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4. Blocking immunosuppression by human Tregs in vivo with antibodies targeting integrin αVβ8

Author

Stockis, Julie, Liénart, Stéphanie, Colau, Didier, Collignon, Amandine, Nishimura, Stephen L, Sheppard, Dean, Coulie, Pierre G, and Lucas, Sophie

Subjects
Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Immunology, Immunotherapy, Biotechnology, 2.1 Biological and endogenous factors, Animals, Antibodies, Monoclonal, Cells, Cultured, Disease Models, Animal, Graft vs Host Disease, Humans, Immune Tolerance, Integrins, Membrane Proteins, Mice, Mice, SCID, Neoplasms, T-Lymphocytes, Regulatory, Transforming Growth Factor beta1, Transplantation, Heterologous, GARP, integrin alpha V beta 8, human regulatory T cells, TGF-beta, cancer immunotherapy, TGF-β, integrin αVβ8
Abstract

Human regulatory T cells (Tregs) suppress other T cells by converting the latent, inactive form of TGF-β1 into active TGF-β1. In Tregs, TGF-β1 activation requires GARP, a transmembrane protein that binds and presents latent TGF-β1 on the surface of Tregs stimulated through their T cell receptor. However, GARP is not sufficient because transduction of GARP in non-Treg T cells does not induce active TGF-β1 production. RGD-binding integrins were shown to activate TGF-β1 in several non-T cell types. Here we show that αVβ8 dimers are present on stimulated human Tregs but not in other T cells, and that antibodies against αV or β8 subunits block TGF-β1 activation in vitro. We also show that αV and β8 interact with GARP/latent TGF-β1 complexes in human Tregs. Finally, a blocking antibody against β8 inhibited immunosuppression by human Tregs in a model of xenogeneic graft-vs.-host disease induced by the transfer of human T cells in immunodeficient mice. These results show that TGF-β1 activation on the surface of human Tregs implies an interaction between the integrin αVβ8 and GARP/latent TGF-β1 complexes. Immunosuppression by human Tregs can be inhibited by antibodies against GARP or against the integrin β8 subunit. Such antibodies may prove beneficial against cancer or chronic infections.

Published
2017

5. Quantitative methods in immuno-oncology: deconvolution tool, anti-PD1 therapy, model of chronic myeloid leukemia

Author

Lenaerts, Tom, Leo, Oberdan, Loris, Ignace, Flot, Jean-François, Lucas, Sophie, Dendievel, Sarah, Vande Velde, Sylvie, Lenaerts, Tom, Leo, Oberdan, Loris, Ignace, Flot, Jean-François, Lucas, Sophie, Dendievel, Sarah, and Vande Velde, Sylvie

Abstract

During my PhD thesis, I mainly worked on three projects involving mathematical and bioinformatics methods in immuno-oncology. 1) Project 1: development of the SmartFACS deconvolution tool. I developed a deconvolution tool called SmartFACS in collaboration with the Mechanics and Applied Mathematics Department (ULB) and the Immunobiology Laboratory (ULB). The role of this computer program is to estimate the cellular composition of a sample from RNA sequencing data. This tool has been developed in the context of immunology, where it is often of interest to identify immune cells present in the blood or in tumors. At the time this project began, no deconvolution tool for mouse data was yet available, despite the fact that much biomedical research is carried out in mouse models. During my thesis, I therefore decided to develop a tool adapted to mouse data, while trying to improve existing tools for human data by detecting a wider range of immune populations. 2) Project 2: research of clinical biomarkers for anti-PD1 immunotherapy treatment. In collaboration with the Immunobiology group (ULB), I worked on anti-PD1 therapy, which is already used clinically for certain cancers. Unfortunately, the success rate of this treatment is still relatively moderate. This is why the aim of my project was to determine predictive markers of response to anti-PD1 in order to better understand the mechanisms of resistance and find avenues of improvement for this treatment, as well as to better identify responder patients. To achieve these objectives, a mouse model was developed in the Immunobiology Laboratory. This model enabled us to reproduce the dichotomous response observed in the clinic. My work focused on analyzing pre-treatment tumor sequencing data obtained using the mouse model, in order to compare the immune infiltrate of responder and non-responder mice. My data analyses, together with experiments conducted by Jelena Gabrilo, revealed two immune populations important for treatmen, Doctorat en Sciences, info:eu-repo/semantics/nonPublished

Published
2024

7. Diagnosing borderline personality disorder: Reports and recommendations from people with lived experience.

Author

Tedesco, Vanessa, Day, Nicholas John Stephen, Lucas, Sophie, and Grenyer, Brin F. S.

Subjects
TREATMENT of borderline personality disorder, RESEARCH funding, QUALITATIVE research, INTERVIEWING, STATISTICAL sampling, QUESTIONNAIRES, CLASSIFICATION of mental disorders, SEVERITY of illness index, DESCRIPTIVE statistics, BORDERLINE personality disorder, THEMATIC analysis, AGE factors in disease, RESEARCH methodology, DELAYED diagnosis, DATA analysis software, SOCIAL support, EARLY diagnosis, PATIENTS' attitudes, SOCIAL stigma, PSYCHOSOCIAL factors
Abstract

Borderline personality disorder (BPD) is a severe mental health condition marked by impairments in self and interpersonal functioning. Stigma from health staff may often result in a reluctance to diagnose, impacting recovery trajectories. Qualitative interviews were conducted with participants (N = 15; M Age = 36.4 years, SD = 7.5; 93.3% female) with lived experience of BPD exploring topics of illness onset, insight, experience of diagnosis and treatment. Qualitative responses were analysed within a co‐design framework with a member of the research team who identifies as having a lived experience of BPD. On average, participant symptoms emerged at 12.1 years of age (SD = 6.6 years, range 1.5–27), but diagnoses of BPD were delayed until 30.2 years (SD = 7.8 years, range 18–44) resulting in a 'diagnosis gap' of 18.1 years (SD = 9.6 years, range 3–30). Participant explanations for BPD emergence varied from biological, psychological and social factors. Benefits of diagnosis (e.g., fostering insight, aiding treatment planning and reducing isolation) were contrasted with challenges (e.g., stigma and treatment unavailability). Delay in diagnosis was common, and no participants reported receiving a diagnosis of BPD during their adolescence yet 85% felt they would have benefited from a diagnosis in adolescence. Only a quarter (27%) felt highly supported in the diagnostic process. An ideal four‐step diagnosis procedure was outlined based on recommendations from participants with a lived experience; this involved the following: (1) explain the process, (2) assess thoroughly, (3) explore how the features are active in everyday life and (4) link diagnosis to evidence‐based treatment planning. [ABSTRACT FROM AUTHOR]

Published
2024
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9. p16Ink4a, a marker of cellular senescence, is associated with renal disease in the B6.NZMSle1/Sle2/Sle3mouse model of lupus

Author

Tilman, Gaëlle, primary, Dupré, Emilie, additional, Watteyne, Laura, additional, Baert, Charlotte Anne, additional, Nolf, Delphine, additional, Benhaddi, Fatima, additional, Lambert, Fanny, additional, Daumerie, Aurélie, additional, Bouzin, Caroline, additional, Lucas, Sophie, additional, and Limaye, Nisha, additional

Published
2023
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11. Behaviour of endocrine disrupting chemicals and nitrate in the environment

Author

Lucas, Sophie and Jones, David

Subjects
577.27
Abstract

The work in this thesis is divided into two discrete sections: the first describes the behaviour of estrogenic pollutants in soil, whilst the second describes the development of a nitrate and turbidity sonde for use in monitoring pollutants in groundwater boreholes. Endocrine disrupting chemicals are of increasing concern due to their effects on aquatic organisms especially the feminisation of male fish. Some of the chemicals of concern are naturally occurring steroid hormones such as estrogens (reviewed in Chapter 2). Investigations into the biodegradation of the estrogens: estrone and 17 β-estradiol (published in the journal Soil Biology and Biochemistry; Chapter 3) were undertaken, alongside investigations into the sorption of the estrogens to soil (Chapters 3 and 4) and their ability to be leached through the soil profile during rainfall events (Chapter 4).Throughout these investigations ¹⁴C-labelled estrogens was applied to different soils in various animal wastes. It was concluded that the estrogens were mineralised rapidly in soil and they behave differently when applied to soil in urine rather than water, which has implications for future work. Groundwater is an important resource for water supplies in the UK. The most common pollutant is nitrate, as reviewed in Chapter 5. UV spectrophotometry was investigated in the laboratory to develop a standard nitrate analysis method (Chapter 6). A major interference in nitrate measurement with UV in natural waters is dissolved organic carbon (DOC), which has an absorbance in the same range as nitrate (Chapter 7). Following laboratory development and calibration with humic acids to overcome the complications arising from DOC a field sonde was developed using UV spectrophotometry (Chapters 8 & 9). A separate sonde was developed to evaluate turbidity in natural waters. Chapter 10 shows the laboratory and field tests involved with the turbidity sonde, the work that goes into developing a new product and the results obtained. There are many further experiments that could be developed from the work in this thesis. In the estrogen section experiments need to be carried out with intact soil cores and in the field with conditions that cannot be achieved in a laboratory. To put the work into a more global context different animals, agricultural practices, climate and geography would need to be considered. In the nitrate section future work includes the continued testing of the nitrate and turbidity sondes. There is also the possibility of developing a DOC sonde and the potential of phosphorus measurement could be explored.

Published
2008

14. Selective inhibition of TGF-β1 produced by GARP-expressing Tregs overcomes resistance to PD-1/PD-L1 blockade in cancer

Author

de Streel, Grégoire, Bertrand, Charlotte, Chalon, Nicolas, Liénart, Stéphanie, Bricard, Orian, Lecomte, Sara, Devreux, Julien, Gaignage, Mélanie, De Boeck, Gitte, Mariën, Lore, Van De Walle, Inge, van der Woning, Bas, Saunders, Michael, de Haard, Hans, Vermeersch, Elien, Maes, Wim, Deckmyn, Hans, Coulie, Pierre G., van Baren, Nicolas, and Lucas, Sophie

Published
2020
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15. Functional Th1-oriented T follicular helper cells that infiltrate human breast cancer promote effective adaptive immunity

Author

Noel, Gregory, Fontsa, Mireille Langouo, Garaud, Soizic, De Silva, Pushpamali, de Wind, Alexandre, Van den Eynden, Gert G., Salgado, Roberto, Boisson, Anais, Locy, Hanne, Thomas, Noemie, Solinas, Cinzia, Migliori, Edoardo, Naveaux, Celine, Duvillier, Hugues, Lucas, Sophie, Craciun, Ligia, Thielemans, Kris, Larsimont, Denis, and Willard-Gallo, Karen

Subjects
Immune system -- Health aspects, Tumor-infiltrating lymphocytes -- Physiological aspects -- Health aspects, CD4 lymphocytes -- Physiological aspects -- Health aspects, Breast cancer -- Care and treatment, Health care industry
Abstract

We previously demonstrated that tumor-infiltrating lymphocytes (TIL) in human breast cancer sometimes form organized tertiary lymphoid structures (TLS) characterized by CXCL13-producing T follicular helper (Tfh) cells. The present study found that [CD4.sup.+] Tfh TIL, [CD8.sup.+] TIL, and TIL-B, colocalizing in TLS, all express the CXCL13 receptor CXCR5. An ex vivo functional assay determined that only activated, functional Thl-oriented Tfh TIL ([PD-1.sup.hi][ICOS.sup.int] phenotype) provide help for immunoglobulin and IFN-[gamma] production. A functional Tfh TIL presence signals an active TLS, characterized by humoral (immunoglobulins, [Ki-67.sup.+] TIL-B in active germinal centers) and cytotoxic ([GZMB.sup.+][CD8.sup.+] and [GZMB.sup.+][CD68.sup.+] TIL plus Th1 gene expression) immune responses. Analysis of active versus inactive TLS in untreated patients revealed that the former are associated with positive clinical outcomes. TLS also contain functional T follicular regulatory (Tfr) TIL, which are characterized by a [CD25.sup.+][CXCR5.sup.+][GARP.sup.+][FOXP3.sup.+] phenotype and a demethylated FOXP3 gene. Functional Tfr inhibited functional Tfh activities via a glycoprotein A repetitions predominant (GARP)-associated TGF-[beta]-dependent mechanism. The activity of tumor-associated TLS was dictated by the relative balance between functional Tfh TIL and functional Tfr TIL. These data provide mechanistic insight into TLS processes orchestrated by functional Th1-oriented Tfh TIL, including TIL-B and [CD8.sup.+] TIL activation and immunological memory generation. Tfh TIL, regulated by functional Tfr TIL, are an expected key target of PD-1/PD-L1 blockade., Introduction Adaptive and innate antitumor immune responses and their exploitation in immunotherapy are recognized as key defenses in the fight against cancer. Across a diversity of tumor types, data support [...]

Published
2021
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17. Caractérisation des effets anti tumoraux de la chémérine dans des modèles de mélanome chez le poisson-zèbre

Author

Wittamer, Valérie, Parmentier, Marc, Lybaert, Pascale, Braun, Michel Y, Patushenko, Ievgeniia, Stamatopoulos, Basile, Levraud, Jean-Pierre, Lucas, Sophie, Pozo Gomez, Jennifer, Wittamer, Valérie, Parmentier, Marc, Lybaert, Pascale, Braun, Michel Y, Patushenko, Ievgeniia, Stamatopoulos, Basile, Levraud, Jean-Pierre, Lucas, Sophie, and Pozo Gomez, Jennifer

Abstract

Le mélanome est la forme la plus agressive et la plus mortelle des cancers de la peau. Une mutation activatrice dans les gènes BRAF ou NRAS est présente dans 95% des cas de mélanomes humains. L'importance de l'inflammation chronique et du microenvironnement tumoral dans le développement, la progression et le potentiel métastatique de cette maladie est bien établie. Les molécules chimioattractantes comme la chémérine jouent dans ce contexte un rôle clé via le recrutement sélectif de populations leucocytaires spécifiques exprimant le récepteur ChemR23. Lors de ma thèse, nous avons étudié le rôle de la chémérine, dans les différentes étapes de la carcinogenèse. Elle possède des propriétés antitumorales, et notamment dans le mélanome. Cependant, les mécanismes de base de son action in vivo restent à déterminer.Suite aux études sur le modèle murin, nous avons choisi d’utiliser le poisson-zèbre afin d’investiguer in vivo les fonctions de la chémérine dans la biologie du mélanome. En effet, les résultats chez le poisson-zèbre obtenus au sein de notre laboratoire, suggèrent que l'axe chémérine/ChemR23 est hautement conservé à travers le phylum des vertébrés. Pour évaluer les propriétés antitumorales de la chémérine, j’ai utilisé différentes stratégies préalablement établies et validées chez le poisson-zèbre :un modèle mosaïque utilisant le système MiniCoopR exprimant l'oncogène NRASQ61L, un modèle génétique stable de mélanome faisant intervenir l’oncogène BRAF sur fond d’absence d’une protéine p53 fonctionnelle, et un modèle de xénogreffe de tumeurs. Mes analyses comparant l’apparition et la progression tumorale entre des animaux invalidés pour le cluster b de la chémérine ou pour son récepteur cmklr1.1 et leurs contrôles WT démontrent de manière non ambigüe que les propriétés antitumorales du système chémérine/ChemR23 sont conservées chez le poisson-zèbre.En ouvrant la voie à l’utilisation du poisson-zèbre pour l’étude des mécanismes clés par lesquels la chémérine agit sur, Doctorat en Sciences biomédicales et pharmaceutiques (Médecine), info:eu-repo/semantics/nonPublished

Published
2023

18. Spatial Distribution of Non-Immune Cells Expressing Glycoprotein A Repetitions Predominant in Human and Murine Metastatic Lymph Nodes.

Author

Rouaud, Loïc, Baudin, Louis, Gautier-Isola, Marine, Van Meerbeeck, Pierre, Feyereisen, Emilie, Blacher, Silvia, van Baren, Nicolas, Kridelka, Frédéric, Lucas, Sophie, and Noel, Agnes

Subjects
IN vitro studies, FLOW cytometry, SEQUENCE analysis, CELL culture, ANIMAL experimentation, WESTERN immunoblotting, FLUOROIMMUNOASSAY, ONE-way analysis of variance, LYMPH nodes, METASTASIS, MANN Whitney U Test, MEMBRANE glycoproteins, GENE expression, MESSENGER RNA, RESEARCH funding, T cells, CELL lines, DATA analysis software, MICE
Abstract

Simple Summary: Glycoprotein A repetitions predominant (GARP) is expressed at the surface of regulatory T lymphocytes (Tregs) in human and murine primary tumors and was shown to mediate TGF-β1 activation and immunosuppression by Tregs in tumor-bearing mice. The cellular sources and the implication of GARP in lymph nodes (LNs) during the metastatic cascade are still elusive. Here, we mined available scRNA-Seq datasets and conducted immunohistochemistry and in situ hybridization analyses of metastatic LNs from mice and patients with cervical or breast cancer. We found GARP expression not only in Tregs, but also in blood/lymphatic vessels, fibroblastic cells, and perivascular cells. Our study highlights for the first time GARP expression by specialized lymphatic endothelial cells in the subcapsular sinus, high endothelial venules (HEVs), and matrix-associated (fibroblastic/perivascular) cells. Several types of cancer spread through the lymphatic system via the sentinel lymph nodes (LNs). Such LN-draining primary tumors, modified by tumor factors, lead to the formation of a metastatic niche associated with an increased number of Foxp3+ regulatory T cells (Tregs). These cells are expected to contribute to the elaboration of an immune-suppressive environment. Activated Tregs express glycoprotein A repetitions predominant (GARP), which binds and presents latent transforming growth factor beta 1 (TGF-β1) at their surface. GARP is also expressed by other non-immune cell types poorly described in LNs. Here, we mapped GARP expression in non-immune cells in human and mouse metastatic LNs. The mining of available (human and murine) scRNA-Seq datasets revealed GARP expression by blood (BEC)/lymphatic (LEC) endothelial, fibroblastic, and perivascular cells. Consistently, through immunostaining and in situ RNA hybridization approaches, GARP was detected in and around blood and lymphatic vessels, in (αSMA+) fibroblasts, and in perivascular cells associated with an abundant matrix. Strikingly, GARP was detected in LECs forming the subcapsular sinus and high endothelial venules (HEVs), two vascular structures localized at the interface between LNs and the afferent lymphatic and blood vessels. Altogether, we here provide the first distribution maps for GARP in human and murine LNs. [ABSTRACT FROM AUTHOR]

Published
2023
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19. Supplementary Table 1 from Route of Administration Modulates the Induction of Dendritic Cell Vaccine–Induced Antigen-Specific T Cells in Advanced Melanoma Patients

Author

Lesterhuis, W. Joost, primary, de Vries, I. Jolanda M., primary, Schreibelt, Gerty, primary, Lambeck, Annechien J.A., primary, Aarntzen, Erik H.J.G., primary, Jacobs, Joannes F.M., primary, Scharenborg, Nicole M., primary, van de Rakt, Mandy W.M.M., primary, de Boer, Annemiek J., primary, Croockewit, Sandra, primary, van Rossum, Michelle M., primary, Mus, Roel, primary, Oyen, Wim J.G., primary, Boerman, Otto C., primary, Lucas, Sophie, primary, Adema, Gosse J., primary, Punt, Cornelis J.A., primary, and Figdor, Carl G., primary

Published
2023
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20. Supplementary Data from Frequency of Circulating Tregs with Demethylated FOXP3 Intron 1 in Melanoma Patients Receiving Tumor Vaccines and Potentially Treg-Depleting Agents

Author

de Vries, I. Jolanda M., primary, Castelli, Chiara, primary, Huygens, Caroline, primary, Jacobs, Joannes F.M., primary, Stockis, Julie, primary, Schuler-Thurner, Beatrice, primary, Adema, Gosse J., primary, Punt, Cornelis J.A., primary, Rivoltini, Licia, primary, Schuler, Gerold, primary, Coulie, Pierre G., primary, and Lucas, Sophie, primary

Published
2023
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21. Supplementary Figure 2 from Route of Administration Modulates the Induction of Dendritic Cell Vaccine–Induced Antigen-Specific T Cells in Advanced Melanoma Patients

Author

Lesterhuis, W. Joost, primary, de Vries, I. Jolanda M., primary, Schreibelt, Gerty, primary, Lambeck, Annechien J.A., primary, Aarntzen, Erik H.J.G., primary, Jacobs, Joannes F.M., primary, Scharenborg, Nicole M., primary, van de Rakt, Mandy W.M.M., primary, de Boer, Annemiek J., primary, Croockewit, Sandra, primary, van Rossum, Michelle M., primary, Mus, Roel, primary, Oyen, Wim J.G., primary, Boerman, Otto C., primary, Lucas, Sophie, primary, Adema, Gosse J., primary, Punt, Cornelis J.A., primary, and Figdor, Carl G., primary

Published
2023
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22. Supplementary Figure 1 from Route of Administration Modulates the Induction of Dendritic Cell Vaccine–Induced Antigen-Specific T Cells in Advanced Melanoma Patients

Author

Lesterhuis, W. Joost, primary, de Vries, I. Jolanda M., primary, Schreibelt, Gerty, primary, Lambeck, Annechien J.A., primary, Aarntzen, Erik H.J.G., primary, Jacobs, Joannes F.M., primary, Scharenborg, Nicole M., primary, van de Rakt, Mandy W.M.M., primary, de Boer, Annemiek J., primary, Croockewit, Sandra, primary, van Rossum, Michelle M., primary, Mus, Roel, primary, Oyen, Wim J.G., primary, Boerman, Otto C., primary, Lucas, Sophie, primary, Adema, Gosse J., primary, Punt, Cornelis J.A., primary, and Figdor, Carl G., primary

Published
2023
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30. Supplementary Figure Legends 1-6 from The CD4+ T-Cell Response of Melanoma Patients to a MAGE-A3 Peptide Vaccine Involves Potential Regulatory T Cells

Author

François, Violaine, primary, Ottaviani, Sabrina, primary, Renkvist, Nicolina, primary, Stockis, Julie, primary, Schuler, Gerold, primary, Thielemans, Kris, primary, Colau, Didier, primary, Marchand, Marie, primary, Boon, Thierry, primary, Lucas, Sophie, primary, and van der Bruggen, Pierre, primary

Published
2023
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35. 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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36. The importance of naturally attenuated SARS-CoV-2in the fight against COVID-19

Author

Armengaud, Jean [0000-0003-1589-445X], Thuret, Jean-Yves [0000-0001-5385-7620], Anken, Eelco van [0000-0001-9529-2701], Acosta-Alvear, Diego [0000-0002-1139-8486], Aragón, Tomás [0000-0002-1700-2729], Arias, Carolina [0000-0002-4445-0826], Blondel, Marc [0000-0003-4897-2995], Braakman, Ineke [0000-0003-1592-4364], Collet, Jean-François [0000-0001-8069-7036], Courcol, René [0000-0003-2324-5687], Danchin, Antoine [0000-0002-6350-5001], Deleuze, Jean-François [0000-0002-5358-4463], Lavigne, Jean-Philippe [0000-0002-9484-0304], Lucas, Sophie [0000-0003-1287-7996], Michiels, Thomas [0000-0001-9615-8053], Moore, Edward R.B. [0000-0001-7693-924X], Nixon-Abell, Jonathon [0000-0003-4169-0012], Rosselló-Mora, Ramón [0000-0001-8253-3107], Shi, Zheng-Li [0000-0001-8089-163X], Siccardi, Antonio G. [0000-0002-1654-5545], Sitia, Roberto [0000-0001-7086-4152], Tillett, Daniel [0000-0003-1061-0489], Timmis, Kenneth N. [0000-0002-0066-4670], Toledano, Michel B. [0000-0002-3079-1179], Sluijs, Peter van der [0000-0002-4485-3342], Vicenzi, Elisa [0000-0003-0051-3968], Armengaud, Jean, Delaunay, Agnes, Thuret, Jean-Yves, Anken, Eelco van, Acosta-Alvear, Diego, Aragón, Tomás, Arias, Carolina, Blondel, Marc, Braakman, Ineke, Collet, Jean-François, Courcol, René, Danchin, Antoine, Deleuze, Jean-François, Lavigne, Jean-Philippe, Lucas, Sophie, Michiels, Thomas, Moore, Edward R.B., Nixon-Abell, Jonathon, Rosselló-Mora, Ramón, Shi, Zheng-Li, Siccardi, Antonio G., Sitia, Roberto, Tillett, Daniel, Timmis, Kenneth N., Toledano, Michel B., Sluijs, Peter van der, Vicenzi, Elisa, Armengaud, Jean [0000-0003-1589-445X], Thuret, Jean-Yves [0000-0001-5385-7620], Anken, Eelco van [0000-0001-9529-2701], Acosta-Alvear, Diego [0000-0002-1139-8486], Aragón, Tomás [0000-0002-1700-2729], Arias, Carolina [0000-0002-4445-0826], Blondel, Marc [0000-0003-4897-2995], Braakman, Ineke [0000-0003-1592-4364], Collet, Jean-François [0000-0001-8069-7036], Courcol, René [0000-0003-2324-5687], Danchin, Antoine [0000-0002-6350-5001], Deleuze, Jean-François [0000-0002-5358-4463], Lavigne, Jean-Philippe [0000-0002-9484-0304], Lucas, Sophie [0000-0003-1287-7996], Michiels, Thomas [0000-0001-9615-8053], Moore, Edward R.B. [0000-0001-7693-924X], Nixon-Abell, Jonathon [0000-0003-4169-0012], Rosselló-Mora, Ramón [0000-0001-8253-3107], Shi, Zheng-Li [0000-0001-8089-163X], Siccardi, Antonio G. [0000-0002-1654-5545], Sitia, Roberto [0000-0001-7086-4152], Tillett, Daniel [0000-0003-1061-0489], Timmis, Kenneth N. [0000-0002-0066-4670], Toledano, Michel B. [0000-0002-3079-1179], Sluijs, Peter van der [0000-0002-4485-3342], Vicenzi, Elisa [0000-0003-0051-3968], Armengaud, Jean, Delaunay, Agnes, Thuret, Jean-Yves, Anken, Eelco van, Acosta-Alvear, Diego, Aragón, Tomás, Arias, Carolina, Blondel, Marc, Braakman, Ineke, Collet, Jean-François, Courcol, René, Danchin, Antoine, Deleuze, Jean-François, Lavigne, Jean-Philippe, Lucas, Sophie, Michiels, Thomas, Moore, Edward R.B., Nixon-Abell, Jonathon, Rosselló-Mora, Ramón, Shi, Zheng-Li, Siccardi, Antonio G., Sitia, Roberto, Tillett, Daniel, Timmis, Kenneth N., Toledano, Michel B., Sluijs, Peter van der, and Vicenzi, Elisa

Abstract

The current SARS‐CoV‐2 pandemic is wreaking havoc throughout the world and has rapidly become a global health emergency. A central question concerning COVID‐19 is why some individuals become sick and others not. Many have pointed already at variation in risk factors between individuals. However, the variable outcome of SARS‐CoV‐2 infections may, at least in part, be due also to differences between the viral subspecies with which individuals are infected. A more pertinent question is how we are to overcome the current pandemic. A vaccine against SARS‐CoV‐2 would offer significant relief, although vaccine developers have warned that design, testing and production of vaccines may take a year if not longer. Vaccines are based on a handful of different designs (i), but the earliest vaccines were based on the live, attenuated virus. As has been the case for other viruses during earlier pandemics, SARS‐CoV‐2 will mutate and may naturally attenuate over time (ii). What makes the current pandemic unique is that, thanks to state‐of‐the‐art nucleic acid sequencing technologies, we can follow in detail how SARS‐CoV‐2 evolves while it spreads. We argue that knowledge of naturally emerging attenuated SARS‐CoV‐2 variants across the globe should be of key interest in our fight against the pandemic.

Published
2020

37. The importance of naturally attenuated SARS‐CoV ‐2 in the fight against COVID ‐19

Author

Armengaud, Jean, Delaunay‐Moisan, Agnès, Thuret, Jean‐Yves, Anken, Eelco, Acosta‐Alvear, Diego, Aragón, Tomás, Arias, Carolina, Blondel, Marc, Braakman, Ineke, Collet, Jean‐François, Courcol, René, Danchin, Antoine, Deleuze, Jean‐François, Lavigne, Jean‐Philippe, Lucas, Sophie, Michiels, Thomas, Moore, Edward R. B., Nixon‐Abell, Jonathon, Rossello‐Mora, Ramon, Shi, Zheng‐Li, Siccardi, Antonio G., Sitia, Roberto, Tillett, Daniel, Timmis, Kenneth N., Toledano, Michel B., Sluijs, Peter, Vicenzi, Elisa, Médicaments et Technologies pour la Santé (MTS), Université Paris-Saclay-Direction de Recherche Fondamentale (CEA) (DRF (CEA)), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Institut National de Recherche pour l’Agriculture, l’Alimentation et l’Environnement (INRAE), Institut de Biologie Intégrative de la Cellule (I2BC), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Paris-Saclay-Centre National de la Recherche Scientifique (CNRS), Stress Oxydatif et Cancer (SOC), Département Biologie Cellulaire (BioCell), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Paris-Saclay-Centre National de la Recherche Scientifique (CNRS)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Paris-Saclay-Centre National de la Recherche Scientifique (CNRS)-Institut de Biologie Intégrative de la Cellule (I2BC), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Paris-Saclay-Centre National de la Recherche Scientifique (CNRS)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Université Paris-Saclay-Centre National de la Recherche Scientifique (CNRS), Sénescence et stabilité génomique (SEN), Département Biologie des Génomes (DBG), San Raffaele Scientific Institute, Vita-Salute San Raffaele University and Center for Translational Genomics and Bioinformatics, University of California [Santa Barbara] (UC Santa Barbara), University of California (UC), Universidad Pública de Navarra [Espagne] = Public University of Navarra (UPNA), Génétique, génomique fonctionnelle et biotechnologies (UMR 1078) (GGB), EFS-Université de Brest (UBO)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Institut Brestois Santé Agro Matière (IBSAM), Université de Brest (UBO), Université de Bretagne Occidentale - UFR Médecine et Sciences de la Santé (UBO UFR MSS), Utrecht University [Utrecht], Université Catholique de Louvain = Catholic University of Louvain (UCL), Walloon Excellence in Life sciences and BIOtechnology [Liège] (WELBIO), Institut Cochin (IC UM3 (UMR 8104 / U1016)), Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Université Paris Cité (UPCité), Centre National de Recherche en Génomique Humaine (CNRGH), Commissariat à l'énergie atomique et aux énergies alternatives (CEA), Institut de Biologie François JACOB (JACOB), Direction de Recherche Fondamentale (CEA) (DRF (CEA)), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA), Virulence bactérienne et maladies infectieuses (VBMI), Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Montpellier (UM), University of Gothenburg (GU), Sahlgrenska University Hospital [Gothenburg], University of Cambridge [UK] (CAM), Institut Mediterrani d'Estudis Avancats (IMEDEA), Consejo Superior de Investigaciones Científicas [Madrid] (CSIC)-Universidad de las Islas Baleares (UIB), Wuhan Institute of Virology [Wuhan, China], Chinese Academy of Sciences [Wuhan Branch], Technische Universität Braunschweig = Technical University of Braunschweig [Braunschweig], ANR-17-CE18-0023,Phylopeptidomics,Identification rapide de bactéries pathogènes et résistances aux antibiotiques(2017), Armengaud, Jean [0000-0003-1589-445X], Thuret, Jean-Yves [0000-0001-5385-7620], Anken, Eelco van [0000-0001-9529-2701], Acosta-Alvear, Diego [0000-0002-1139-8486], Aragón, Tomás [0000-0002-1700-2729], Arias, Carolina [0000-0002-4445-0826], Blondel, Marc [0000-0003-4897-2995], Braakman, Ineke [0000-0003-1592-4364], Collet, Jean-François [0000-0001-8069-7036], Courcol, René [0000-0003-2324-5687], Danchin, Antoine [0000-0002-6350-5001], Deleuze, Jean-François [0000-0002-5358-4463], Lavigne, Jean-Philippe [0000-0002-9484-0304], Lucas, Sophie [0000-0003-1287-7996], Michiels, Thomas [0000-0001-9615-8053], Moore, Edward R.B. [0000-0001-7693-924X], Nixon-Abell, Jonathon [0000-0003-4169-0012], Rosselló-Mora, Ramón [0000-0001-8253-3107], Shi, Zheng-Li [0000-0001-8089-163X], Siccardi, Antonio G. [0000-0002-1654-5545], Sitia, Roberto [0000-0001-7086-4152], Tillett, Daniel [0000-0003-1061-0489], Timmis, Kenneth N. [0000-0002-0066-4670], Toledano, Michel B. [0000-0002-3079-1179], Sluijs, Peter van der [0000-0002-4485-3342], Vicenzi, Elisa [0000-0003-0051-3968], University of California [Santa Barbara] (UCSB), University of California, Institut Brestois Santé Agro Matière (IBSAM), Université de Brest (UBO)-Université de Brest (UBO)-EFS-Institut National de la Santé et de la Recherche Médicale (INSERM), Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Université de Paris (UP), Technical University Braunschweig, Armengaud, Jean, Thuret, Jean-Yves, Anken, Eelco van, Acosta-Alvear, Diego, Aragón, Tomás, Arias, Carolina, Blondel, Marc, Braakman, Ineke, Collet, Jean-François, Courcol, René, Danchin, Antoine, Deleuze, Jean-François, Lavigne, Jean-Philippe, Lucas, Sophie, Michiels, Thomas, Moore, Edward R.B., Nixon-Abell, Jonathon, Rosselló-Mora, Ramón, Shi, Zheng-Li, Siccardi, Antonio G., Sitia, Roberto, Tillett, Daniel, Timmis, Kenneth N., Toledano, Michel B., Sluijs, Peter van der, Vicenzi, Elisa, Armengaud, J., Delaunay-Moisan, A., Thuret, J. -Y., van Anken, E., Acosta-Alvear, D., Aragon, T., Arias, C., Blondel, M., Braakman, I., Collet, J. -F., Courcol, R., Danchin, A., Deleuze, J. -F., Lavigne, J. -P., Lucas, S., Michiels, T., Moore, E. R. B., Nixon-Abell, J., Rossello-Mora, R., Shi, Z., Siccardi, A. G., Sitia, R., Tillett, D., Timmis, K. N., Toledano, M. B., van der Sluijs, P., Vicenzi, E., and UCL - SSS/DDUV - Institut de Duve

Subjects
Opinion, viruses, Pneumonia, Viral, Gene Expression, Microbiology, Disease Outbreaks, Evolution, Molecular, Betacoronavirus, [SDV.MHEP.MI]Life Sciences [q-bio]/Human health and pathology/Infectious diseases, Animals, Humans, Health emergency, Selection, Genetic, Pandemics, Ecology, Evolution, Behavior and Systematics, [SDV.MHEP.ME]Life Sciences [q-bio]/Human health and pathology/Emerging diseases, Virulence, SARS-CoV-2, fungi, COVID-19, SARS Virus, Adaptation, Physiological, Severe acute respiratory syndrome-related coronavirus, Host-Pathogen Interactions, Mutation, Spike Glycoprotein, Coronavirus, [SDV.MP.VIR]Life Sciences [q-bio]/Microbiology and Parasitology/Virology, Coronavirus Infections
Abstract

The current SARS‐CoV‐2 pandemic is wreaking havoc throughout the world and has rapidly become a global health emergency. A central question concerning COVID‐19 is why some individuals become sick and others not. Many have pointed already at variation in risk factors between individuals. However, the variable outcome of SARS‐CoV‐2 infections may, at least in part, be due also to differences between the viral subspecies with which individuals are infected. A more pertinent question is how we are to overcome the current pandemic. A vaccine against SARS‐CoV‐2 would offer significant relief, although vaccine developers have warned that design, testing and production of vaccines may take a year if not longer. Vaccines are based on a handful of different designs (i), but the earliest vaccines were based on the live, attenuated virus. As has been the case for other viruses during earlier pandemics, SARS‐CoV‐2 will mutate and may naturally attenuate over time (ii). What makes the current pandemic unique is that, thanks to state‐of‐the‐art nucleic acid sequencing technologies, we can follow in detail how SARS‐CoV‐2 evolves while it spreads. We argue that knowledge of naturally emerging attenuated SARS‐CoV‐2 variants across the globe should be of key interest in our fight against the pandemic.

Published
2020
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38. Delayed Humoral Response After 2 Doses of the BNT162b2 Vaccine in a Belgian Kidney Transplant Cohort.

Author

UCL - SSS/IREC/NEFR - Pôle de Néphrologie, UCL - (MGD) Service de néphrologie, UCL - SSS/IREC - Institut de recherche expérimentale et clinique, UCL - (SLuc) Service de microbiologie, UCL - SSS/DDUV - Institut de Duve, UCL - (SLuc) Département de médecine interne et services associés, Georgery, Hélène, Devresse, Arnaud, Saad Albichr, Imane, Lucas, Sophie, Yombi, Jean Cyr, Belkhir, Leïla, De Greef, Julien, Scohy, Anaïs, Kabamba Mukadi, Benoît, Goffin, Eric, Kanaan, Nada, UCL - SSS/IREC/NEFR - Pôle de Néphrologie, UCL - (MGD) Service de néphrologie, UCL - SSS/IREC - Institut de recherche expérimentale et clinique, UCL - (SLuc) Service de microbiologie, UCL - SSS/DDUV - Institut de Duve, UCL - (SLuc) Département de médecine interne et services associés, Georgery, Hélène, Devresse, Arnaud, Saad Albichr, Imane, Lucas, Sophie, Yombi, Jean Cyr, Belkhir, Leïla, De Greef, Julien, Scohy, Anaïs, Kabamba Mukadi, Benoît, Goffin, Eric, and Kanaan, Nada

Published
2022

39. 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

40. Combination of immunotherapy and local chemotherapy for the treatment of unresectable glioblastoma

Author

UCL - SSS/LDRI - Louvain Drug Research Institute, UCL - Faculté de pharmacie et des sciences biomédicales, Sonveaux, Pierre, Lucas, Sophie, Gallez, Bernard, Florindo, Helena, Hollevoet, Kevin, Préat, Véronique, Malfanti, Alessio, Bausart, Mathilde, UCL - SSS/LDRI - Louvain Drug Research Institute, UCL - Faculté de pharmacie et des sciences biomédicales, Sonveaux, Pierre, Lucas, Sophie, Gallez, Bernard, Florindo, Helena, Hollevoet, Kevin, Préat, Véronique, Malfanti, Alessio, and Bausart, Mathilde

Abstract

Glioblastoma is the most common and aggressive brain cancer. The low median survival of patients diagnosed with this disease makes it an unmet medical need. Nowadays, immunotherapeutic treatments have shown remarkable results in some populations of cancer patients but are rather ineffective in improving glioblastoma patients’ outcomes when used in monotherapy. The aim of this Ph.D. thesis is to contribute to the research of glioblastoma treatments by developing combination strategies of drug delivery systems to potentiate immunotherapy efficacy. The strategies used in this work include a DNA vaccine encoding glioblastoma-associated antigens, immune checkpoint blockades, and an immunogenic chemotherapeutic agent delivered locally. Our findings confirm the benefit of combination strategies to improve the immune response and increase the survival of glioblastoma., (BIFA - Sciences biomédicales et pharmaceutiques) -- UCL, 2022

Published
2022

41. Nouveaux concepts dans la gestion des urgences dentaires

Author

UCL - SSS/LDRI - Louvain Drug Research Institute, UCL - Faculté de médecine et médecine dentaire, Leprince , Julian, Lucas, Sophie, Leloup, Gaëtane, des Rieux, Anne, Gaudin, Alexis, Blasco, Vincent, Beauquis, Julien, UCL - SSS/LDRI - Louvain Drug Research Institute, UCL - Faculté de médecine et médecine dentaire, Leprince , Julian, Lucas, Sophie, Leloup, Gaëtane, des Rieux, Anne, Gaudin, Alexis, Blasco, Vincent, and Beauquis, Julien

Abstract

The management of dental emergencies is a central and essential issue in the daily practice of dentists. Through two clinical studies, we were able to identify new perspectives: 1/ The strategy of emergency management based on triage with the establishment of recommendations allowed to find an effective compromise between limiting the admission of patients and ensuring the control of their pain and the relief of their symptoms. 2/ More conservative management of irreversible pulpitis. Our data tend to support pulpotomy as an acceptable and more conservative permanent treatment option for irreversible pulpitis of mature molars. Our strategies could be considered as first-line treatments, thus providing additional steps in the therapeutic gradient., (DENT - Sciences dentaires) -- UCL, 2022

Published
2022

43. 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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45. Combined Blockade of GARP:TGF-β1 and PD-1 Increases Infiltration of T Cells and Density of Pericyte-Covered GARP+ Blood Vessels in Mouse MC38 Tumors

Author

Bertrand, Charlotte, primary, Van Meerbeeck, Pierre, additional, de Streel, Grégoire, additional, Vaherto-Bleeckx, Noora, additional, Benhaddi, Fatima, additional, Rouaud, Loïc, additional, Noël, Agnès, additional, Coulie, Pierre G., additional, van Baren, Nicolas, additional, and Lucas, Sophie, additional

Published
2021
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46. Characterization of a new intermediate macrophage subpopulation : SDC-1 positive SPM-like macrophages possess immunosuppressive functions in early mesotheliomagenic responses to carbon nanotubes

Author

UCL - SSS/IREC/LTAP - Louvain Centre for Toxicology and Applied Pharmacology, UCL - Faculté de pharmacie et des sciences biomédicales, Huaux, François, Lucas, Sophie, Marbaix , Etienne, Pilette , Charles, Hoet , Peter, Marichal , Thomas, van der Bruggen, Pierre, Orsi, Micaela, UCL - SSS/IREC/LTAP - Louvain Centre for Toxicology and Applied Pharmacology, UCL - Faculté de pharmacie et des sciences biomédicales, Huaux, François, Lucas, Sophie, Marbaix , Etienne, Pilette , Charles, Hoet , Peter, Marichal , Thomas, van der Bruggen, Pierre, and Orsi, Micaela

Abstract

Malignant mesothelioma is a disease caused by inhalation of needle-like shaped particles and whose pathogenesis is not yet fully elucidated. A long-lasting general inflammation caused by persistent mesotheliomagenic particles is not sufficient to explain mesothelioma onset. Indeed, challenging data have shown that mesothelioma occurs without chronic inflammation. Our research team previously helped to discover that, beside inflammation, particles such as silica also induce a selective, rapid and sustained accumulation of immunosuppressive cells (regulatory T lymphocytes, myeloid derived suppressive cells and M2/regulatory macrophages) participating to fibrogenesis. To determine whether carcinogenic particles such as asbestos and carbon nanotubes (CNT) also elicit immunosuppressive responses, we investigated the impact of these particles on macrophage turnover, phenotype and immunosuppressive activity. With that purpose, we intraperitoneally injected mesotheliomagenic CNT-7 (needle-like, Mitsui & Co) and non-mesotheliomagenic CNT-T (tangled, Nagoya University) particles in Wistar rats and compared the effects on peritoneal macrophage subpopulations. We showed that macrophages die very rapidly in the attempt to phagocyte mesotheliomagenic CNT. They are later replenished by monocytic-derived small peritoneal macrophages (SPM-like macrophages) possessing comparable immunosuppressive functions and signatures to Tumor-Associated Macrophages (TAM), which infiltrate mesothelioma and block T cell antitumor activities. Early immunosuppressive SPM-like macrophages express and release the shed form of the immunoregulatory syndecan-1 glycoprotein, which could explain the immunosuppression that they exert on T cells. Non-mesotheliomagenic peritoneal responses induced by CNT-T are, in contrast, characterized by a recruitment of self-proliferating large peritoneal macrophages (LPM-like macrophages) that correspond to homeostatic macrophages without immunosuppressive activity. Our o, (BIFA - Sciences biomédicales et pharmaceutiques) -- UCL, 2021

Published
2021

48. Multiple modes of action for antibodies targeting GARP-expressing cells in tumors

Author

UCL - SSS/DDUV - Institut de Duve, UCL - Faculté de pharmacie et des sciences biomédicales, Lucas, Sophie, Michiels, Thomas, Dumoutier, Laure, Van Baren, Nicolas, Coulie, Pierre, Noel, Agnès, Labarrière, Nathalie, Bertrand, Charlotte, UCL - SSS/DDUV - Institut de Duve, UCL - Faculté de pharmacie et des sciences biomédicales, Lucas, Sophie, Michiels, Thomas, Dumoutier, Laure, Van Baren, Nicolas, Coulie, Pierre, Noel, Agnès, Labarrière, Nathalie, and Bertrand, Charlotte

Abstract

Cancer immunotherapies, such as monoclonal antibodies (mAbs) directed against PD-1, aim at boosting immune responses against tumor cells. They have become a standard of care for several types of cancer. However, a majority of patients do not respond to current immunotherapies. Resistance to PD-1 blockade can in part be explained by the action of TGF-b1, an immunosuppressive cytokine activated notably by regulatory T cells (Tregs) via a mechanism that requires protein GARP. We developed antibodies against GARP:TGF-b1 complexes that block TGF-b1 activation by Tregs and we evaluated their anti-tumor efficacy in tumor-bearing mice. We observed that anti-GARP:TGF-b1 mAbs induce the regression of tumors otherwise resistant to anti-PD-1, and we showed that combined blockade of GARP:TGF-b1 and PD-1 can exert anti-tumor activity via multiple modes of action. This may prove important for the selection of cancer patients who could benefit from this novel form of immunotherapy in the clinics., (BIFA - Sciences biomédicales et pharmaceutiques) -- UCL, 2021

Published
2021

49. Molecular mechanisms leading to the emergence of mouse regulatory T lymphocytes specific to non-inherited maternal antigens

Author

Braun, Michel Y, Corazza, Francis, Lucas, Sophie, Geenen, Vincent, Marchant, Arnaud, Truyens, Carine, Oldenhove, Guillaume, Lefevre, Nicolas, Li, Shuang, Braun, Michel Y, Corazza, Francis, Lucas, Sophie, Geenen, Vincent, Marchant, Arnaud, Truyens, Carine, Oldenhove, Guillaume, Lefevre, Nicolas, and Li, Shuang

Abstract

[EN]It is well illustrated that the generation of Tregs is the main mechanism responsible for maintaining immune tolerance during developmental exposure to non-inherited maternal antigen (NIMA). Moreover, the presence of NIMA-specific Tregs in the uterus of pregnant mice promote reproductive fitness by enforcing maternal tolerance to overlapping paternal antigens expressed by the fetus during next-generation pregnancies. However, the reason why perinatal T cell lineage is biased towards immune tolerance is poorly understood. Due to the fact that terminal deoxynucleotidyl transferase (TdT) is not expressed in neonatal T cells in the mouse, neonatal T cells have a less diverse TCR repertoire. This is known to limit their specificity and to increase their affinity for MHC/peptide complexes. At the start of the present work, we postulated that expressing high affinity TCR might be the reason that forces the development of antigen-specific Tregs in neonates. We undertook our study with the aim to investigate the mechanisms underlying mouse NIMA-specific Treg development in the perinatal period. Using 2W1S-OVA+ heterozygous mouse model in which 2W1S antigen was transformed into surrogate NIMA for half of the offspring, we observed an increased frequency of 2W1S-specific Tregs in NIMA-2W1S-exposed animals. Moreover, we also observed that periphery-derived NIMA-2W1S Tregs had a less diverse TCR repertoire and were phenotypically distinct from thymus-derived SELF-2W1S-specific Tregs. In order to investigate whether the lack of diversity was responsible for the development of neonatal NIMA-specific Tregs, we generated transgenic mice where TdT expression was enforced in T cells before birth. We found that transgenic TdT added clonal TCR diversity but did not prevent the development of T cell clones with neonatal type TCR repertoire and did not modify the frequency of neonatal NIMA-specific Tregs. On the contrary, TdT expression increased significantly generation of SELF-speci, [FR]Il est bien illustré que la génération périnatal de Treg est le principal mécanisme responsable du maintien de la tolérance immunitaire fœtale qui se développe suite à l'exposition aux antigènes maternels non-hérités (NIMA). De plus, la présence de Tregs spécifiques des NIMA dans l'utérus des femmes enceintes favorise la capacité de reproduction en renforçant la tolérance maternelle aux mêmes antigènes paternels exprimés par le fœtus pendant les grossesses de prochaine génération. Cependant, la raison pour laquelle la lignée des cellules T fœtales est biaisée en faveur de la tolérance immunitaire est mal comprise. Chez la souris, en raison du manque d'expression de la désoxynucléotidyl transférase terminale (TdT), les cellules T néonatales ont un répertoire de TCR moins diversifié. Ceci est connu pour limiter leur spécificité et augmenter leur affinité pour les complexes CMH / peptide. Au début du présent travail, nous avons émis l'hypothèse que l'expression de TCRs de haute affinité pourrait être la raison qui force le développement de Treg spécifiques chez les nouveau-nés. Nous avons plus particulièrement entrepris notre étude dans le but d'étudier les mécanismes sous-jacents au développement de Tregs spécifiques des NIMA chez la souris pendant la période périnatale. En utilisant le modèle de souris hétérozygotes pour 2W1S-OVA+ dans lequel l'antigène 2W1S a été transformé en NIMA pour la moitié de la progéniture, nous avons observé une fréquence accrue de Tregs spécifiques de 2W1S chez les animaux exposés au NIMA. De plus, nous avons également observé que les Treg NIMA-2W1S dérivés de la périphérie avaient un répertoire de TCRs moins diversifié et étaient phénotypiquement distincts des Tregs spécifiques de SELF-2W1S dérivés du thymus. Afin de déterminer si le manque de diversité était responsable du développement de Tregs néonataux spécifiques de NIMA, nous avons généré des souris transgéniques où l'expression de TdT était appliquée dans les cellules T avant l, Doctorat en Sciences biomédicales et pharmaceutiques (Médecine), info:eu-repo/semantics/nonPublished

Published
2021

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