kB como marcadores de prognóstico de carcinomas epidermóides de boca / Immunohistochemical evaluation of Metallothionein, pAkt and NF-kB proteins as prognostic factors of Oral Squamous Cell Carcinoma

Pontes, Helder Antonio Rebêlo

26 May 2008

O carcinoma epidermóide é a neoplasia maligna que ocorre com maior freqüência na boca. Os pacientes portadores desta neoplasia ainda apresentam um pobre prognóstico com índices de sobrevida, em cinco anos, variando de 20 a 40% em vários estudos. Um grande número de trabalhos tem sido direcionado para identificar marcadores que auxiliem no direcionamento do tratamento e melhorem o prognóstico. A metalotioneína (MT) é uma proteína de baixo peso molecular, com alto conteúdo de cisteína e que está associada à resistência neoplásica a várias modalidades de tratamento, e que por isso tem sido estudada como fator prognóstico em uma variedade de neoplasias malignas humanas. O Fator Nuclear B desempenha um importante papel na ativação de genes que estão relacionados à imunidade, inflamação, sobrevida, apoptose, proteção celular à radiação e à quimioterapia. A proteína serina/treonina quinase Akt é um alvo downstream da quinase 3-fosfaditilinositol, desempenhando um importante papel na proliferação e no bloqueio da apoptose de células cancerígenas. Neste estudo, nós examinamos a expressão das proteínas MT, NF-kB e pAKT em 51 casos de carcinomas epidermóides de boca, através de imunoistoquímica, com a finalidade de investigar suas influências prognosticas, assim como estudar as correlações entre alguns fatores clínicos com a sobrevida. Os resultados mostraram uma associação estatisticamente significante entre a expressão pAkt e NF-kB e entre MT e NF-kB. Ao lado disso, nossos resultados mostraram que a expressão de pAkt está associada a um pior prognóstico. Nossos resultados, portanto, sugerem que a proteína pAkt pode ter implicações terapêuticas em carcinomas epidermóides de boca. / Oral squamous cell carcinoma (OSCC) is the most frequent malignant tumor of the oral cavity. In spite of improved therapeutic procedures, patients with OSCC in advanced stage generally present a poor prognosis, with an overall 5-year survival rate that ranges from 20% to 40%. An extensive effort has started to identify features of the oral tumors that predict treatment response and prognosis. The metallothionein (MT), a low-molecular weight protein with high cysteine content, seems to be related to neoplastic resistance to oncologic treatment and therefore has been studied as a prognostic factor for a variety of human malignant tumors. The nuclear factor B (NF-B) plays an important role in the activation of the genes that code for immunity, survival, inflammation, apoptosis and in the cell protection for radiation and chemotherapy. The serine/threonine protein kinase Akt is a downstream target of phosphatidylinositol-3-kinase and it plays a key regulator of cancerous cell growth. Therefore, we have examined the MT, NF-kB and pAkt expression in 51 samples of oral squamous cell carcinoma by immunohistochemistry in order to investigate their prognostic influence on oral cancer, as well as studying the correlations between clinical factors and patient survival. The results showed a significant association between pAkt and NF-kB and between MT and NF-kB expression in tumor tissue. Besides pAkt over-expression was found in OSCC clinical samples and its expression was significantly associated with a poor overall patient survival. In conclusion, our findings suggested that pAkt expression may have therapeutic implications in squamous cell carcinoma.

Akt

Carcinoma epidermóide

Metallothionein

Metalotioneína

NF-kB

NF-kB

pAkt

Sobrevida.

Survival.

Regulation of angiogenic processes in omental endothelial cells during metastasis of epithelial ovarian cancer

Pranjol, Md Zahidul Islam

January 2017

Epithelial ovarian cancer frequently metastasizes to the omentum, a process that requires pro-angiogenic activation of local microvascular endothelial cells (ECs) by tumour-secreted factors. We have previously shown that ovarian cancer cells secrete factors, other than vascular endothelial growth factor (VEGF), with possible roles in metastatic angiogenesis including the lysosomal proteases cathepsin L (CathL) and cathepsin D (CathD), and insulin-like growth factor binding protein 7 (IGFBP7). However, the mechanisms by which these factors may contribute to omental endothelial angiogenic changes are unknown. Therefore the aims of this thesis were a) to examine disease relevant human omental microvascular endothelial cell (HOMEC) proliferation, migration and angiogenesis tube-formation induced by CathL, CathD and IGFBP7; b) to investigate whether CathL and CathD act via a proteolytic or non-proteolytic mechanism; c) to identify activated downstream intracellular signalling cascades in HOMECs and their activation in proliferation and migration; and finally d) to identify activated cell surface receptors by these factors. CathL, CathD and IGFBP7 significantly induced proliferation and migration in HOMECs, with CathL and CathD acting in a non-proteolytic manner. Proteome-profiler and ELISA data identified increased phosphorylation of the ERK1/2 and AKT (protein kinase B) pathways in HOMECs in response to these factors. CathL induced HOMEC proliferation and migration via the ERK1/2 pathway, whereas, although CathD-induced proliferation was mediated by activation of ERK1/2, its migratory effect was dependent on both ERK1/2 and AKT pathways. Interestingly, CathL induced secretion of galectin-1 (Gal1) from HOMECs which in turn significantly induced HOMEC proliferation via ERK1/2. However, none of the ERK1/2 or AKT pathways was observed to be active in Gal1-induced HOMEC migration. Interestingly, Gal1-induced proliferation and migration were significantly inhibited by L-glucose, suggesting a role for a receptor with extracellular sugar moieties. IGFBP7-induced migration was shown to be mediated via activation of the ERK1/2 pathway only. CathL, Gal1 and IGFBP7 significantly induced angiogenesis tube-formation in HOMECs which was not observed in CathD-treated cells. Receptor tyrosine kinase array revealed activation of Tie-1 and VEGF receptor type 2 (VEGFR2) in CathL and IGFBP7-treated HOMECs respectively. In conclusion, all CathL, CathD, Gal1 and IGFBP7 have the potential to act as proangiogenic factors in the metastasis of ovarian cancer to the omentum. These in vitro data suggest all four factors activate intracellular pathways which are involved in well-known angiogenesis models.

610