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Detection and Segmentation of Brain Metastases with Deep Convolutional NetworksLosch, Max January 2015 (has links)
As deep convolutional networks (ConvNets) reach spectacular results on a multitude of computer vision tasks and perform almost as well as a human rater on the task of segmenting gliomas in the brain, I investigated the applicability for detecting and segmenting brain metastases. I trained networks with increasing depth to improve the detection rate and introduced a border-pair-scheme to reduce oversegmentation. A constraint on the time for segmenting a complete brain scan required the utilization of fully convolutional networks which reduced the time from 90 minutes to 40 seconds. Despite some present noise and label errors in the 490 full brain MRI scans, the final network achieves a true positive rate of 82.8% and 0.05 misclassifications per slice where all lesions greater than 3 mm have a perfect detection score. This work indicates that ConvNets are a suitable approach to both detect and segment metastases, especially as further architectural extensions might improve the predictive performance even more.
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Treating Metastatic Brain Cancers With Stem CellsSadanandan, Nadia, Shear, Alex, Brooks, Beverly, Saft, Madeline, Cabantan, Dorothy Anne Galang, Kingsbury, Chase, Zhang, Henry, Anthony, Stefan, Wang, Zhen Jie, Salazar, Felipe Esparza, Lezama Toledo, Alma R., Rivera Monroy, Germán, Vega Gonzales-Portillo, Joaquin, Moscatello, Alexa, Lee, Jea Young, Borlongan, Cesario V. 24 November 2021 (has links)
Stem cell therapy may present an effective treatment for metastatic brain cancer and glioblastoma. Here we posit the critical role of a leaky blood-brain barrier (BBB) as a key element for the development of brain metastases, specifically melanoma. By reviewing the immunological and inflammatory responses associated with BBB damage secondary to tumoral activity, we identify the involvement of this pathological process in the growth and formation of metastatic brain cancers. Likewise, we evaluate the hypothesis of regenerating impaired endothelial cells of the BBB and alleviating the damaged neurovascular unit to attenuate brain metastasis, using the endothelial progenitor cell (EPC) phenotype of bone marrow-derived mesenchymal stem cells. Specifically, there is a need to evaluate the efficacy for stem cell therapy to repair disruptions in the BBB and reduce inflammation in the brain, thereby causing attenuation of metastatic brain cancers. To establish the viability of stem cell therapy for the prevention and treatment of metastatic brain tumors, it is crucial to demonstrate BBB repair through augmentation of vasculogenesis and angiogenesis. BBB disruption is strongly linked to metastatic melanoma, worsens neuroinflammation during metastasis, and negatively influences the prognosis of metastatic brain cancer. Using stem cell therapy to interrupt inflammation secondary to this leaky BBB represents a paradigm-shifting approach for brain cancer treatment. In this review article, we critically assess the advantages and disadvantages of using stem cell therapy for brain metastases and glioblastoma. / National Institutes of Health / Revisión por pares
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Defining the role of extravesicular TIMP1 in colorectal liver metastasesRao, Venkatesh Sadananda 18 April 2023 (has links)
Despite progress in our understanding of the molecular drivers that propagate the overall process of metastasis, the adaptation of specific organs upon these molecular interactions for metastatic entry remains poorly understood. This is particularly true for liver metastases, the liver being a common site for metastatic disease, and metastatic hepatic tumors are more prominent than primary hepatocellular or biliary tumors. Liver metastases most commonly arise from colorectal cancer than any other cancer and constitute one of the most detrimental outcomes of cancer, characterized by poor prognosis, high mortality, and no effective therapies available other than surgical interventions. Since interactions between tumour cells and the tumour microenvironment play an important part in the engraftment, survival, and progression of the metastases, the discovery of new drivers of liver metastasis with the potential to become therapeutic and preventive targets is required to advance the care of liver metastasis patients as well as cancer patients at risk of metastatic spread to the liver. The alteration of the physical structure of the tissue is extremely important in the progression of malignant diseases, such as cancer metastasis, as it directly affects the extravasation and colonization of tumour cells. The major hurdles in liver metastasis research, stem not only from our insufficient understanding of the molecular mechanisms directing and mediating metastasis particularly to the liver but also from the limited number of pre-clinical models available that mimic human disease and enable the study of the complex interactions between tumor cells and the liver microenvironment. The liver metastatic process underlies the acquisition of key adaptations by tumor-derived factors and is determined by both tumour-intrinsic properties and the crosstalk between tumour cells and stromal cells in the liver. A normal functioning and structurally intact extracellular matrix (ECM) constitute a hostile “soil” for seeding tumor cells to colonize. Eventually, it is the ability of tumor cells to remodel the liver microenvironment and create a supportive niche for metastatic tumor cell survival and outgrowth that determines successful metastatic colonization. Among tumour-secreted factors, which are recognized as major contributors to the formation of pre-metastatic and metastatic niches, tumor-derived extracellular vesicles (EVs) have recently arisen as crucial players in cell-to-cell communication and in the remodeling of distant microenvironments that favor organ-specific metastasis. Therefore, we sought to determine the role of tumor-derived EVs in the modulation of the liver microenvironment and their specific contribution to supporting metastatic colonization of the liver. The preliminary step to this process was to establish a model system to identify EV-associated targets and their effect on the ECM remodelling. Immunohistochemical analyses of primary colon tumour (CRC) and secondary liver metastases (CRC liver MET) tissue samples from patients with CRC revealed higher stromal TIMP1 levels in CRC liver MET than in CRC. The elevated stromal TIMP1 signature in the invasive front was associated with poor progression-free survival in patients with CRC liver MET. Our characterisation of the CRC tumour-derived EVs showed TIMP1 enrichment in the EVs (TIMP1EV) compared to its parental cell. Using cultures of primary liver fibroblasts, we could demonstrate that TIMP1 enrichment in the CRC-EVs was associated with regulation of TIMP1 levels in the EV-conditioned liver fibroblasts. Using our optimized ex vivo 3D ECM remodelling assay, we observed that pre-conditioning the liver fibroblasts with EVs from CRC cells promotes ECM remodelling. In accordance with our cell line model, we showed that serum-derived TIMP1EV from CRC patients promotes ECM remodelling. Moreover, high serum TIMP1EV expression in CRC liver MET patients was significantly associated with poor overall survival. In addition, our data also indicated that the determination of EV-associated TIMP1 is superior for non-invasive diagnosis than the analysis of soluble TIMP1 from total serum. Finally, we showed that HSP90AA is constitutively bound to TIMP1EV and that targeting HSP90AA leads to TIMP1 downregulation and inhibits ECM-mediated remodelling. This study defining the contribution of extravesicular TIMP1 to liver metastasis brings a novel insight into the molecular mechanisms through which tumor-secreted factors packaged via EVs promote remodelling of the liver microenvironment. The clinical significance of overexpression of extravesicular TIMP1 in patients with colorectal liver metastases highlights its potential as a prognostic biomarker and therapeutic target. With further clinical studies, Heparin and HSP90 inhibitors targeting the EV mediated TIMP1 regulation could be a putative treatment strategy to treat colorectal liver metastases.:Table of Contents
Abbreviations v
1. Introduction 1
1.1 Colorectal cancer 1
1.1.1. Incidence and mortality 1
1.1.1. Tumor staging 2
1.1.1. Pattern of distant metastases in colorectal cancer 5
1.2 Colorectal liver metastases 6
1.2.1 Current evaluation and treatment strategies for colorectal liver metastases 7
1.2.2 The liver metastasis cascade - a multi-step process 10
1.3 Tumor microenvironment 12
1.3.1 Tumour-stroma interactions 15
1.3.2 ECM remodelling and its role in CRC tumor progression 17
1.4 Extracellular vesicles 21
1.4.1 EV types 21
1.4.2 Biogenesis and secretion of EVs 22
1.4.3 Molecular composition of EVs 24
1.4.4 Biological functions of EVs 26
1.4.5 EVs in Tumor microenvironment 28
1.4.6 EVs in Tumor-fibroblast communication 29
1.4.7 Role of EVs in colorectal cancer 31
1.5 Tissue inhibitor of metalloproteinases (TIMP1) 35
1.5.1 TIMP1 in cancer 37
2. Background and Research Aims 39
3. Material and Methods 40
3.1 Material 40
3.1.1 Devices 40
3.1.2 Additional material and equipment 42
3.1.3 Fine chemicals 43
3.1.4 Biochemicals 45
3.1.5 Primary antibodies 46
3.1.6 Secondary antibodies 47
3.1.7 Nucleic acids 47
3.1.8 Consumables 50
3.1.9 Softwares 51
3.2 Methods 52
3.2.1 Patients 52
3.2.2 Immunohistochemistry 52
3.2.3 Hematoxylin eosin staining 54
3.2.4 Cell lines 54
3.2.5 Primary liver fibroblast cell lines 54
3.2.6 Passaging and freezing of cells 55
3.2.7 Revival of frozen cells 55
3.2.8 Cell counting 56
3.2.9 EV Isolation from CRC cell lines 56
3.2.10 Isolation of serum-derived EVs from liquid biopsies 56
3.2.11 Characterisation of EVs 57
3.2.12 Treatment of Fibroblasts with EVs 58
3.2.13 Stimulation of PFs with recombinant TIMP1 59
3.2.14 RNA isolation 59
3.2.15 cDNA synthesis 59
3.2.16 Quantitative Real-Time PCR (qRT-PCR) 60
3.2.17 Protein quantification 61
3.2.18 Immunoblotting and co-immunoprecipitation 61
3.2.19 ELISA 62
3.2.20 TIMP1 Knock-Out (KO) and Over-Expression (OE) 62
3.2.21 17 AAG and HSP90AA antibody treatment 63
3.2.22 3D ECM-remodelling assay 63
3.2.23 PKH staining 65
3.2.24 In vivo experiments 65
3.2.25 DAPI staining 66
3.2.26 Tissue explant model 66
3.2.27 Statistical analysis and reproducibility 67
4. Results 68
4.1 Identification of TIMP1 as target molecule 68
4.1.1 Identification of TIMP1 as a target through data mining 68
4.1.2 Localization pattern of TIMP1 in CRC and CRC liver MET 70
4.1.3 Invasion front-specific overexpression of TIMP1 in the stroma of patients with CRC liver MET is associated with poor progression-free survival (PFS) 72
4.2 Model system to study CRC-EV mediated ECM remodelling 73
4.2.1 Investigating the role of CRC- derived EVs in the evolution of colorectal liver metastases 73
4.2.2 Characterizsation of isolated EVs from the CRC cell lines 74
4.2.3 TIMP1 enrichment in EVs derived from CRC cell lines 75
4.2.4 CRC-derived TIMP1EV regulates TIMP1 levels in recipient fibroblasts 76
4.2.5 TIMP1EV mediated TIMP1 upregulation in the recipient fibroblast is an EV-mediated effect 79
4.2.6 Recombinant TIMP-1 induces TIMP1 levels in recipient pFs in a time- and concentration-dependent manner 81
4.2.7 Alteration of TIMP1 levels in HCT 116 cells translates into EVs but does not affect EV packaging. 83
4.2.8 TIMP1EV levels in CRC EVs determine TIMP1 levels in recipient fibroblasts 85
4.2.9 EV-mediated TIMP1 upregulation in pFs induces ECM remodelling 86
4.2.10 TIMP1 levels in the PFs influence the extent of ECM remodelling 88
4.3 Clinical significance of TIMP1EV 89
4.3.1 TIMP1 enriched in serum-derived EVs of CRC patients compared to healthy controls 89
4.3.2 Serum derived TIMP1EV from CRC patients regulate TIMP1 levels in primary liver fibroblasts 91
4.3.3 Serum derived TIMP1EV from CRC patients promote ECM remodelling 93
4.3.4 TIMP1EV exhibits superior stratification power compared to soluble TIMP1 in liquid biopsies 93
4.3.5 TIMP1EV is a non-invasive independent prognostic marker in colorectal liver metastases 94
4.4 Targeting TIMP1EV mediated ECM remodelling 97
4.4.1 TIMP1EV binds to HSP90AA 97
4.4.2 HSP90 inhibition interferes with TIMP1 protein stabilisation 99
4.4.3 17AAG attenuates TIMP1EV-mediated ECM remodelling 101
4.5 EVs derived from murine CRC cell lines regulate TIMP1 levels in recipient fibroblasts 104
4.6 Increased homing of CRC EVs to the liver compared to other organs 106
4.7 TIMPEV regulates TIMP1 levels in liver tissues 108
5. Discussion 112
5.1 TIMP1 Localization and its significance in liver metastases 112
5.2 Model system to study the role of CRC-EVs in liver metastasis 113
5.3 In-vitro model to study the pro-metastatic effects of TIMP1EV 114
5.4 Serum-derived extravesicular TIMP1 and its pro-metastatic functions underlying remodeling of the extracellular matrix 116
5.5 Clinical significance of TIMP1EV in colorectal liver metastases 117
5.6 Scope of HSP90 inhibitors in the prevention and treatment of CRC liver metastases...……………………………………………………………………………………..118
6. Future perspectives and concluding remarks 120
7. Graphical summary of the findings 122
Zusammenfassung 123
Summary 125
List of figures 127
List of Tables 129
References 130
Acknowledgements 163
Appendix 165
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Integrative Genomic Analyses of Patient-Matched Intracranial and Extracranial Metastases Reveal a Novel Brain-Specific Landscape of Genetic Variants in Driver Genes of Malignant MelanomaVáraljai, Renáta, Horn, Susanne, Sucker, Antje, Piercianek, Daniela, Schmitt, Verena, Carpinteiro, Alexander, Becker, Katrin Anne, Reifenberger, Julia, Roesch, Alexander, Felsberg, Jörg, Reifenberger, Guido, Sure, Ulrich, Schadendorf, Dirk, Helfrich, Iris 26 April 2023 (has links)
Background: Development of brain metastases in advanced melanoma patients is a frequent event that limits patients’ quality of life and survival. Despite recent insights into melanoma genetics, systematic analyses of genetic alterations in melanoma brain metastasis formation are lacking. Moreover, whether brain metastases harbor distinct genetic alterations beyond those observed at different anatomic sites of the same patient remains unknown. Experimental Design and Results: In our study, 54 intracranial and 18 corresponding extracranial melanoma metastases were analyzed for mutations using targeted next generation sequencing of 29 recurrently mutated driver genes in melanoma. In 11 of 16 paired samples, we detected nucleotide modifications in brain metastases that were absent in matched metastases at extracranial sites. Moreover, we identified novel genetic variants in ARID1A, ARID2, SMARCA4 and BAP1, genes that have not been linked to brain metastases before; albeit most frequent mutations were found in ARID1A, ARID2 and BRAF. Conclusion: Our data provide new insights into the genetic landscape of intracranial melanoma metastases supporting a branched evolution model of metastasis formation.
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Randomised, placebo-controlled, phase 3 trial of the effect of the omega-3 polyunsaturated fatty acid eicosapentaenoic acid (EPA) on colorectal cancer recurrence and survival after surgery for resectable liver metastases: EPA for Metastasis Trial 2 (EMT2) study protocolHull, M.A., Ow, P.L., Ruddock, S., Brend, T., Smith, A.F., Marshall, H., Song, M., Chan, A.T., Garrett, W.S., Yilmaz, O., Drew, D.A., Collinson, F., Cockbain, A.J., Jones, R., Loadman, Paul, Hall, P.S., Moriarty, C., Cairns, D.A., Toogood, G.J. 30 November 2023 (has links)
Yes / There remains an unmet need for safe and cost-effective adjunctive treatment of advanced colorectal
cancer (CRC). The omega-3 polyunsaturated fatty acid
eicosapentaenoic acid (EPA) is safe, well-tolerated and
has anti-inflammatory as well as antineoplastic properties.
A phase 2 randomised trial of preoperative EPA free fatty
acid 2 g daily in patients undergoing surgery for CRC liver
metastasis showed no difference in the primary endpoint
(histological tumour proliferation index) compared with
placebo. However, the trial demonstrated possible benefit
for the prespecified exploratory endpoint of postoperative
disease-free survival. Therefore, we tested the hypothesis
that EPA treatment, started before liver resection surgery
(and continued postoperatively), improves CRC outcomes
in patients with CRC liver metastasis.
Methods and analysis: The EPA for Metastasis Trial 2 trial
is a randomised, double-blind, placebo-controlled, phase 3
trial of 4 g EPA ethyl ester (icosapent ethyl (IPE; Vascepa))
daily in patients undergoing liver resection surgery for
CRC liver metastasis with curative intent. Trial treatment
continues for a minimum of 2 years and maximum of
4 years, with 6monthly assessments, including quality
of life outcomes, as well as annual clinical record review
after the trial intervention. The primary endpoint is CRC
progression-free survival. Key secondary endpoints are
overall survival, as well as the safety and tolerability of IPE.
A minimum 388 participants are estimated to provide 247
CRC progression events during minimum 2-year follow-up,
allowing detection of an HR of 0.7 in favour of IPE, with a
power of 80% at the 5% (two sided) level of significance,
assuming drop-out of 15%.
Ethics and dissemination: Ethical and health research
authority approval was obtained in January 2018. All data
will be collected by 2025. Full trial results will be published
in 2026. Secondary analyses of health economic data,
biomarker studies and other translational work will be
published subsequently.
Trial registration number NCT03428477. / The EMT2 trial is funded by Yorkshire Cancer Research (L387) and is sponsored by the University of Leeds. The EMT2 biospecimen collection is funded by the National Institutes of Health (1R01CA243454-01A1) and is sponsored by the University of Leeds ( governance-ethics@ leeds. ac. uk). Both studies have been adopted to the NIHR Clinical Research Network (CRN) Portfolio (CPMS ID 34700 and 47372, respectively) and have benefited from CRN research staff support.
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Disease-Specific Survival in Prostate Cancer Patients : Results from the Scandinavian Prostate Cancer Group (SPCG) Trial No. 5 and Regional Cancer Register DataKlaff, Rami January 2016 (has links)
Introduction Prostate cancer (PCa) is the most common cancer among men in Sweden. The clinical course varies considerably, which makes it difficult to predict the prognosis in the individual case. In order to explore the early as well as the late course of the disease, large study groups and population-based cohorts are necessary. Aims To explore factors that influence the long-term outcome of men with low-risk tumours in a population-based register, to predict the long-term course, and to assess the mortality rate for men with prostate cancer (Paper I) To analyse long-term outcome and to investigate factors associated with long-term survival in patients with metastases to the skeleton (Paper II) To analyse early androgen deprivation treatment (ADT) failure and to define clinical predictors associated with short survival due to early ADT failure in prostate cancer patients with bone metastases (Paper III) To analyse the prognostic significance of the extent of bone metastases in relation to other pretreatment variables in prostate cancer patients, and to explore the impact of bone metastases on quality-of-life (Paper IV) Material and methods The study groups were assembled from The South East Region Prostate Cancer Register (SERPCR), and The Scandinavian Prostate Cancer Group (SPCG) Trial No. 5. In the first study, prognostic factors and long-term disease-specific mortality rates of low-risk prostate cancer patients from the early PSA era were analysed. In the second study, patient-related factors, quality-of-life (QoL) and long-term survival in 915 PCa patients with bone metastases (M1b) under ADT, were analysed. In Study III factors predicting primary failure to respond to ADT were identified. Study IV explored the impact of the extent of bone metastases on survival and QoL for these men. Result and conclusions The long-term disease-specific mortality of low-risk localised PCa is low, but the annual mortality rate gradually increases. This indicates that some tumours slowly develop into lethal cancer, particularly in men 70 years or older and with a PSA level ≥ 4 μg/L. From the SPCG Trial No. 5, a subgroup of patients with M1b disease and favourable set of predictive factors survived more than 10 years under ADT with an acceptable QoL. Independent predictors of long-term survival were identified as performance status (PS) < 2, limited extent of bone metastases, and a PSA level < 231 μg/L at the time of enrolment in the trial. However, four independent clinical predictors of early ADT failure could be defined. Men exhibiting these features should be considered for an alternative treatment. Patient grouping based on three categories of extent of bone metastases related to PS, haemoglobin, and QoL at presentation, as independent predictors of mortality, may provide improved accuracy of prognosis.
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Modélisation, analyse mathématique de thérapies anti-cancéreuses pour les cancers métastatiquesBenzekry, Sébastien 10 November 2011 (has links)
Nous introduisons un modèle mathématique d'évolution d'une maladie cancéreuse à l'échelle de l'organisme, prenant en compte les métastases ainsi que leur taille et permettant de simuler l'action de plusieurs thérapies telles que la chirurgie, la chimiothérapie ou les traitements anti-angiogéniques. Le problème mathématique est une équation de renouvellement structurée en dimension deux. Son analyse mathématique ainsi que l'analyse fonctionnelle d'un espace de Sobolev sous-jacent sont effectuées. Existence, unicité, régularité et comportement asymptotique des solutions sont établis dans le cas autonome. Un schéma numérique lagrangien est introduit et analysé, permettant de prouver l'existence de solutions dans le cas non-autonome. L'effet de la concentration de la donnée au bord en une masse de Dirac est aussi envisagé.Le potentiel du modèle est ensuite illustré pour des problématiques cliniques telles que l'échec des anti-angiogéniques, les protocoles temporels d'administration pour la combinaison d'une chimiothérapie et d'un anti-angiogénique et les chimiothérapies métronomiques. Pour tenter d'apporter des réponses mathématiques à ces problèmes cliniques, un problème de contrôle optimal est formulé, analysé et simulé. / We introduce a mathematical model for the evolution of a cancer disease at the organism scale, taking into account for the metastases and their sizes as well as action of several therapies such as primary tumor surgery, chemotherapy and anti-angiogenic therapy. The mathematical problem is a renewal equation with bi-dimensional structuring variable. Mathematical analysis and functional analysis of an underlying Sobolev space are performed. Existence, uniqueness, regularity and asymptotic behavior of the solutions are proven in the autonomous case. A lagrangian numerical scheme is introduced and analyzed. Convergence of this scheme proves existence in the non-autonomous case. The effect of concentration of the boundary data into a Dirac mass is also investigated.Possible applications of the model are numerically illustrated for clinical issues such as the failure of anti-angiogenic monotherapies, scheduling of combined cytotoxic and anti-angiogenic therapies and metronomic chemotherapies. In order to give mathematical answers to these clinical problems an optimal control problem is formulated, analyzed and simulated.
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Imagerie des métastases hépatiques colorectales à l’ère des résections chirurgicales complexes : peut-on en améliorer la spécificité ? / Imaging of colorectal cancer liver metastases in the era of complex surgical resections : can we improve its specificity?Milot, Laurent 19 March 2019 (has links)
Les métastases hépatiques du cancer colorectal (MHCR) sont fréquentes et sont associées à une mortalité significative. Ces dernières décennies, des progrès thérapeutiques importants ont permis d'en améliorer le pronostic. Plus particulièrement, le rôle des résections hépatiques s'est considérablement élargi dans la maladie métastatique limitée au foie, conduisant à un changement radical dans la prise en charge. Ceci a naturellement eu des répercussions sur l'imagerie, qui doit être très performante au niveau lésionnel, nécessitant des sensibilité et spécificité très élevées. Si les techniques modernes ont permis une amélioration très nette en termes de sensibilité, en particulier grâce aux produits de contraste hépatospécifiques et de l'imagerie pondérée en diffusion, l'amélioration de la spécificité est moins claire et moins bien évaluée. Pourtant, la spécificité est tout aussi importante dans ce contexte, où les erreurs diagnostiques sont coûteuses, avec des chirurgies inutiles en cas de faux positifs, et des résections incomplètes en cas de faux négatifs. Ces deux situations sont accompagnées d'une morbi-mortalité très importante. Le présent travail de thèse va donc explorer de nouvelles pistes dont l'objectif ultime serait d'améliorer la spécificité de l'imagerie des MHCR. La première étude confronte l'apparence des métastases d'origine colorectale en IRM de haute résolution et leur histologie sous-jacente. Cette étude originale démontre que la fibrose tumorale apparait en hypersignal T2 et la nécrose tumorale en hyposignal T2 et hypersignal T1, ce qui va à l'encontre du dogme classique. La seconde étude explore la faisabilité de la fusion d'images IRM/échographie dans l'exploration de lésions hépatiques focales chez des patients ayant un cancer colorectal. Cette étude montre qu'un nombre significatif de lésions ne peuvent être visualisées à l'échographie qu'en utilisant la fusion, ouvrant la voie à une meilleure caractérisation lésionnelle en combinant les atouts de l'échographie et de l'IRM. Enfin, la troisième étude, complétée d'une revue iconographique, analyse le comportement IRM des lésions hépatiques après injection d'un produit de contraste intravasculaire. Elle montre une accumulation progressive du contraste au sein des angiomes, mais pas dans les métastases, conduisant à des apparences très différentes sur la phase tardive. Ceci était aussi observé dans les lésions de petites tailles, ce qui devrait permettre une meilleure spécificité dans les cas difficiles / Colorectal cancer liver metastases (CRCLM) are common and result in significant mortality. During the past decades, important therapeutic advances have improved the prognosis signficantly, especially through a marked expansion of the role of hepatic resections in liverlimited metastatic disease, leading to a radical change in management. This was naturally accompanied by an equally radical change in the imaging paradigm, now centered at the lesion level and not at the patient level, requiring very high sensitivity and specificity. While modern techniques have allowed a significant improvement in terms of sensitivity, especially through the use of hepatospecific contrast agents and diffusion imaging, the benefits in term of specificity are less clear, with only few studies focusing on and reporting the specificity of the techniques. However, specificity is equally important in this context, where diagnostic errors are costly, resulting either in unnecessary surgeries in case of false positives or in incomplete resections in case of false negatives. In this setting, our thesis will examine the results of three studies, which objective is to offer possible solutions to better understand the imaging of metastases and improve the specificity of liver imaging of CRCLM. The first study analyzes the association between high resolution MRI appearance of CRCLM and their underlying histology, showing that tumor fibrosis was in hypersignal on T2 Weighted Imaging while tumor necrosis was in hyposignal on T2 Weighted Imaging and hypersignal on T1 Weighted Imaging, which goes against the classical teaching about these lesions. The second study assesses the feasibility of using an MRI/Ultrasound fusion system in the exploration of liver lesions in patients with colorectal cancer. This study shows that more lesions were detected with ultrasound when using the fusion system, suggesting that a fusion system may allow a better characterization of lesions by combining the complementary information of MRI and ultrasound. Finally, the third study and its accompanying pictorial essay, explored the behavior of liver lesions after injection of an intravascular contrast agent. The main finding of this study was that hemangioma were accumulating the contrast over time while metastases were not, a key differentiating feature. This finding was found even in small lesions, often difficult to diagnose, suggesting that using such contrast in the exploration of liver lesions in patients with CRCLM would result in a higher specificity of the method
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Maturation protéolytique par les proprotéines convertases (PCs) dans l'angiogenèse, l'oncogenèse et l'infection virale : identification et étude de deux substrats des PCs / Proteolytic maturation by Proprotein Convertases (PCs) in angiogenesis, oncogenesis and viral infection : iIdentification and study of two PCs substratesDemoures, Béatrice 09 December 2016 (has links)
Les proprotéines convertases (PCs) sont des enzymes impliquées de nombreux processus pathologiques. Nous avons étudié deux substrats des PCs: l'apeline et la glycoprotéine B (gB) du virus d'Epstein Barr (EBV), et le rôle de cette maturation protéolytique dans la médiation de leurs fonctions. L'apeline est surexprimée dans plusieurs cancers dont le cancer colorectal (CCR), et nous avons montré que la furine, un membre des PCs, clive l’apeline. Pour déterminer le rôle de ce clivage dans le CCR métastatique, nous avons généré un mutant non clivable (apeline-DM). In vitro, ce mutant inhibe la croissance de cellules cancéreuses du côlonet ne les protège pas de l'apoptose, contrairement à l'apeline sauvage. In vivo, l'apeline-DM diminue drastiquement la croissance tumorale et la formation de métastases hépatiques chez la souris. Les mêmes résultats sont obtenus dans des modèles de souris déficientes pour l’apeline, démontrant l'intérêt d'utiliser l'apeline-DM ou des dérivés comme potentiels agents anticancéreux dans le traitement des CCR métastatiques. La gB du virus EBV, virus impliqué dans certains cancers lymphoïdes et épithéliaux chez l'homme, permet l'entrée du virus dans la cellule lors de l'infection. Nous avons montré que les PCs, et notamment la furine, clivent la gB. In vitro, l'induction de la protéine virale LMP1 augmente l'expression de la furine, qui se traduit par une augmentation de l'infection par EBV. Ces résultats suggèrent l'existence d'une boucle de régulation entre la furine et LMP1 permettant d'améliorer la propagation cellulaire du virus. L'utilisation d'inhibiteurs de l'activité des PCs permettrait donc de bloquer l'infection par EBV. / Proprotein convertases (PCs) are enzymes involved in many pathological processes. We have identified two novel substrates of the PCs: apelin and glycoprotein B (gB) of Epstein Barr Virus (EBV), and studied the role of PC-mediated proteolytic maturation in their functions. Apelin is overexpressed in some cancers including colorectal cancer (CRC), and we demonstrated that furin, one of the PCs member, cleaves apelin in two peptides. To determine the role of apelin cleavage by furin in the metastatic CRC, we generated a non-cleavable mutant (apelin-DM). This mutant inhibited the growth of colon cancer cells in vitro and could not protect against apoptosis, unlike the wild-type apelin. In vivo, apelin-DM drastically reduces tumor growth and the formation of hepatic metastases in mice. These results were confirmed in apelin deficient mouse models thus demonstrating the potential interest of using apelin-DM, or its derivatives, as anticancer agents in the treatment of metastatic CRC. The gB of EBV, a virus involved in some lymphoid and epithelial cancers in humans, is involved in the entry of the virus into the cell during infection. We have shown that PCs, especially furin, cleave gB. In vitro,induction of the LMP1 viral protein increases furin expression, which results in an increase in EBV infection. These results suggest the existence of a regulatory loop between furin and LMP1 to improve the cellular propagation of the virus. The use of inhibitors of PCs activity would thus block EBV infection, a virus against which there is no treatment nowadays.
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Avaliação dos efeitos genotóxico e citotóxico do 153Sm-EDTMP em linfócitos periféricos de pacientes com metástase óssea / Evaluation of genotoxic and cytotoxic effects of 153Sm-EDTMP in peripheral blood lymphocytes of bone metastasis patientsSuzuki, Miriam Fussae 21 March 2003 (has links)
Neste estudo, foi determinado o dano celular em linfócitos periféricos após exposição ao 153Sm-EDTMP (Samário-153 etilenodiaminotetrametilenofosfonato) por meio da técnica de análise de micronúcleos e coloração diferencial. O 153Sm-EDTMP é um radiofármaco utilizado para alívio da dor em pacientes com metástase óssea. A análise da freqüência de micronúcleos em amostras sangüíneas de pacientes obtidas uma hora após a administração endovenosa do radiofármaco (41 MBq/kg) mostrou que não houve diferença estatística em relação aos valores basais em células binucleadas. Porém, a análise da distribuição do dano em células mononucleadas mostrou que os pacientes sem tratamento radioterápico prévio apresentaram um aumento significativo na freqüência de células com um micronúcleo e aqueles com tratamento radioterápico prévio, nas células com dois ou mais micronúcleos. Os experimentos in vitro realizados com exposição de sangue total a três concentrações radioativas de 153Sm-EDTMP (0,370; 0,555 e 1,110 MBq/mL) por uma hora mostraram um aumento na freqüência de micronúcleos e de células necróticas e apoptóticas com o aumento da dose de radiação. Foram construídas curvas dose-resposta para os indivíduos sadios e para os pacientes com metástases óssea sem prévio tratamento radioterápico. A comparação das curvas mostrou que os pacientes apresentaram uma radiossensibilidade mais alta que os indivíduos sadios tanto quanto a porcentagem de células com micronúcleos como de células mortas (necróticas e apoptóticas). / In this study the cellular damage in peripheral lymphocytes after exposure to 153Sm-EDTMP (Samarium-153 ethylenediaminetetrametylenephosphonate) was determined using the technique of micronuclei analysis and differential coloration. 153Sm- EDTMP is a radiopharmaceutical used for pain relief in patients with bone metastases. The analysis of the frequency of micronuclei in patient blood samples obtained one hour after endovenous administration of radiopharmaceutical (41 MBq/kg) showed no statistical difference in relation to basal values in binucleated cells. However the analysis of damage distribution in mononucleated cells, showed that the patients without previous radiotherapic treatment presented a significant increase in the frequency of cells with one micronucleus and in those who had taken previous radiotherapic treatment, in cells with two or more micronuclei. The in vitro experiments conducted with the exposition of total blood to three radiation concentrations of 153Sm-EDTMP (0.370, 0.555 and 1.110 MBq/mL) during one hour showed an increase in the frequency of micronuclei and necrotic and apoptotic cells with increasing radiation dose. Dose-response curves for healthy donors and patients with bone metastasis without previous radiotherapic treatment were constructed. The comparison of the curves showed that patients presented higher radiosensitivity, either micronuclei or dead cell (necrotic or apoptotic) percentages, than healthy donors.
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