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4. HELIOS-expressing human CD8 T cells exhibit limited effector functions

Author

Neyens, Damien, primary, Hirsch, Thibault, additional, Abdel Aziz Issa Abdel Hadi, Achraqat, additional, Dauguet, Nicolas, additional, Vanhaver, Christophe, additional, Bayard, Alexandre, additional, Wildmann, Claude, additional, Luyckx, Mathieu, additional, Squifflet, Jean-Luc, additional, D’Hondt, Quentin, additional, Duhamel, Céline, additional, Huaux, Antoine, additional, Montiel, Virginie, additional, Dechamps, Mélanie, additional, and van der Bruggen, Pierre, additional

Published
2023
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10. HELIOS-expressing human CD8 T cells exhibit limited effector functions.

Author

Neyens, Damien, Hirsch, Thibault, Hadi, Achraqat Abdel Aziz Issa Abdel, Dauguet, Nicolas, Vanhaver, Christophe, Bayard, Alexandre, Wildmann, Claude, Luyckx, Mathieu, Squifflet, Jean-Luc, D'Hondt, Quentin, Duhamel, Céline, Huaux, Antoine, Montiel, Virginie, Dechamps, Mélanie, and van der Bruggen, Pierre

Subjects
T cells, SCURFIN (Protein), T cell receptors, T-cell exhaustion, REGULATORY T cells, CD8 antigen, IMMUNE response
Abstract

Introduction: The transcription factor HELIOS is primarily known for its expression in CD4 regulatory T cells, both in humans and mice. In mice, HELIOS is found in exhausted CD8 T cells. However, information on human HELIO+ CD8 T cells is limited and conflicting. Methods: In this study, we characterized by flow cytometry and transcriptomic analyses human HELIOS+ CD8 T cells. Results: These T cells primarily consist of memory cells and constitute approximately 21% of blood CD8 T cells. In comparison with memory HELIOST-BEThigh CD8 T cells that displayed robust effector functions, the memory HELIOS+ T-BEThigh CD8 T cells produce lower amounts of IFN-g and TNF-a and have a lower cytotoxic potential. We wondered if these cells participate in the immune response against viral antigens, but did not find HELIOS+ cells among CD8 T cells recognizing CMV peptides presented by HLA-A2 and HLA-B7. However, we found HELIOS+ CD8 T cells that recognize a CMV peptide presented by MHC class Ib molecule HLA-E. Additionally, a portion of HELIOS+ CD8 T cells is characterized by the expression of CD161, often used as a surface marker for identifying TC17 cells. These CD8 T cells express TH17/TC17-related genes encoding RORgt, RORa, PLZF, and CCL20. Discussion: Our findings emphasize that HELIOS is expressed across various CD8 T cell populations, highlighting its significance beyond its role as a transcription factor for Treg or exhausted murine CD8 T cells. The significance of the connection between HELIOS and HLA-E restriction is yet to be understood. [ABSTRACT FROM AUTHOR]

Published
2024
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12. BRAFV600E Expression in Thyrocytes Causes Recruitment of Immunosuppressive STABILIN-1 Macrophages

Author

Spourquet, Catherine, primary, Delcorte, Ophélie, additional, Lemoine, Pascale, additional, Dauguet, Nicolas, additional, Loriot, Axelle, additional, Achouri, Younes, additional, Hollmén, Maija, additional, Jalkanen, Sirpa, additional, Huaux, François, additional, Lucas, Sophie, additional, Meerkeeck, Pierre Van, additional, Knauf, Jeffrey A., additional, Fagin, James A., additional, Dessy, Chantal, additional, Mourad, Michel, additional, Henriet, Patrick, additional, Tyteca, Donatienne, additional, Marbaix, Etienne, additional, and Pierreux, Christophe E., additional

Published
2022
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14. Axon guidance genes control hepatic artery development.

Author

Gannoun, Lila, De Schrevel, Catalina, Belle, Morgane, Dauguet, Nicolas, Achouri, Younes, Loriot, Axelle, Vanderaa, Christophe, Cordi, Sabine, Alexandra Dili, Heremans, Yves, Rooman, Ilse, Leclercq, Isabelle A., Jacquemin, Patrick, Gatto, Laurent, and Lemaigre, Frédéric P.

Subjects
HEPATIC artery, VASCULAR smooth muscle, EPHRIN receptors, BILE ducts, LIVER regeneration, GENE silencing, HOMEOSTASIS, AXONS
Abstract

Earlier data on liver development demonstrated that morphogenesis of the bile duct, portal mesenchyme and hepatic artery is interdependent, yet how this interdependency is orchestrated remains unknown. Here, using 2D and 3D imaging, we first describe how portal mesenchymal cells become organised to form hepatic arteries. Next, we examined intercellular signalling active during portal area development and found that axon guidance genes are dynamically expressed in developing bile ducts and portal mesenchyme. Using tissue-specific gene inactivation in mice, we show that the repulsive guidance molecule BMP co-receptor A (RGMA)/neogenin (NEO1) receptor/ligand pair is dispensable for portal area development, but that deficient roundabout 2 (ROBO2)/ SLIT2 signalling in the portal mesenchyme causes reduced maturation of the vascular smooth muscle cells that form the tunica media of the hepatic artery. This arterial anomaly does not impact liver function in homeostatic conditions, but is associated with significant tissular damage following partial hepatectomy. In conclusion, our work identifies new players in development of the liver vasculature in health and liver regeneration. [ABSTRACT FROM AUTHOR]

Published
2023
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15. BRAFV600E Induction in Thyrocytes Triggers Important Changes in the miRNAs Content and the Populations of Extracellular Vesicles Released in Thyroid Tumor Microenvironment

Author

UCL - SSS/DDUV - Institut de Duve, UCL - SSS/DDUV/BCHM - Biochimie-Recherche métabolique, UCL - SSS/DDUV/CELL - Biologie cellulaire, UCL - SSS/DDUV/CBIO - Computational Biology and Bioinformatics, UCL - SSS/DDUV/GEPI - Epigénétique, Delcorte, Ophélie, Spourquet, Catherine, Lemoine, Pascale, Degosserie, Jonathan, Van Der Smissen, Patrick, Dauguet, Nicolas, Loriot, Axelle, Knauf, Jeffrey A., Gatto, Laurent, Marbaix, Etienne, Fagin, James A., Pierreux, Christophe, UCL - SSS/DDUV - Institut de Duve, UCL - SSS/DDUV/BCHM - Biochimie-Recherche métabolique, UCL - SSS/DDUV/CELL - Biologie cellulaire, UCL - SSS/DDUV/CBIO - Computational Biology and Bioinformatics, UCL - SSS/DDUV/GEPI - Epigénétique, Delcorte, Ophélie, Spourquet, Catherine, Lemoine, Pascale, Degosserie, Jonathan, Van Der Smissen, Patrick, Dauguet, Nicolas, Loriot, Axelle, Knauf, Jeffrey A., Gatto, Laurent, Marbaix, Etienne, Fagin, James A., and Pierreux, Christophe

Abstract

Papillary thyroid cancer (PTC) is the most common endocrine malignancy for which diagnosis and recurrences still challenge clinicians. New perspectives to overcome these issues could come from the study of extracellular vesicle (EV) populations and content. Here, we aimed to elucidate the heterogeneity of EVs circulating in the tumor and the changes in their microRNA content during cancer progression. Using a mouse model expressing BRAFV600E, we isolated and characterized EVs from thyroid tissue by ultracentrifugations and elucidated their microRNA content by small RNA sequencing. The cellular origin of EVs was investigated by ExoView and that of deregulated EV-microRNA by qPCR on FACS-sorted cell populations. We found that PTC released more EVs bearing epithelial and immune markers, as compared to the healthy thyroid, so that changes in EV-microRNAs abundance were mainly due to their deregulated expression in thyrocytes. Altogether, our work provides a full description of in vivo-derived EVs produced by, and within, normal and cancerous thyroid. We elucidated the global EV-microRNAs signature, the dynamic loading of microRNAs in EVs upon BRAFV600E induction, and their cellular origin. Finally, we propose that thyroid tumor-derived EV-microRNAs could support the establishment of a permissive immune microenvironment.

Published
2022

16. Identification and implication of tissue-enriched ligands in epithelial–endothelial crosstalk during pancreas development

Author

UCL - SSS/DDUV - Institut de Duve, UCL - SSS/DDUV/CELL - Biologie cellulaire, UCL - SSS/DDUV/CBIO - Computational Biology and Bioinformatics, UCL - SSS/DDUV/GECE - Génétique cellulaire, Moulis, Manon, Runser, Steve Vincent Maurice, Glorieux, Laura, Dauguet, Nicolas, Vanderaa, Christophe, Gatto, Laurent, Tyteca, Donatienne, Henriet, Patrick, Spagnoli, Francesca M., Iber, Dagmar, Pierreux, Christophe, UCL - SSS/DDUV - Institut de Duve, UCL - SSS/DDUV/CELL - Biologie cellulaire, UCL - SSS/DDUV/CBIO - Computational Biology and Bioinformatics, UCL - SSS/DDUV/GECE - Génétique cellulaire, Moulis, Manon, Runser, Steve Vincent Maurice, Glorieux, Laura, Dauguet, Nicolas, Vanderaa, Christophe, Gatto, Laurent, Tyteca, Donatienne, Henriet, Patrick, Spagnoli, Francesca M., Iber, Dagmar, and Pierreux, Christophe

Abstract

Development of the pancreas is driven by an intrinsic program coordinated with signals from other cell types in the epithelial environment. These intercellular communications have been so far challenging to study because of the low concentration, localized production and diversity of the signals released. Here, we combined scRNAseq data with a computational interactomic approach to identify signals involved in the reciprocal interactions between the various cell types of the developing pancreas. This in silico approach yielded 40,607 potential ligand‑target interactions between the different main pancreatic cell types. Among this vast network of interactions, we focused on three ligands potentially involved in communications between epithelial and endothelial cells. BMP7 and WNT7B, expressed by pancreatic epithelial cells and predicted to target endothelial cells, and SEMA6D, involved in the reverse interaction. In situ hybridization confirmed the localized expression of Bmp7 in the pancreatic epithelial tip cells and of Wnt7b in the trunk cells. On the contrary, Sema6d was enriched in endothelial cells. Functional experiments on ex vivo cultured pancreatic explants indicated that tip cell‑produced BMP7 limited development of endothelial cells. This work identified ligands with a restricted tissular and cellular distribution and highlighted the role of BMP7 in the intercellular communications contributing to vessel development and organization during pancreas organogenesis.

Published
2022

17. BRAFV600E expression in thyrocytes causes recruitment of immunosuppressive STABILIN-1 macrophages

Author

UCL - SSS/DDUV - Institut de Duve, UCL - SSS/DDUV/BCHM - Biochimie-Recherche métabolique, UCL - SSS/DDUV/CELL - Biologie cellulaire, UCL - SSS/DDUV/GECE - Génétique cellulaire, UCL - SSS/DDUV/GEPI - Epigénétique, UCL - SSS/DDUV/LPAD - Liver and pancreas differentiation, UCL - SSS/IREC/FATH - Pôle de Pharmacologie et thérapeutique, UCL - SSS/IREC/CHEX - Pôle de chirgurgie expérimentale et transplantation, UCL - SSS/IREC/LTAP - Louvain Centre for Toxicology and Applied Pharmacology, UCL - (SLuc) Service de radiologie, UCL - (SLuc) Service de chirurgie et transplantation abdominale, Spourquet, Catherine, Delcorte, Ophélie, Lemoine, Pascale, Dauguet, Nicolas, Loriot, Axelle, Achouri, Younes, Hollmén, Maija, Jalkanen, Sirpa, Huaux, François, Lucas, Sophie, Van Meerbeeck, Pierre, Knauf, Jeffrey, Fagin, James A., Dessy, Chantal, Mourad, Michel, Henriet, Patrick, Tyteca, Donatienne, Marbaix, Etienne, Pierreux, Christophe, UCL - SSS/DDUV - Institut de Duve, UCL - SSS/DDUV/BCHM - Biochimie-Recherche métabolique, UCL - SSS/DDUV/CELL - Biologie cellulaire, UCL - SSS/DDUV/GECE - Génétique cellulaire, UCL - SSS/DDUV/GEPI - Epigénétique, UCL - SSS/DDUV/LPAD - Liver and pancreas differentiation, UCL - SSS/IREC/FATH - Pôle de Pharmacologie et thérapeutique, UCL - SSS/IREC/CHEX - Pôle de chirgurgie expérimentale et transplantation, UCL - SSS/IREC/LTAP - Louvain Centre for Toxicology and Applied Pharmacology, UCL - (SLuc) Service de radiologie, UCL - (SLuc) Service de chirurgie et transplantation abdominale, Spourquet, Catherine, Delcorte, Ophélie, Lemoine, Pascale, Dauguet, Nicolas, Loriot, Axelle, Achouri, Younes, Hollmén, Maija, Jalkanen, Sirpa, Huaux, François, Lucas, Sophie, Van Meerbeeck, Pierre, Knauf, Jeffrey, Fagin, James A., Dessy, Chantal, Mourad, Michel, Henriet, Patrick, Tyteca, Donatienne, Marbaix, Etienne, and Pierreux, Christophe

Abstract

Papillary thyroid carcinoma (PTC) is the most frequent histological subtype of thyroid cancers (TC), and BRAFV600E genetic alteration is found in 60% of this endocrine cancer. This oncogene is associated with poor prognosis, resistance to radioiodine therapy and tumor progression. Histological follow-up by anatomo-pathologists reveals that 2/3 of surgically-removed thyroids do not present malignant lesions. Continued fundamental research into the molecular mechanisms of TC downstream of BRAFV600E remains thus central to better understand the clinical behavior of these tumors. To study PTC, we used a mouse model in which expression of BRAFV600E is specifically switched on in thyrocytes by doxycycline administration. Upon daily intraperitoneal doxycycline injection, thyroid tissue rapidly acquired histological features mimicking human PTC. Transcriptomic analysis revealed major changes in immune signaling pathways upon BRAFV600E induction. Multiplex immunofluorescence confirmed the abundant recruitment of macrophages, among which a population of LYVE-1+/CD206+/STABILIN-1+ was dramatically increased. By genetically inactivating the gene coding for the scavenger receptor STABILIN-1, we showed an increase of CD8+ T cells in this in situ BRAFV600E dependent TC. Finally, we demonstrated the presence of CD206+/STABILIN-1+ macrophages in human thyroid pathologies. Altogether, we revealed the recruitment of immunosuppressive STABILIN-1 macrophages a PTC mouse model and the relevance of these observations in human thyroid tissues.

Published
2022

18. Investigation of chalcogen bioisosteric replacement in a series of heterocyclic inhibitors of tryptophan 2,3-dioxygenase

Author

UCL - SSS/LDRI - Louvain Drug Research Institute, UCL - SSS/DDUV/GECE - Génétique cellulaire, Kozlova, Arina, Thabault, Léopold, Dauguet, Nicolas, Deskeuvre, Marine, Stroobant, Vincent, Pilotte, Luc, Liberelle, Maxime, Van den Eynde, Benoît, Frédérick, Raphaël, UCL - SSS/LDRI - Louvain Drug Research Institute, UCL - SSS/DDUV/GECE - Génétique cellulaire, Kozlova, Arina, Thabault, Léopold, Dauguet, Nicolas, Deskeuvre, Marine, Stroobant, Vincent, Pilotte, Luc, Liberelle, Maxime, Van den Eynde, Benoît, and Frédérick, Raphaël

Abstract

Selenium is an underexplored element that can be used for bioisosteric replacement of lower molecular weight chalcogens such as oxygen and sulfur. More studies regarding the impact of selenium substitution in different chemical scaffolds are needed to fully grasp this element's potential. Herein, we decided to evaluate the impact of selenium incorporation in a series of tryptophan 2,3-dioxygenase (TDO2) inhibitors, a target of interest in cancer immunotherapy. First, we synthesized the different chalcogen isosteres through Suzuki-Miyaura type coupling. Next, we evaluated the isosteres' affinity and selectivity for TDO2, as well as their lipophilicity, microsomal stability and cellular toxicity on TDO2-expressing cell lines. Overall, chalcogen isosteric replacements did not disturb the on-target activity but allowed for a modulation of the compounds' lipophilicity, toxicity and stability profiles. The present work contributes to our understanding of oxygen/sulfur/selenium isostery towards increasing structural options in medicinal chemistry for the development of novel and distinctive drug candidates.

Published
2022

19. BRAFV600E Induction in Thyrocytes Triggers Important Changes in the miRNAs Content and the Populations of Extracellular Vesicles Released in Thyroid Tumor Microenvironment

Author

Delcorte, Ophélie, primary, Spourquet, Catherine, additional, Lemoine, Pascale, additional, Degosserie, Jonathan, additional, Van Der Smissen, Patrick, additional, Dauguet, Nicolas, additional, Loriot, Axelle, additional, Knauf, Jeffrey A., additional, Gatto, Laurent, additional, Marbaix, Etienne, additional, Fagin, James A., additional, and Pierreux, Christophe E., additional

Published
2022
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21. BRAF V600E Expression in Thyrocytes Causes Recruitment of Immunosuppressive STABILIN-1 Macrophages.

Author

Spourquet, Catherine, Delcorte, Ophélie, Lemoine, Pascale, Dauguet, Nicolas, Loriot, Axelle, Achouri, Younes, Hollmén, Maija, Jalkanen, Sirpa, Huaux, François, Lucas, Sophie, Meerkeeck, Pierre Van, Knauf, Jeffrey A., Fagin, James A., Dessy, Chantal, Mourad, Michel, Henriet, Patrick, Tyteca, Donatienne, Marbaix, Etienne, and Pierreux, Christophe E.

Subjects
BIOLOGICAL models, INJECTIONS, THYROID gland tumors, PAPILLARY carcinoma, ONCOGENES, ANIMAL experimentation, MACROPHAGES, IMMUNOSUPPRESSION, DOXYCYCLINE, INTRAPERITONEAL injections, GENE expression, CELLULAR signal transduction, TRANSFERASES, EPITHELIAL cells, MICE
Abstract

Simple Summary: Incidence of thyroid cancer, including papillary thyroid cancer, is rapidly increasing. Oncogenes, such as the BRAFV600E, have been identified, and their effect on thyroid cancer cells have been studied in vitro and in mouse models. What is less understood is the impact of these mutations on thyroid cancer microenvironment and, in turn, the effect of changes in the microenvironment on tumor progression. We investigated the modifications in the cellular composition of thyroid cancer microenvironment using an inducible mouse model. We focused on a subpopulation of macrophages, expressing the STABILIN-1 protein, recruited in the thyroid tumor microenvironment following BRAFV600E expression. CRISPR/Cas9 genetic inactivation of Stablin-1 did not change macrophage recruitment but highlighted the immunosuppressive role of STABILIN-1-expressing macrophages. The identification of a similar subpopulation of STABILIN-1 macrophages in human thyroid diseases supports a conserved role for these macrophages and offers an opportunity for intervention. Papillary thyroid carcinoma (PTC) is the most frequent histological subtype of thyroid cancers (TC), and BRAFV600E genetic alteration is found in 60% of this endocrine cancer. This oncogene is associated with poor prognosis, resistance to radioiodine therapy, and tumor progression. Histological follow-up by anatomo-pathologists revealed that two-thirds of surgically-removed thyroids do not present malignant lesions. Thus, continued fundamental research into the molecular mechanisms of TC downstream of BRAFV600E remains central to better understanding the clinical behavior of these tumors. To study PTC, we used a mouse model in which expression of BRAFV600E was specifically switched on in thyrocytes by doxycycline administration. Upon daily intraperitoneal doxycycline injection, thyroid tissue rapidly acquired histological features mimicking human PTC. Transcriptomic analysis revealed major changes in immune signaling pathways upon BRAFV600E induction. Multiplex immunofluorescence confirmed the abundant recruitment of macrophages, among which a population of LYVE-1+/CD206+/STABILIN-1+ was dramatically increased. By genetically inactivating the gene coding for the scavenger receptor STABILIN-1, we showed an increase of CD8+ T cells in this in situ BRAFV600E-dependent TC. Lastly, we demonstrated the presence of CD206+/STABILIN-1+ macrophages in human thyroid pathologies. Altogether, we revealed the recruitment of immunosuppressive STABILIN-1 macrophages in a PTC mouse model and the interest to further study this macrophage subpopulation in human thyroid tissues. [ABSTRACT FROM AUTHOR]

Published
2022
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22. Peroxiredoxin-I Sustains Inflammation During Pancreatitis

Author

Buckens, Hortense, Pirenne, Sophie, Achouri, Younes, Dauguet, Nicolas, Dahou, Hajar, Baldan, Jonathan, Bouwens, Luc, Lemaigre, Frédéric, Jacquemin, Patrick, Assi, Mohamad, Faculty of Medicine and Pharmacy, Basic (bio-) Medical Sciences, Cell Differentiation, and UCL - SSS/DDUV/LPAD - Liver and pancreas differentiation

Subjects
medicine.medical_specialty, Inflammation, RC799-869, Gastroenterology, Mice, Internal medicine, Research Letter, Medicine, Animals, Medicine(all), Hepatology, Peroxiredoxin I, business.industry, Peroxiredoxin-I, Peroxiredoxins, Diseases of the digestive system. Gastroenterology, medicine.disease, Ctrl, control, PRX-I, mouse and human peroxiredoxin-1 protein, Pancreatitis, Cytokines, medicine.symptom, Inflammation Mediators, NF-κB, nuclear factor κB, business
Abstract

[no abstract available]

Published
2020

23. A Mouse Model of Cholangiocarcinoma Uncovers a Role for Tensin-4 in Tumor Progression.

Author

UCL - SSS/DDUV/LPAD - Liver and pancreas differentiation, Di-Luoffo, Mickaël, Pirenne, Sophie, Saandi, Thoueiba, Loriot, Axelle, Gérard, Claude, Dauguet, Nicolas, Manzano-Núñez, Fátima, Alves Souza Carvalhais, Natália, Lamoline, Florence, Cordi, Sabine, Konobrocka, Katarzyna, De Greef, Vitaline, Komuta, Mina, Halder, Georg, Jacquemin, Patrick, Lemaigre, Frédéric P, UCL - SSS/DDUV/LPAD - Liver and pancreas differentiation, Di-Luoffo, Mickaël, Pirenne, Sophie, Saandi, Thoueiba, Loriot, Axelle, Gérard, Claude, Dauguet, Nicolas, Manzano-Núñez, Fátima, Alves Souza Carvalhais, Natália, Lamoline, Florence, Cordi, Sabine, Konobrocka, Katarzyna, De Greef, Vitaline, Komuta, Mina, Halder, Georg, Jacquemin, Patrick, and Lemaigre, Frédéric P

Abstract

Earlier diagnosis and treatment of intrahepatic cholangiocarcinoma (iCCA) are necessary to improve therapy, yet limited information is available about initiation and evolution of iCCA precursor lesions. Therefore, there is a need to identify mechanisms driving formation of precancerous lesions and their progression toward invasive tumors using experimental models that faithfully recapitulate human tumorigenesis. To this end, we generated a mouse model which combines cholangiocyte-specific expression of Kras with 3,5-diethoxycarbonyl-1,4-dihydrocollidine (DDC) diet-induced inflammation to mimic iCCA development in patients with cholangitis. Histological and transcriptomic analyses of the mouse precursor lesions and iCCA were performed and compared with human analyses. The function of genes overexpressed during tumorigenesis was investigated in human cell lines. We found that mice expressing Kras in cholangiocytes and fed a DDC diet developed cholangitis, ductular proliferations, intraductal papillary neoplasms of bile ducts (IPNBs), and, eventually, iCCAs. The histology of mouse and human IPNBs was similar, and mouse iCCAs displayed histological characteristics of human mucin-producing, large-duct-type iCCA. Signaling pathways activated in human iCCA were also activated in mice. The identification of transition zones between IPNB and iCCA on tissue sections, combined with RNA-sequencing analyses of the lesions supported that iCCAs derive from IPNBs. We further provide evidence that tensin-4 (TNS4), which is stimulated by KRAS and SRY-related HMG box transcription factor 17, promotes tumor progression. We developed a mouse model that faithfully recapitulates human iCCA tumorigenesis and identified a gene cascade which involves TNS4 and promotes tumor progression.

Published
2021

24. Dynamic regulation of expression of KRAS and its effectors determines the ability to initiate tumorigenesis in pancreatic acinar cells.

Author

UCL - SSS/DDUV - Institut de Duve, Assi, Mohamad, Achouri, Younes, Loriot, Axelle, Dauguet, Nicolas, Dahou, Hajar, Baldan, Jonathan, Libert, Maxime, Fain, Jean, Guerra, Carmen, Bouwens, Luc, Barbacid, Mariano, Lemaigre, Frédéric, Jacquemin, Patrick, UCL - SSS/DDUV - Institut de Duve, Assi, Mohamad, Achouri, Younes, Loriot, Axelle, Dauguet, Nicolas, Dahou, Hajar, Baldan, Jonathan, Libert, Maxime, Fain, Jean, Guerra, Carmen, Bouwens, Luc, Barbacid, Mariano, Lemaigre, Frédéric, and Jacquemin, Patrick

Abstract

Pancreatic acinar cells are a cell type of origin for pancreatic cancer that become progressively less sensitive to tumorigenesis induced by oncogenic Kras mutations after birth. This sensitivity is increased when Kras mutations are combined with pancreatitis. Molecular mechanisms underlying these observations are still largely unknown. To identify these mechanisms, we generated the first CRISPR-edited mouse models that enable detection of wild-type and mutant KRAS proteins in vivo. Analysis of these mouse models revealed that more than 75% of adult acinar cells are devoid of detectable KRAS protein. In the 25% of acinar cells expressing KRAS protein, transcriptomic analysis highlighted a slight upregulation of the RAS and MAPK pathways. However, at the protein level, only marginal pancreatic expression of essential KRAS effectors, including C-RAF, was observed. The expression of KRAS and its effectors gradually decreased after birth. The low sensitivity of adult acinar cells to Kras mutations resulted from low expression of KRAS and its effectors and the subsequent lack of activation of RAS/MAPK pathways. Pancreatitis triggered expression of KRAS and its effectors as well as subsequent activation of downstream signaling; this induction required the activity of EGFR. Finally, expression of C-RAF in adult pancreas was required for pancreatic tumorigenesis. In conclusion, our study reveals that control of the expression of KRAS and its effectors regulates the sensitivity of acinar cells to transformation by oncogenic Kras mutations.

Published
2021

25. Peroxiredoxin-I Sustains Inflammation During Pancreatitis

Author

UCL - SSS/DDUV/LPAD - Liver and pancreas differentiation, Buckens, Hortense, Pirenne, Sophie, Achouri, Younes, Dauguet, Nicolas, Dahou, Hajar, Baldan, Jonathan, Bouwens, Luc, Lemaigre, Frédéric, Jacquemin, Patrick, Assi, Mohamad, UCL - SSS/DDUV/LPAD - Liver and pancreas differentiation, Buckens, Hortense, Pirenne, Sophie, Achouri, Younes, Dauguet, Nicolas, Dahou, Hajar, Baldan, Jonathan, Bouwens, Luc, Lemaigre, Frédéric, Jacquemin, Patrick, and Assi, Mohamad

Abstract

[no abstract available]

Published
2021

26. Dynamic Regulation of Expression of KRAS and Its Effectors Determines the Ability to Initiate Tumorigenesis in Pancreatic Acinar Cells

Author

Assi, Mohamad, primary, Achouri, Younes, additional, Loriot, Axelle, additional, Dauguet, Nicolas, additional, Dahou, Hajar, additional, Baldan, Jonathan, additional, Libert, Maxime, additional, Fain, Jean S., additional, Guerra, Carmen, additional, Bouwens, Luc, additional, Barbacid, Mariano, additional, Lemaigre, Frédéric P., additional, and Jacquemin, Patrick, additional

Published
2021
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28. Interplay Between Plasma Membrane Lipid Alteration, Oxidative Stress and Calcium-Based Mechanism for Extracellular Vesicle Biogenesis From Erythrocytes During Blood Storage

Author

Cloos, Anne-Sophie, primary, Ghodsi, Marine, additional, Stommen, Amaury, additional, Vanderroost, Juliette, additional, Dauguet, Nicolas, additional, Pollet, Hélène, additional, D’Auria, Ludovic, additional, Mignolet, Eric, additional, Larondelle, Yvan, additional, Terrasi, Romano, additional, Muccioli, Giulio G., additional, Van Der Smissen, Patrick, additional, and Tyteca, Donatienne, additional

Published
2020
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29. Abstract A07: Inflammation enables pancreatic acinar cells to overcome resistance to oncogenic Kras by increasing its expression and plasma membrane localization

Author

Assi, Mohamad Nabil, primary, Lodewyckx, Jean-Nicolas, additional, Achouri, Younes, additional, Gérard, Claude, additional, Dauguet, Nicolas, additional, Houbracken, Isabelle, additional, Heremans, Yves, additional, Tyteca, Donatienne, additional, Rooman, Ilse, additional, Bouwens, Luc, additional, Lemaigre, Frédéric, additional, and Jacquemin, Patrick, additional

Published
2020
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30. Mouse nidovirus LDV infection alleviates graft versus host disease and induces type I IFN‐dependent inhibition of dendritic cells and allo‐responsive T cells

Author

Gaignage, Mélanie, Marillier, Reece G., Uyttenhove, Catherine, Dauguet, Nicolas, Saxena, Anubha, Ryffel, Bernard, Michiels, Thomas, Coutelier, Jean‐Paul, and Van Snick, Jacques

Subjects
CD4-Positive T-Lymphocytes, Mice, Knockout, GVHD, Graft vs Host Disease, Dendritic Cells, CD8-Positive T-Lymphocytes, Nidovirales, Nidovirales Infections, Allografts, DC, nidovirus, Mice, Interferon Type I, Animals, type I IFN, Original Research
Abstract

Introduction Viruses have developed multiple mechanisms to alter immune reactions. In 1969, it was reported that lactate dehydrogenase‐elevating virus (LDV), a single stranded positive sense mouse nidovirus, delays skin allograft rejection and inhibits spleen alterations in graft versus host disease (GVHD). As the underlying mechanisms have remained unresolved and given the need for new therapies of this disease, we reassessed the effects of the virus on GVHD and tried to uncover its mode of action. Methods GVHD was induced by transfer of parent (B6) spleen cells to non‐infected or LDV‐infected B6D2F1 recipients. In vitro mixed‐lymhocyte culture (MLC) reactions were used to test the effects of the virus on antigen‐presenting cells (APC) and responder T cells. Results LDV infection resulted in a threefold increase in survival rate with reduced weight loss and liver inflammation but with the establishment of permanent chimerism that correlated with decreased interleukine (IL)‐27 and interferon (IFN)γ plasma levels. Infected mice showed a transient elimination of splenic CD11b+ and CD8α+ conventional dendritic cells (cDCs) required for allogeneic CD4 and CD8 T cell responses in vitro. This drop of APC numbers was not observed with APCs derived from toll‐like receptor (TLR)7‐deficient mice. A second effect of the virus was a decreased T cell proliferation and IFNγ production during MLC without detectable changes in Foxp3+ regulatory T cell (Tregs) numbers. Both cDC and responder T cell inhibition were type I IFN dependent. Although the suppressive effects were very transient, the GVHD inhibition was long‐lasting. Conclusion A type I IFN‐dependent suppression of DC and T cells just after donor spleen cell transplantation induces permanent chimerism and donor cell implantation in a parent to F1 spleen cell transplantation model. If this procedure can be extended to full allogeneic bone marrow transplantation, it could open new therapeutic perspectives for hematopoietic stem cell transplantation (HSCT).

Published
2017

31. BRAF V600E Induction in Thyrocytes Triggers Important Changes in the miRNAs Content and the Populations of Extracellular Vesicles Released in Thyroid Tumor Microenvironment.

Author

Delcorte, Ophélie, Spourquet, Catherine, Lemoine, Pascale, Degosserie, Jonathan, Van Der Smissen, Patrick, Dauguet, Nicolas, Loriot, Axelle, Knauf, Jeffrey A., Gatto, Laurent, Marbaix, Etienne, Fagin, James A., and Pierreux, Christophe E.

Subjects
EXTRACELLULAR vesicles, THYROID gland tumors, TUMOR microenvironment, THYROID cancer, NON-coding RNA, BRAF genes
Abstract

Papillary thyroid cancer (PTC) is the most common endocrine malignancy for which diagnosis and recurrences still challenge clinicians. New perspectives to overcome these issues could come from the study of extracellular vesicle (EV) populations and content. Here, we aimed to elucidate the heterogeneity of EVs circulating in the tumor and the changes in their microRNA content during cancer progression. Using a mouse model expressing BRAFV600E, we isolated and characterized EVs from thyroid tissue by ultracentrifugations and elucidated their microRNA content by small RNA sequencing. The cellular origin of EVs was investigated by ExoView and that of deregulated EV-microRNA by qPCR on FACS-sorted cell populations. We found that PTC released more EVs bearing epithelial and immune markers, as compared to the healthy thyroid, so that changes in EV-microRNAs abundance were mainly due to their deregulated expression in thyrocytes. Altogether, our work provides a full description of in vivo-derived EVs produced by, and within, normal and cancerous thyroid. We elucidated the global EV-microRNAs signature, the dynamic loading of microRNAs in EVs upon BRAFV600E induction, and their cellular origin. Finally, we propose that thyroid tumor-derived EV-microRNAs could support the establishment of a permissive immune microenvironment. [ABSTRACT FROM AUTHOR]

Published
2022
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32. Interplay Between Plasma Membrane Lipid Alteration, Oxidative Stress and Calcium-Based Mechanism for Extracellular Vesicle Biogenesis From Erythrocytes During Blood Storage.

Author

UCL - SSS/DDUV - Institut de Duve, UCL - SSS/DDUV/CELL - Biologie cellulaire, UCL - SSS/DDUV/GECE - Génétique cellulaire, UCL - SSS/IONS - Institute of NeuroScience, UCL - SSS/IONS/CEMO - Pôle Cellulaire et moléculaire, UCL - SSS/LDRI - Louvain Drug Research Institute, UCL - SST/LIBST - Louvain Institute of Biomolecular Science and Technology, Cloos, Anne-Sophie, Ghodsi, Marine, Stommen, Amaury, Vanderroost, Juliette, Dauguet, Nicolas, Pollet, Hélène, D'Auria, Ludovic, Mignolet, Eric, Larondelle, Yvan, Terrasi, Romano, Muccioli, Giulio, Van Der Smissen, Patrick, Tyteca, Donatienne, UCL - SSS/DDUV - Institut de Duve, UCL - SSS/DDUV/CELL - Biologie cellulaire, UCL - SSS/DDUV/GECE - Génétique cellulaire, UCL - SSS/IONS - Institute of NeuroScience, UCL - SSS/IONS/CEMO - Pôle Cellulaire et moléculaire, UCL - SSS/LDRI - Louvain Drug Research Institute, UCL - SST/LIBST - Louvain Institute of Biomolecular Science and Technology, Cloos, Anne-Sophie, Ghodsi, Marine, Stommen, Amaury, Vanderroost, Juliette, Dauguet, Nicolas, Pollet, Hélène, D'Auria, Ludovic, Mignolet, Eric, Larondelle, Yvan, Terrasi, Romano, Muccioli, Giulio, Van Der Smissen, Patrick, and Tyteca, Donatienne

Abstract

The shedding of extracellular vesicles (EVs) from the red blood cell (RBC) surface is observed during senescence and RBC storage . Two main models for EV shedding, respectively based on calcium rise and oxidative stress, have been proposed in the literature but the role of the plasma membrane lipid composition and properties is not understood. Using blood in K/EDTA tubes stored for up to 4 weeks at 4°C as a relevant RBC vesiculation model, we showed here that the RBC plasma membrane lipid composition, organization in domains and biophysical properties were progressively modified during storage and contributed to the RBC vesiculation. First, the membrane content in cholesterol and linoleic acid decreased whereas lipid peroxidation and spectrin:membrane occupancy increased, all compatible with higher membrane rigidity. Second, phosphatidylserine surface exposure showed a first rapid rise due to membrane cholesterol decrease, followed by a second calcium-dependent increase. Third, lipid domains mainly enriched in GM1 or sphingomyelin strongly increased from the 1st week while those mainly enriched in cholesterol or ceramide decreased during the 1st and 4th week, respectively. Fourth, the plasmatic acid sphingomyelinase activity considerably increased upon storage following the sphingomyelin-enriched domain rise and potentially inducing the loss of ceramide-enriched domains. Fifth, in support of the shedding of cholesterol- and ceramide-enriched domains from the RBC surface, the number of cholesterol-enriched domains lost and the abundance of EVs released during the 1st week perfectly matched. Moreover, RBC-derived EVs were enriched in ceramide at the 4th week but depleted in sphingomyelin. Then, using K/EDTA tubes supplemented with glucose to longer preserve the ATP content, we better defined the sequence of events. Altogether, we showed that EV shedding from lipid domains only represents part of the global vesiculation mechanistics, for which we propose four successiv

Published
2020

33. Cationic Nanoliposomes Are Efficiently Taken up by Alveolar Macrophages but Have Little Access to Dendritic Cells and Interstitial Macrophages in the Normal and CpG-Stimulated Lungs.

Author

UCL - SSS/DDUV - Institut de Duve, UCL - SSS/DDUV/CELL - Biologie cellulaire, UCL - SSS/DDUV/GECE - Génétique cellulaire, UCL - SSS/IREC/LTAP - Louvain Centre for Toxicology and Applied Pharmacology, UCL - SSS/LDRI - Louvain Drug Research Institute, Vanbever, Rita, Loira Pastoriza, Cristina, Dauguet, Nicolas, Hérin, Caroline, Ibouraadaten, Saloua, Vanvarenberg, Kevin, Ucakar, Bernard, Tyteca, Donatienne, Huaux, François, UCL - SSS/DDUV - Institut de Duve, UCL - SSS/DDUV/CELL - Biologie cellulaire, UCL - SSS/DDUV/GECE - Génétique cellulaire, UCL - SSS/IREC/LTAP - Louvain Centre for Toxicology and Applied Pharmacology, UCL - SSS/LDRI - Louvain Drug Research Institute, Vanbever, Rita, Loira Pastoriza, Cristina, Dauguet, Nicolas, Hérin, Caroline, Ibouraadaten, Saloua, Vanvarenberg, Kevin, Ucakar, Bernard, Tyteca, Donatienne, and Huaux, François

Abstract

The purpose of this study was to assess whether cationic nanoliposomes could address tumor vaccines to dendritic cells in the lungs in vivo. Nanoliposomes were prepared using a cationic lipid, dimethylaminoethanecarbamoyl-cholesterol (DC-cholesterol) or dioleoyltrimethylammoniumpropane (DOTAP), and dipalmitoylphosphatidylcholine (DPPC), the most abundant phospholipid in lung surfactant. The liposomes presented a size below 175 nm and they effectively entrapped tumor antigens, an oligodeoxynucletotide containing CpG motifs (CpG) and the fluorescent dye calcein used as a tracer. Although the liposomes could permanently entrap a large fraction of the actives, they could not sustain their release in vitro. Liposomes made of DOTAP were safe to respiratory cells in vitro, while liposomes composed of DC-cholesterol were cytotoxic. DOTAP nanoliposomes were mainly taken up by alveolar macrophages following delivery to the lungs in mice. Few dendritic cells took up the liposomes, and interstitial macrophages did not take up liposomal calcein more than they took up soluble calcein. Stimulation of the innate immune system using liposomal CpG strongly enhanced uptake of calcein liposomes by all phagocytes in the lungs. Although a small percentage of dendritic cells took up the nanoliposomes, alveolar macrophages represented a major barrier to dendritic cell access in the lungs.

Published
2019

34. MicroRNA-337-3p controls hepatobiliary gene expression and transcriptional dynamics during hepatic cell differentiation

Author

UCL - SSS/DDUV/LPAD - Liver and pancreas differentiation, Demarez, Céline, Gérard, Claude, Cordi, Sabine, Poncy, Alexis, Achouri, Younes, Dauguet, Nicolas, Rosa, David A., Gunning, Patrick T., Manfroid, Isabelle, Lemaigre, Frédéric, UCL - SSS/DDUV/LPAD - Liver and pancreas differentiation, Demarez, Céline, Gérard, Claude, Cordi, Sabine, Poncy, Alexis, Achouri, Younes, Dauguet, Nicolas, Rosa, David A., Gunning, Patrick T., Manfroid, Isabelle, and Lemaigre, Frédéric

Abstract

Transcriptional networks control the differentiation of the hepatocyte and cholangiocyte lineages from embryonic liver progenitor cells and their subsequent maturation to the adult phenotype. However, how relative levels of hepatocyte and cholangiocyte gene expression are determined during differentiation remains poorly understood. Here, we identify microRNA (miR)-337-3p as a regulator of liver development. miR-337-3p stimulates expression of cholangiocyte genes and represses hepatocyte genes in undifferentiated progenitor cells in vitro and in embryonic mouse livers. Beyond the stage of lineage segregation, miR-337-3p controls the transcriptional network dynamics of developing hepatocytes and balances both cholangiocyte populations that constitute the ductal plate. miR-337-3p requires Notch and transforming growth factor-b signaling and exerts a biphasic control on the hepatocyte transcription factor hepatocyte nuclear factor 4a by modulating its activation and repression. With the help of an experimentally validated mathematical model, we show that this biphasic control results from an incoherent feedforward loop between miR-337-3p and hepatocyte nuclear factor 4a. Conclusion: Our results identify miR- 337-3p as a regulator of liver development and highlight how tight quantitative control of hepatic cell differentiation is exerted through specific gene regulatory network motifs.

Published
2018

36. AhR modulates the IL-22-producing cell proliferation/recruitment in imiquimod-induced psoriasis mouse model

Author

Cochez, Perrine, Michiels, Camille, Hendrickx, Emilie, Van Belle, Astrid B, Lemaire, Muriel M, Dauguet, Nicolas, Warnier, Guy, de Heusch, Magali, Togbe, Dieudonnée, Ryffel, Bernhard, Coulie, Pierre, Renauld, Jean-Christophe, Dumoutier, Laure, and UCL - SSS/DDUV - Institut de Duve

Subjects
Mice, Knockout, Imiquimod, Chemotaxis, Interleukins, Receptors, Antigen, T-Cell, alpha-beta, Receptors, Antigen, T-Cell, gamma-delta, Immunity, Innate, Disease Models, Animal, Mice, Receptors, Aryl Hydrocarbon, T-Lymphocyte Subsets, Aminoquinolines, Animals, Psoriasis, Th17 Cells, Cell Proliferation
Abstract

IL-22 has a detrimental role in skin inflammatory processes, for example in psoriasis. As transcription factor, AhR controls the IL-22 production by several cell types (i.e. Th17 cells). Here, we analyzed the role of Ahr in IL-22 production by immune cells in the inflamed skin, using an imiquimod-induced psoriasis mouse model. Our results indicate that IL-22 is expressed in the ear of imiquimod-treated Ahr(-/-) mice but less than in wild-type mice. We then studied the role of AhR on three cell populations known to produce IL-22 in the skin: γδ T cells, Th17 cells, and ILC3, and a novel IL-22-producing cell type identified in this setting: CD4(-) CD8(-) TCRβ(+) T cells. We showed that AhR is required for IL-22 production by Th17, but not by the three other cell types, in the imiquimod-treated ears. Moreover, AhR has a role in the recruitment of γδ T cells, ILC3, and CD4(-) CD8(-) TCRβ(+) T cells into the inflamed skin or in their local proliferation. Taken together, AhR has a direct role in IL-22 production by Th17 cells in the mouse ear skin, but not by γδ T cells, CD4(-) CD8(-) TCRβ(+) T cells and ILCs.

Published
2015

37. Sex chromosomes and quantitative sex expression in monoecious hemp (Cannabis sativa L.)

Author

UCL - SST/ELI/ELIA - Agronomy, Faux, Anne-Michelle, Berhin, Alice, Dauguet, Nicolas, Bertin, Pierre, UCL - SST/ELI/ELIA - Agronomy, Faux, Anne-Michelle, Berhin, Alice, Dauguet, Nicolas, and Bertin, Pierre

Abstract

Hemp (Cannabis sativa) has a highly variable sexual phenotype. In dioecious hemp, the sex is controlled by heteromorphic sex chromosomes according to an X-to-autosomes equilibrium. However, in monoecious hemp, the sex determinism remains widely unknown and has never been related to a quantitative approach of sex expression. The present paper aims to contribute to the comprehension of the sex determinism in monoecious hemp by assessing the genotypic variability of its sex expression and establishing its sex chromosomes. Five monoecious and one dioecious cultivars were grown in controlled conditions under several photoperiods. The monoecy degree of 194 monoecious plants was recorded at each node by a figure ranging from 0 (male flowers only) to 6 (female flowers only). The genome size of 55 plants was determined by flow cytometry. The DNA of 115 monoecious plants was screened with the male-associated marker MADC2. The monoecy degree varied significantly among monoecious cultivars from 3.36 ± 2.28 in 'Uso 31' to 5.70 ± 0.81 in the most feminised 'Epsilon 68'. The variation of monoecy degree among cultivars remained consistent across trials despite a significant "cultivar × trial" interaction and partly agreed with their earliness. The genome size of monoecious plants (1.791 ± 0.017 pg) was not different from that of females (1.789 ± 0.019 pg) but significantly lower than that of males (1.835 ± 0.019 pg). MADC2 was absent from all monoecious plants. These results strongly support that cultivars of monoecious hemp have the XX constitution and that their sex expression has a genetic basis. © 2013 Springer Science+Business Media Dordrecht.

Published
2014

38. Let-7b and miR-495 Stimulate Differentiation and Prevent Metaplasia of Pancreatic Acinar Cells by Repressing HNF6

Author

UCL - SSS/DDUV - Institut de Duve, Prévot, Pierre-Paul, Augereau, Cécile, Simion, Alexandru, Van den Steen, Géraldine, Dauguet, Nicolas, Lemaigre, Frédéric, Jacquemin, Patrick, UCL - SSS/DDUV - Institut de Duve, Prévot, Pierre-Paul, Augereau, Cécile, Simion, Alexandru, Van den Steen, Géraldine, Dauguet, Nicolas, Lemaigre, Frédéric, and Jacquemin, Patrick

Abstract

BACKGROUND & AIMS: Diseases of the exocrine pancreas are often associated with perturbed differentiation of acinar cells. MicroRNAs (miRNAs) regulate pancreas development, yet little is known about their contribution to acinar cell differentiation. We aimed to identify miRNAs that promote and control the maintenance of acinar differentiation. METHODS: We studied mice with pancreas- or acinar-specific inactivation of Dicer (Foxa3-Cre/DicerloxP/- mice), combined (or not) with inactivation of Hepatocyte Nuclear Factor (HNF) 6 (Foxa3-Cre/Dicerloxp/-/Hnf6-/- mice). The role of specific miRNAs in acinar differentiation was investigated by transfecting cultured cells with miRNA mimics or inhibitors. Pancreatitis-induced metaplasia was investigated in mice following administration of cerulein. RESULTS: Inhibition of miRNA synthesis in acini by inactivation of Dicer, as well as pancreatitis-induced metaplasia, were associated with repression of acinar differentiation and with induction of HNF6 and hepatic genes. The phenotype of Dicer-deficient acini depends on the induction of HNF6; overexpression of this factor in developing acinar cells is sufficient to repress acinar differentiation and to induce hepatic genes. Let-7b and miR-495 repress HNF6 and are expressed in developing acini. Their expression is inhibited in Dicer-deficient acini, as well as in pancreatitis-induced metaplasia. Moreover, inhibiting let-7b and miR-495 in acinar cells results in similar effects to those found in Dicer-deficient acini and metaplastic cells, namely induction of HNF6 and hepatic genes and repression of acinar differentiation. CONCLUSIONS: Let-7b, miR-495, and their targets constitute a gene network that is required to establish and maintain pancreatic acinar cell differentiation. Further studies of this network will increase our understanding of pancreatic diseases.

Published
2013

39. Let-7b and miR-495 stimulate differentiation and prevent metaplasia of pancreatic acinar cells by repressing HNF6.

Author

Prévot, Pierre-Paul, Augereau, Cécile, Simion, Alexandru, Van Den Steen, Géraldine, Dauguet, Nicolas, Lemaigre, Frédéric P, Jacquemin, Patrick, Prévot, Pierre-Paul, Augereau, Cécile, Simion, Alexandru, Van Den Steen, Géraldine, Dauguet, Nicolas, Lemaigre, Frédéric P, and Jacquemin, Patrick

Abstract

Diseases of the exocrine pancreas are often associated with perturbed differentiation of acinar cells. MicroRNAs (miRNAs) regulate pancreas development, yet little is known about their contribution to acinar cell differentiation. We aimed to identify miRNAs that promote and control the maintenance of acinar differentiation., Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published
2013

40. Arsenic trioxide treatment decreases the oxygen consumption rate of tumor cells and radiosensitizes solid tumors

Author

UCL - SSS/LDRI - Louvain Drug Research Institute, UCL - SSS/IREC/FATH - Pôle de Pharmacologie et thérapeutique, UCL - SSS/IREC/MIRO - Pôle d'imagerie moléculaire, radiothérapie et oncologie, UCL - SSS/DDUV - Institut de Duve, UCL - SSS/IREC - Institut de recherche expérimentale et clinique, UCL - (SLuc) Service de radiothérapie oncologique, Diépart, Caroline, Karroum, Oussama, Magat, Julie, Feron, Olivier, Verrax, Julien, Buc Calderon, Pedro, Grégoire, Vincent, Levêque, Philippe, Stockis, Julie, Dauguet, Nicolas, Jordan, Bénédicte, Gallez, Bernard, UCL - SSS/LDRI - Louvain Drug Research Institute, UCL - SSS/IREC/FATH - Pôle de Pharmacologie et thérapeutique, UCL - SSS/IREC/MIRO - Pôle d'imagerie moléculaire, radiothérapie et oncologie, UCL - SSS/DDUV - Institut de Duve, UCL - SSS/IREC - Institut de recherche expérimentale et clinique, UCL - (SLuc) Service de radiothérapie oncologique, Diépart, Caroline, Karroum, Oussama, Magat, Julie, Feron, Olivier, Verrax, Julien, Buc Calderon, Pedro, Grégoire, Vincent, Levêque, Philippe, Stockis, Julie, Dauguet, Nicolas, Jordan, Bénédicte, and Gallez, Bernard

Abstract

Arsenic trioxide (As(2)O(3)) is an effective therapeutic against acute promyelocytic leukemia and certain solid tumors. Because As(2)O(3) inhibits mitochondrial respiration in leukemia cells, we hypothesized that As(2)O(3) might enhance the radiosensitivity of solid tumors by increasing tumor oxygenation [partial pressure of oxygen (pO(2))] via a decrease in oxygen consumption. Two murine models of radioresistant hypoxic cancer were used to study the effects of As(2)O(3). We measured pO(2) and the oxygen consumption rate in vivo by electron paramagnetic resonance oximetry and (19)fluorine-MRI relaxometry. Tumor perfusion was assessed by Patent blue staining. In both models, As(2)O(3) inhibited mitochondrial respiration, leading to a rapid increase in pO(2). The decrease in oxygen consumption could be explained by an observed decrease in glutathione in As(2)O(3)-treated cells, as this could increase intracellular reactive oxygen species that can disrupt mitochondrial membrane potential. When tumors were irradiated during periods of As(2)O(3)-induced augmented oxygenation, radiosensitivity increased by 2.2-fold compared with control mice. Notably, this effect was abolished when temporarily clamped tumors were irradiated. Together, our findings show that As(2)O(3) acutely increases oxygen consumption and radiosensitizes tumors, providing a new rationale for clinical investigations of As(2)O(3) in irradiation protocols to treat solid tumors. Cancer Res; 72(2); 482-90. ©2011 AACR.

Published
2012

41. Rôle immunomodulateur du lenalidomide sur les cellules Natural Killer humaines. Etude des effecteurs lymphoïdes cytotoxiques chez les patients atteints de leucémies aiguës myéloïdes en 1ère rémission complète

Author

Dauguet, Nicolas and Dauguet, Nicolas

Abstract

La plupart des patients atteints de leucémies aiguës myéloïdes (LAM) sont en rémission complète après la chimiothérapie d'induction (1ère RC). Or, la persistance de cellules cancéreuses résistantes aux traitements et à la réponse immunitaire engendre de nombreuses rechutes. Nos travaux montrent la prééminence et la persistance de cellules NK CD56bright immatures chez ces patients en 1ère RC. Ainsi, tout agent ou tout protocole favorisant la reconstitution ou potentialisant les fonctions cytotoxiques des cellules NK pourrait être bénéfique. Nous avons ainsi choisi d'évaluer le rôle du Lenalidomide sur les cellules NK de donneurs sains. Nos travaux montrent, pour la 1ère fois, un effet direct mais cependant complexe sur les cellules NK. En effet, le Lenalidomide augmente l'expression du CD56 mais diminue la production d'IFN-gamma deux effets qui s'opposent au regard de la description classique des cellules NK CD56bright. L'augmentation du CD56 ne présagerait pas d'un effet bénéfique sur les cellules NK des patients LAM en 1ère RC. De plus, la modulation de l'expression de divers récepteurs de lyse n'a pas d'impact sur les fonctions cytotoxiques de ces effecteurs. Cependant, la diminution de l'expression de l'IFN-gamma pourrait être bénéfique car ce dernier favorise l'expression des molécules du CMH-I par les cellules leucémiques de LAM et inhibant ainsi l'activité cytotoxique des cellules NK. Les nombreuses actions du Lenalidomide sur le microenvironnement tumoral encouragent à poursuivre l'étude de ces effets dans les LAM., Most Acute Myeloide Leukemia (AML) patients achieve complete remission after induction chemotherapy (1st CR). Nevertheless, persistence of resistant tumor cells to treatments and immune response is associated with high risk of relapse. Our works highlight a pre-eminence and persistence of immature CD56 bright NK cells in patients at 1st CR. Thus, every agent or protocol dedicated to improve reconstitution or to potentiate cytotoxic functions of NK cells would be beneficial. Thus, we have chosen to evaluate the role of Lenalidomide upon NK cells of healthy donors. Our works show, for the first time, a direct but complexe effect on NK cells. Indeed, Lenalidomide upregulates the CD56 expression but decreases IFN-gamma production, two opposite effects with respect to the classical description of CD56bright NK cell population. The upregulation of CD56 do not augur a beneficial effect on NK cells of AML patients in 1st CR. Moreover, the modulation of expression of various lytic receptors has no impact on NK cell cytotoxic functions. However, the decrease of IFN-gamma expression coulb be beneficial as it upregulates MHC-I expression on AML leukemic cells and inhibit NK cell cytotoxic activity. The wide range of Lenalidomide actions on tumoral microenvironment is a strong support to pursue the study of its effects on AML.

Published
2010

43. Arsenic Trioxide Treatment Decreases the Oxygen Consumption Rate of Tumor Cells and Radiosensitizes Solid Tumors

Author

Diepart, Caroline, primary, Karroum, Oussama, additional, Magat, Julie, additional, Feron, Olivier, additional, Verrax, Julien, additional, Calderon, Pedro Buc, additional, Grégoire, Vincent, additional, Leveque, Philippe, additional, Stockis, Julie, additional, Dauguet, Nicolas, additional, Jordan, Bénédicte F., additional, and Gallez, Bernard, additional

Published
2012
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