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1. Emergence of the B.1.214.2 SARS-CoV-2 lineage with an Omicron-like spike insertion and a unique upper airway immune signature.

Author

Holtz, Andrew, Van Weyenbergh, Johan, Hong, Samuel, Cuypers, Lize, OToole, Áine, Dudas, Gytis, Gerdol, Marco, Potter, Barney, Ntoumi, Francine, Mapanguy, Claujens, Vanmechelen, Bert, Wawina-Bokalanga, Tony, Van Holm, Bram, Menezes, Soraya, Soubotko, Katja, Van Pottelbergh, Gijs, Wollants, Elke, Vermeersch, Pieter, Jacob, Ann-Sophie, Maes, Brigitte, Obbels, Dagmar, Matheeussen, Veerle, Martens, Geert, Gras, Jérémie, Verhasselt, Bruno, Laffut, Wim, Vael, Carl, Goegebuer, Truus, van der Kant, Rob, Rousseau, Frederic, Schymkowitz, Joost, Serrano, Luis, Delgado, Javier, Wenseleers, Tom, Bours, Vincent, André, Emmanuel, Suchard, Marc, Rambaut, Andrew, Dellicour, Simon, Maes, Piet, Durkin, Keith, and Baele, Guy

Subjects
COVID-19, Disease spread, Genomic epidemiology, Phylodynamics, Phylogeography, SARS-CoV-2, Humans, SARS-CoV-2, COVID-19, Spike Glycoprotein, Coronavirus, Aged, Male, Travel, Belgium, Middle Aged, Female, Adult, Phylogeography, Nasopharynx
Abstract

We investigate the emergence, mutation profile, and dissemination of SARS-CoV-2 lineage B.1.214.2, first identified in Belgium in January 2021. This variant, featuring a 3-amino acid insertion in the spike protein similar to the Omicron variant, was speculated to enhance transmissibility or immune evasion. Initially detected in international travelers, it substantially transmitted in Central Africa, Belgium, Switzerland, and France, peaking in April 2021. Our travel-aware phylogeographic analysis, incorporating travel history, estimated the origin to the Republic of the Congo, with primary European entry through France and Belgium, and multiple smaller introductions during the epidemic. We correlate its spread with human travel patterns and air passenger data. Further, upon reviewing national reports of SARS-CoV-2 outbreaks in Belgian nursing homes, we found this strain caused moderately severe outcomes (8.7% case fatality ratio). A distinct nasopharyngeal immune response was observed in elderly patients, characterized by 80% unique signatures, higher B- and T-cell activation, increased type I IFN signaling, and reduced NK, Th17, and complement system activation, compared to similar outbreaks. This unique immune response may explain the variants epidemiological behavior and underscores the need for nasal vaccine strategies against emerging variants.

Published
2024

4. Transcriptome analysis reveals tumor microenvironment changes in glioblastoma

Author

Hoogstrate, Youri, Draaisma, Kaspar, Ghisai, Santoesha A., van Hijfte, Levi, Barin, Nastaran, de Heer, Iris, Coppieters, Wouter, van den Bosch, Thierry P.P., Bolleboom, Anne, Gao, Zhenyu, Vincent, Arnaud J.P.E., Karim, Latifa, Deckers, Manon, Taphoorn, Martin J.B., Kerkhof, Melissa, Weyerbrock, Astrid, Sanson, Marc, Hoeben, Ann, Lukacova, Slávka, Lombardi, Giuseppe, Leenstra, Sieger, Hanse, Monique, Fleischeuer, Ruth E.M., Watts, Colin, Angelopoulos, Nicos, Gorlia, Thierry, Golfinopoulos, Vassilis, Bours, Vincent, van den Bent, Martin J., Robe, Pierre A., and French, Pim J.

Published
2023
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5. Genotype-first approach to identify associations between CDH1 germline variants and cancer phenotypes: a multicentre study by the European Reference Network on Genetic Tumour Risk Syndromes

Author

Garcia-Pelaez, José, Barbosa-Matos, Rita, Lobo, Silvana, Dias, Alexandre, Garrido, Luzia, Castedo, Sérgio, Sousa, Sónia, Pinheiro, Hugo, Sousa, Liliana, Monteiro, Rita, Maqueda, Joaquin J, Fernandes, Susana, Carneiro, Fátima, Pinto, Nádia, Lemos, Carolina, Pinto, Carla, Teixeira, Manuel R, Aretz, Stefan, Bajalica-Lagercrantz, Svetlana, Balmaña, Judith, Blatnik, Ana, Benusiglio, Patrick R, Blanluet, Maud, Bours, Vincent, Brems, Hilde, Brunet, Joan, Calistri, Daniele, Capellá, Gabriel, Carrera, Sergio, Colas, Chrystelle, Dahan, Karin, de Putter, Robin, Desseignés, Camille, Domínguez-Garrido, Elena, Egas, Conceição, Evans, D Gareth, Feret, Damien, Fewings, Eleanor, Fitzgerald, Rebecca C, Coulet, Florence, Garcia-Barcina, María, Genuardi, Maurizio, Golmard, Lisa, Hackmann, Karl, Hanson, Helen, Holinski-Feder, Elke, Hüneburg, Robert, Krajc, Mateja, Lagerstedt-Robinson, Kristina, Lázaro, Conxi, Ligtenberg, Marjolijn J L, Martínez-Bouzas, Cristina, Merino, Sonia, Michils, Geneviève, Novaković, Srdjan, Patiño-García, Ana, Ranzani, Guglielmina Nadia, Schröck, Evelin, Silva, Inês, Silveira, Catarina, Soto, José L, Spier, Isabel, Steinke-Lange, Verena, Tedaldi, Gianluca, Tejada, María-Isabel, Woodward, Emma R, Tischkowitz, Marc, Hoogerbrugge, Nicoline, and Oliveira, Carla

Published
2023
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7. Genetic etiology of autism spectrum disorder in the African population: a scoping review.

Author

Hakizimana, Olivier, Hitayezu, Janvier, Uyisenga, Jeanne P., Onohuean, Hope, Palmeira, Leonor, Bours, Vincent, Alagbonsi, Abdullateef Isiaka, and Uwineza, Annette

Subjects
SOUTH Africans, GENOME-wide association studies, AUTISM spectrum disorders, ONLINE databases, CHROMOSOME abnormalities
Abstract

Background: Autism spectrum disorder (ASD) is a neurodevelopmental disorder (NDD) characterized by significant impairments in social, communicative, and behavioral abilities. However, only a limited number of studies address the genetic basis of ASD in the African population. This study aims to document the genes associated with ASD in Africa and the techniques used to identify them. Additionally, genes identified elsewhere but not yet in Africa are also noted. Methods: Online databases such as Wiley Online Library, PubMed, and Africa Journal Online were used. The review was conducted using the keyword related to genetic and genomic ASD study in the African population. Result: In this scoping review, 40 genetic studies on ASD in Africa were reviewed. The Egyptian and South African populations were the most studied, with 25 and 5 studies, respectively. Countries with fewer studies included Tunisia (4), East African countries (3), Libya (1), Nigeria (1), and Morocco (1). Some 61 genes responsible for ASD were identified in the African population: 26 were identified using a polymerase chain reaction (PCR)-based method, 22 were identified using sequencing technologies, and 12 genes and one de novo chromosomal aberration were identified through other techniques. No African study identified any ASD gene with genome-wide association studies (GWAS). Notably, at least 20 ASD risk genes reported in non-African countries were yet to be confirmed in Africa's population. Conclusion: There are insufficient genetic studies on ASD in the African population, with sample size being a major limitation in most genetic association studies, leading to inconclusive results. Thus, there is a need to conduct more studies with large sample sizes to identify other genes associated with ASD in Africa's population using high-throughput sequencing technology. [ABSTRACT FROM AUTHOR]

Published
2024
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8. Outcome of publicly funded nationwide first-tier noninvasive prenatal screening

Author

Van Den Bogaert, Kris, Lannoo, Lore, Brison, Nathalie, Gatinois, Vincent, Baetens, Machteld, Blaumeiser, Bettina, Boemer, François, Bourlard, Laura, Bours, Vincent, De Leener, Anne, De Rademaeker, Marjan, Désir, Julie, Dheedene, Annelies, Duquenne, Armelle, Fieremans, Nathalie, Fieuw, Annelies, Gatot, Jean-Stéphane, Grisart, Bernard, Janssens, Katrien, Janssens, Sandra, Lederer, Damien, Marichal, Axel, Menten, Björn, Meunier, Colombine, Palmeira, Leonor, Pichon, Bruno, Sammels, Eva, Smits, Guillaume, Sznajer, Yves, Vantroys, Elise, Devriendt, Koenraad, and Vermeesch, Joris Robert

Published
2021
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9. Limited Effects of Class II Transactivator-Based Immunotherapy in Murine and Human Glioblastoma

Author

MS KNO, ZL Neuro-Oncologie Medisch, Neurochirurgie, Brain, Cancer, Tan, A Katherine, Henry, Aurelie, Goffart, Nicolas, van Logtestijn, Sofie, Bours, Vincent, Hol, Elly M, Robe, Pierre A, MS KNO, ZL Neuro-Oncologie Medisch, Neurochirurgie, Brain, Cancer, Tan, A Katherine, Henry, Aurelie, Goffart, Nicolas, van Logtestijn, Sofie, Bours, Vincent, Hol, Elly M, and Robe, Pierre A

Published
2024

10. Digenic Inheritance of Mutations in Homologous Recombination Genes in Cancer Patients.

Author

Freire, Maria Valeria, Martin, Marie, Segers, Karin, Sepulchre, Edith, Leroi, Natacha, Coupier, Jérôme, Kalantari, Hassan Rezaei, Wolter, Pascal, Collignon, Joëlle, Polus, Marc, Plomteux, Olivier, Josse, Claire, and Bours, Vincent

Subjects
HEREDITY, HOMOLOGOUS recombination, CANCER genes, CANCER patients, PATIENTS' families
Abstract

Background/Objectives: BRCA1, BRCA2, ATM, and CHEK2 are known cancer predisposition genes (CPGs), but tumor risk in patients with simultaneous pathogenic variants (PVs) in CPGs remains largely unknown. In this study, we describe six patients from five families with multiple cancers who coinherited a combination of PVs in these genes. Methods: PVs were identified using NGS DNA sequencing and were confirmed by Sanger. Results: Families 1, 2, and 3 presented PVs in BRCA2 and ATM, family 4 in BRCA2 and BRCA1, and family 5 in BRCA2 and CHEK2. PVs were identified using NGS DNA sequencing and were confirmed by Sanger. The first family included patients with kidney, prostate, and breast cancer, in addition to pancreatic adenocarcinomas. In the second family, a female had breast cancer, while a male from the third family had prostate, gastric, and pancreatic cancer. The fourth family included a male with pancreatic cancer, and the fifth family a female with breast cancer. Conclusions: The early age of diagnosis and the development of multiple cancers in the reported patients indicate a very high risk of cancer in double-heterozygous patients associated with PVs in HR-related CPGs. Therefore, in families with patients who differ from other family members in terms of phenotype, age of diagnosis, or type of cancer, the cascade testing needs to include the study of other CPGs. [ABSTRACT FROM AUTHOR]

Published
2024
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11. Somatic mosaicism underlies X-linked acrogigantism syndrome in sporadic male subjects.

Author

Daly, Adrian, Yuan, Bo, Fina, Frederic, Caberg, Jean-Hubert, Trivellin, Giampaolo, Rostomyan, Liliya, de Herder, Wouter, Naves, Luciana, Metzger, Daniel, Cuny, Thomas, Rabl, Wolfgang, Shah, Nalini, Jaffrain-Rea, Marie-Lise, Zatelli, Maria, Faucz, Fabio, Castermans, Emilie, Nanni-Metellus, Isabelle, Lodish, Maya, Muhammad, Ammar, Palmeira, Leonor, Potorac, Iulia, Mantovani, Giovanna, Neggers, Sebastian, Klein, Marc, Barlier, Anne, Liu, Pengfei, Ouafik, LHoucine, Bours, Vincent, Lupski, James, Stratakis, Constantine, and Beckers, Albert

Subjects
X-LAG syndrome, gigantism, molecular genetics, mosaicism, pituitary, Adult, Female, Genetic Diseases, X-Linked, Gigantism, Humans, Male, Middle Aged, Mosaicism, Polymerase Chain Reaction, Syndrome, Young Adult
Abstract

Somatic mosaicism has been implicated as a causative mechanism in a number of genetic and genomic disorders. X-linked acrogigantism (XLAG) syndrome is a recently characterized genomic form of pediatric gigantism due to aggressive pituitary tumors that is caused by submicroscopic chromosome Xq26.3 duplications that include GPR101 We studied XLAG syndrome patients (n= 18) to determine if somatic mosaicism contributed to the genomic pathophysiology. Eighteen subjects with XLAG syndrome caused by Xq26.3 duplications were identified using high-definition array comparative genomic hybridization (HD-aCGH). We noted that males with XLAG had a decreased log2ratio (LR) compared with expected values, suggesting potential mosaicism, whereas females showed no such decrease. Compared with familial male XLAG cases, sporadic males had more marked evidence for mosaicism, with levels of Xq26.3 duplication between 16.1 and 53.8%. These characteristics were replicated using a novel, personalized breakpoint junction-specific quantification droplet digital polymerase chain reaction (ddPCR) technique. Using a separate ddPCR technique, we studied the feasibility of identifying XLAG syndrome cases in a distinct patient population of 64 unrelated subjects with acromegaly/gigantism, and identified one female gigantism patient who had had increased copy number variation (CNV) threshold for GPR101 that was subsequently diagnosed as having XLAG syndrome on HD-aCGH. Employing a combination of HD-aCGH and novel ddPCR approaches, we have demonstrated, for the first time, that XLAG syndrome can be caused by variable degrees of somatic mosaicism for duplications at chromosome Xq26.3. Somatic mosaicism was shown to occur in sporadic males but not in females with XLAG syndrome, although the clinical characteristics of the disease were similarly severe in both sexes.

Published
2016

13. Three years pilot of spinal muscular atrophy newborn screening turned into official program in Southern Belgium

Author

Boemer, François, Caberg, Jean-Hubert, Beckers, Pablo, Dideberg, Vinciane, di Fiore, Samantha, Bours, Vincent, Marie, Sandrine, Dewulf, Joseph, Marcelis, Lionel, Deconinck, Nicolas, Daron, Aurore, Blasco-Perez, Laura, Tizzano, Eduardo, Hiligsmann, Mickaël, Lombet, Jacques, Pereira, Tatiana, Lopez-Granados, Lucia, Shalchian-Tehran, Sarvnaz, van Assche, Véronique, Willems, Arabelle, Huybrechts, Sofie, Mast, Bénédicte, van Olden, Rudolf, Dangouloff, Tamara, and Servais, Laurent

Published
2021
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14. Genomic sequencing of SARS-CoV-2 in Rwanda reveals the importance of incoming travelers on lineage diversity

Author

Butera, Yvan, Mukantwari, Enatha, Artesi, Maria, Umuringa, Jeanne d’arc, O’Toole, Áine Niamh, Hill, Verity, Rooke, Stefan, Hong, Samuel Leandro, Dellicour, Simon, Majyambere, Onesphore, Bontems, Sebastien, Boujemla, Bouchra, Quick, Josh, Resende, Paola Cristina, Loman, Nick, Umumararungu, Esperance, Kabanda, Alice, Murindahabi, Marylin Milumbu, Tuyisenge, Patrick, Gashegu, Misbah, Rwabihama, Jean Paul, Sindayiheba, Reuben, Gikic, Djordje, Souopgui, Jacob, Ndifon, Wilfred, Rutayisire, Robert, Gatare, Swaibu, Mpunga, Tharcisse, Ngamije, Daniel, Bours, Vincent, Rambaut, Andrew, Nsanzimana, Sabin, Baele, Guy, Durkin, Keith, Mutesa, Leon, and Rujeni, Nadine

Published
2021
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15. PCIP-seq: simultaneous sequencing of integrated viral genomes and their insertion sites with long reads

Author

Artesi, Maria, Hahaut, Vincent, Cole, Basiel, Lambrechts, Laurens, Ashrafi, Fereshteh, Marçais, Ambroise, Hermine, Olivier, Griebel, Philip, Arsic, Natasa, van der Meer, Frank, Burny, Arsène, Bron, Dominique, Bianchi, Elettra, Delvenne, Philippe, Bours, Vincent, Charlier, Carole, Georges, Michel, Vandekerckhove, Linos, Van den Broeke, Anne, and Durkin, Keith

Published
2021
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19. X-linked acrogigantism syndrome: clinical profile and therapeutic responses

Author

Beckers, Albert, Lodish, Maya Beth, Trivellin, Giampaolo, Rostomyan, Liliya, Lee, Misu, Faucz, Fabio R, Yuan, Bo, Choong, Catherine S, Caberg, Jean-Hubert, Verrua, Elisa, Naves, Luciana Ansaneli, Cheetham, Tim D, Young, Jacques, Lysy, Philippe A, Petrossians, Patrick, Cotterill, Andrew, Shah, Nalini Samir, Metzger, Daniel, Castermans, Emilie, Ambrosio, Maria Rosaria, Villa, Chiara, Strebkova, Natalia, Mazerkina, Nadia, Gaillard, Stéphan, Barra, Gustavo Barcelos, Casulari, Luis Augusto, Neggers, Sebastian J, Salvatori, Roberto, Jaffrain-Rea, Marie-Lise, Zacharin, Margaret, Santamaria, Beatriz Lecumberri, Zacharieva, Sabina, Lim, Ee Mun, Mantovani, Giovanna, Zatelli, Maria Chaira, Collins, Michael T, Bonneville, Jean-François, Quezado, Martha, Chittiboina, Prashant, Oldfield, Edward H, Bours, Vincent, Liu, Pengfei, W de Herder, Wouter, Pellegata, Natalia, Lupski, James R, Daly, Adrian F, and Stratakis, Constantine A

Subjects
Biomedical and Clinical Sciences, Clinical Sciences, Brain Disorders, Rare Diseases, Pediatric, Clinical Research, Cancer, Acromegaly, Adenoma, Adolescent, Child, Child, Preschool, Chromosomes, Human, X, Female, Gigantism, Humans, Infant, Male, Pituitary Neoplasms, Young Adult, gigantism, X chromosome, pituitary adenoma, pediatric, X-LAG syndrome, GPR101, FIPA, duplication, Biological Sciences, Medical and Health Sciences, Oncology & Carcinogenesis, Clinical sciences, Oncology and carcinogenesis
Abstract

X-linked acrogigantism (X-LAG) is a new syndrome of pituitary gigantism, caused by microduplications on chromosome Xq26.3, encompassing the gene GPR101, which is highly upregulated in pituitary tumors. We conducted this study to explore the clinical, radiological, and hormonal phenotype and responses to therapy in patients with X-LAG syndrome. The study included 18 patients (13 sporadic) with X-LAG and microduplication of chromosome Xq26.3. All sporadic cases had unique duplications and the inheritance pattern in two families was dominant, with all Xq26.3 duplication carriers being affected. Patients began to grow rapidly as early as 2-3 months of age (median 12 months). At diagnosis (median delay 27 months), patients had a median height and weight standard deviation scores (SDS) of >+3.9 SDS. Apart from the increased overall body size, the children had acromegalic symptoms including acral enlargement and facial coarsening. More than a third of cases had increased appetite. Patients had marked hypersecretion of GH/IGF1 and usually prolactin, due to a pituitary macroadenoma or hyperplasia. Primary neurosurgical control was achieved with extensive anterior pituitary resection, but postoperative hypopituitarism was frequent. Control with somatostatin analogs was not readily achieved despite moderate to high levels of expression of somatostatin receptor subtype-2 in tumor tissue. Postoperative use of adjuvant pegvisomant resulted in control of IGF1 in all five cases where it was employed. X-LAG is a new infant-onset gigantism syndrome that has a severe clinical phenotype leading to challenging disease management.

Published
2015

20. Gigantism and acromegaly due to Xq26 microduplications and GPR101 mutation.

Author

Trivellin, Giampaolo, Daly, Adrian, Faucz, Fabio, Yuan, Bo, Rostomyan, Liliya, Larco, Darwin, Schernthaner-Reiter, Marie, Szarek, Eva, Leal, Letícia, Caberg, Jean-Hubert, Castermans, Emilie, Villa, Chiara, Dimopoulos, Aggeliki, Chittiboina, Prashant, Xekouki, Paraskevi, Shah, Nalini, Metzger, Daniel, Lysy, Philippe, Ferrante, Emanuele, Strebkova, Natalia, Mazerkina, Nadia, Zatelli, Maria, Lodish, Maya, Horvath, Anelia, de Alexandre, Rodrigo, Manning, Allison, Levy, Isaac, Keil, Margaret, Sierra, Maria, Palmeira, Leonor, Coppieters, Wouter, Georges, Michel, Naves, Luciana, Jamar, Mauricette, Bours, Vincent, Wu, T, Choong, Catherine, Bertherat, Jerome, Chanson, Philippe, Kamenický, Peter, Farrell, William, Barlier, Anne, Quezado, Martha, Bjelobaba, Ivana, Stojilkovic, Stanko, Wess, Jurgen, Costanzi, Stefano, Liu, Pengfei, Lupski, James, Beckers, Albert, and Stratakis, Constantine

Subjects
Acromegaly, Adolescent, Adult, Age of Onset, Child, Child, Preschool, Chromosome Duplication, Chromosomes, Human, X, Female, Gigantism, Human Growth Hormone, Humans, Infant, Male, Mutation, Phenotype, Protein Conformation, Receptors, G-Protein-Coupled
Abstract

BACKGROUND: Increased secretion of growth hormone leads to gigantism in children and acromegaly in adults; the genetic causes of gigantism and acromegaly are poorly understood. METHODS: We performed clinical and genetic studies of samples obtained from 43 patients with gigantism and then sequenced an implicated gene in samples from 248 patients with acromegaly. RESULTS: We observed microduplication on chromosome Xq26.3 in samples from 13 patients with gigantism; of these samples, 4 were obtained from members of two unrelated kindreds, and 9 were from patients with sporadic cases. All the patients had disease onset during early childhood. Of the patients with gigantism who did not carry an Xq26.3 microduplication, none presented before the age of 5 years. Genomic characterization of the Xq26.3 region suggests that the microduplications are generated during chromosome replication and that they contain four protein-coding genes. Only one of these genes, GPR101, which encodes a G-protein-coupled receptor, was overexpressed in patients pituitary lesions. We identified a recurrent GPR101 mutation (p.E308D) in 11 of 248 patients with acromegaly, with the mutation found mostly in tumors. When the mutation was transfected into rat GH3 cells, it led to increased release of growth hormone and proliferation of growth hormone-producing cells. CONCLUSIONS: We describe a pediatric disorder (which we have termed X-linked acrogigantism [X-LAG]) that is caused by an Xq26.3 genomic duplication and is characterized by early-onset gigantism resulting from an excess of growth hormone. Duplication of GPR101 probably causes X-LAG. We also found a recurrent mutation in GPR101 in some adults with acromegaly. (Funded by the Eunice Kennedy Shriver National Institute of Child Health and Human Development and others.).

Published
2014

22. Identification of a new VHL exon and complex splicing alterations in familial erythrocytosis or von Hippel-Lindau disease

Author

Lenglet, Marion, Robriquet, Florence, Schwarz, Klaus, Camps, Carme, Couturier, Anne, Hoogewijs, David, Buffet, Alexandre, Knight, Samantha J.L., Gad, Sophie, Couvé, Sophie, Chesnel, Franck, Pacault, Mathilde, Lindenbaum, Pierre, Job, Sylvie, Dumont, Solenne, Besnard, Thomas, Cornec, Marine, Dreau, Helene, Pentony, Melissa, Kvikstad, Erika, Deveaux, Sophie, Burnichon, Nelly, Ferlicot, Sophie, Vilaine, Mathias, Mazzella, Jean-Michaël, Airaud, Fabrice, Garrec, Céline, Heidet, Laurence, Irtan, Sabine, Mantadakis, Elpis, Bouchireb, Karim, Debatin, Klaus-Michael, Redon, Richard, Bezieau, Stéphane, Bressac-de Paillerets, Brigitte, Teh, Bin Tean, Girodon, François, Randi, Maria-Luigia, Putti, Maria Caterina, Bours, Vincent, Van Wijk, Richard, Göthert, Joachim R., Kattamis, Antonis, Janin, Nicolas, Bento, Celeste, Taylor, Jenny C., Arlot-Bonnemains, Yannick, Richard, Stéphane, Gimenez-Roqueplo, Anne-Paule, Cario, Holger, and Gardie, Betty

Published
2018
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25. Limited Effects of Class II Transactivator-Based Immunotherapy in Murine and Human Glioblastoma.

Author

Tan, A. Katherine, Henry, Aurelie, Goffart, Nicolas, van Logtestijn, Sofie, Bours, Vincent, Hol, Elly M., and Robe, Pierre A.

Subjects
GLIOMA treatment, CELL metabolism, IN vitro studies, REVERSE transcriptase polymerase chain reaction, IMMUNIZATION, ANIMAL experimentation, MACROPHAGES, KILLER cells, HISTOCOMPATIBILITY, TREATMENT effectiveness, LYMPHOCYTES, RESEARCH funding, MYELOID cells, IMMUNOTHERAPY, MICE
Abstract

Simple Summary: The major histocompatibility complex type II is downregulated in glioblastoma (GB) due to the silencing of the major transcriptional regulator class II transactivator (CIITA). Recent studies have posed CIITA as a possible target in treating patients with GB. However, our results show that in mice, vaccination experiments with wildtype (-WT) and CIITA-expressing cells (-CIITA) equivalently protect against subsequent intracerebral challenges with GL261 cells. Adoptive cell transfer experiments likewise showed a similar antitumor potential of lymphocytes harvested from mice implanted intracerebrally with GL261-WT or -CIITA. Human GB-infiltrating myeloid cells, lymphocytes and NK cells remained mostly inactivated and/or tumor-supportive when in co-culture with GB cells, regardless of CIITA. Altogether, these results question the therapeutic potential of CIITA-mediated immunotherapy in glioblastoma. Background: The major histocompatibility complex type II is downregulated in glioblastoma (GB) due to the silencing of the major transcriptional regulator class II transactivator (CIITA). We investigated the pro-immunogenic potential of CIITA overexpression in mouse and human GB. Methods: The intracerebral growth of wildtype GL261-WT cells was assessed following contralateral injection of GL261-CIITA cells or flank injections with GL261-WT or GL261-CIITA cells. Splenocytes obtained from mice implanted intracerebrally with GL261-WT, GL261-CIITA cells or phosphate buffered saline (PBS) were transferred to other mice and subsequently implanted intracerebrally with GL261-WT. Human GB cells and (syngeneic) GB-infiltrating immune cells were isolated from surgical samples and co-cultured with GB cells expressing CIITA or not, followed by RT-qPCR assessment of the expression of key immune regulators. Results: Intracerebral vaccination of GL261-CIITA significantly reduced the subsequent growth of GL261-WT cells implanted contralaterally. Vaccination with GL261-WT or -CIITA subcutaneously, however, equivalently retarded the intracerebral growth of GL261 cells. Adoptive cell transfer experiments showed a similar antitumor potential of lymphocytes harvested from mice implanted intracerebrally with GL261-WT or -CIITA. Human GB-infiltrating myeloid cells and lymphocytes were not activated when cultured with CIITA-expressing GB cells. Tumor-infiltrating NK cells remained mostly inactivated when in co-culture with GB cells, regardless of CIITA. Conclusion: these results question the therapeutic potential of CIITA-mediated immunotherapy in glioblastoma. [ABSTRACT FROM AUTHOR]

Published
2024
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26. Newborn screening for sickle cell disease in Kisangani, Democratic Republic of the Congo: an update.

Author

Kasai, Emmanuel Tebandite, Gulbis, Béatrice, Ntukamunda, Justin Kadima, Bours, Vincent, Batina Agasa, Salomon, Marini Djang'eing'a, Roland, Boemer, François, Katenga Bosunga, Gedeon, Ngbonda Dauly, Nestor, Sokoni Vutseme, La Joie, Boso Mokili, Bosco, and Alworong'a Opara, Jean Pierre

Subjects
SICKLE cell anemia, NEWBORN screening, NEONATAL nursing, ETHNIC groups, HOMOZYGOSITY
Abstract

Neonatal screening is the first action necessary to identify children with sickle cell disease (SCD) and thus ensure their care. Using rapid tests to give an immediate result to families is a new resilient approach of great interest. These two aspects are essential for establishing an adequate health policy for this disease. This study was undertaken in Kisangani to update the current incidence of neonatal SCD. Heel prick blood samples of 1432 babies born from different racial groups of parents living in Kisangani were collected at birth and screened using a point of care test, i.e. the HemoTypeSCTM. The incidence at birth was 2.2% (n = 31; 95% CI: [1.5%−3.1%]) for HbSS homozygosity and 21% (n = 303; 95% CI: [19%−23%]) for HbAS heterozygosity. Compared to a previous study in 2010; the incidence at the birth of the HbSS form has doubled, while that of the heterozygous form HbAS remained almost unchanged. The inter-ethnic incidence of HbSS among the five top-represented ethnic groups was significant (<0.001). The prevalence of homozygote form has doubled compared to the 0.96% reported in 2010. Setting up a neonatal screening program and an awareness unit is necessary to assess the need for care services correctly. [ABSTRACT FROM AUTHOR]

Published
2023
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27. A dualistic model of primary anal canal adenocarcinoma with distinct cellular origins, etiologies, inflammatory microenvironments and mutational signatures: implications for personalised medicine

Author

Herfs, Michael, Roncarati, Patrick, Koopmansch, Benjamin, Peulen, Olivier, Bruyere, Diane, Lebeau, Alizee, Hendrick, Elodie, Hubert, Pascale, Poncin, Aurelie, Penny, William, Piazzon, Nathalie, Monnien, Franck, Guenat, David, Mougin, Christiane, Prétet, Jean-Luc, Vuitton, Lucine, Segers, Karin, Lambert, Frederic, Bours, Vincent, de Leval, Laurence, Valmary-Degano, Severine, Quick, Charles M, Crum, Christopher P, and Delvenne, Philippe

Published
2018
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30. Diagnostic Performance of Immunohistochemistry Compared to Molecular Techniques for Microsatellite Instability and p53 Mutation Detection in Endometrial Cancer

Author

Streel, Sylvie, primary, Salmon, Alixe, additional, Dheur, Adriane, additional, Bours, Vincent, additional, Leroi, Natacha, additional, Habran, Lionel, additional, Delbecque, Katty, additional, Goffin, Frédéric, additional, Pleyers, Clémence, additional, Kakkos, Athanasios, additional, Gonne, Elodie, additional, Seidel, Laurence, additional, Kridelka, Frédéric, additional, and Gennigens, Christine, additional

Published
2023
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31. Integrative multi-omic analysis: towards treatment de-escalation for early stage HER2-positive breast cancer

Author

Sotiriou, Christos, Le Moine, Alain, Beck, Benjamin, Bours, Vincent, Meylan, Etienne, Pistilli, Barbara, Van Keymeulen, Alexandra, Rediti, Mattia, Sotiriou, Christos, Le Moine, Alain, Beck, Benjamin, Bours, Vincent, Meylan, Etienne, Pistilli, Barbara, Van Keymeulen, Alexandra, and Rediti, Mattia

Abstract

Human Epidermal growth factor Receptor 2 (HER2)-positive breast cancer accounts for approximately 15-20% of all breast cancer cases. The HER2-targeting monoclonal antibody trastuzumab revolutionized HER2-positive breast cancer prognosis and was followed by the development of additional anti-HER2 agents. Nonetheless, despite these major therapeutic advances, response to anti-HER2 treatments is heterogeneous. Indeed, dual HER2-blockade in the (neo)adjuvant setting led only to a limited reduction in the risk of recurrence, and disease relapse is still observed in approximately 5-20% of patients in the early disease setting. In addition, after neoadjuvant therapy 40-60% of the patients present residual disease and, consequently, experience worse long-term outcomes compared to those achieving pathological complete response (pCR). In the last years, the concepts of escalation and de-escalation strategies have become an important topic of discussion for the management of patients with early stage HER2-positive breast cancer, as some of them present excellent outcome and may avoid escalation treatment approaches, sparing them from unnecessary toxicities. The main objective of this thesis was to identify biomarkers of treatment resistance and disease recurrence in patients with early stage HER2-positive breast cancer, in order to develop stratification models able to identify patients with excellent prognosis who may benefit from treatment de-escalation approaches. For this purpose, we aimed to analyze “omics” data, immune-related features and clinicopathological characteristics in patients enrolled in the Neoadjuvant Lapatinib and/or Trastuzumab Treatment Optimisation (NeoALTTO) phase 3 trial, as well as in patients treated with trastuzumab alone in the context of the Adjuvant Lapatinib and/or Trastuzumab Treatment Optimisation (ALTTO) phase 3 trial. In the first study, we investigated the role of copy number aberrations in predicting pCR and survival outcomes in the NeoALT, Doctorat en Sciences médicales (Médecine), info:eu-repo/semantics/nonPublished

Published
2023

32. Impact of treatments on the clinical value of immune response in breast cancer: an insilico analysis

Author

Sotiriou, Christos, Maenhaut, Carine, Van Keymeulen, Alexandra, Rooman, Marianne, Singh, Sumeet Pal, Punie, Kevin, Bours, Vincent, Jose, Vinu, Sotiriou, Christos, Maenhaut, Carine, Van Keymeulen, Alexandra, Rooman, Marianne, Singh, Sumeet Pal, Punie, Kevin, Bours, Vincent, and Jose, Vinu

Abstract

Immune response to breast cancer (immunogenicity of breast cancer) has clinical relevance. Further, many studies report that traditional therapies affect immune response. For example, popular microtubule-targeting agents modulate immune cell function preclinically. This thesis investigates whether microtubule-targeting agents impact immune responses to breast cancer and their clinical relevance.Using the FinHER randomized phase III adjuvant trial comparing the microtubule-stabilizing agent Doxcetaxel to the microtubule-destabilizing agent Vinorelbine with FEC as backbone chemotherapy, the thesis explored the effect of microtubule-stabilizing and destabilizing agents on breast cancer immune response and patient survival. FinHER specimens were preserved as FFPE blocks. A pilot study was performed to determine whether gene modules derived from FFPE specimens profiled on Affymetrix arrays are reproducible. Additionally, FFPE expression profiles were analyzed for the reliability of published gene modules. The results of this study revealed 1) the loss of biological signals from FFPE expression profiles and 2) the feasibility of producing reproducible gene modules from FFPE specimens using Affymetrix arrays with FFPE-specific sample preparation protocols. Based on the pilot study results, FinHER FFPE specimens were profiled. Furthermore, published studies with chemotherapy regimen details were extracted from the GEO database and integrated for validation. The integration of published gene expression data from GEO was necessary since well-curated large public datasets like TCGA, METABRIC, and MetaGxBreast do not provide a detailed characterization of the chemotherapy regimen needed for validation. Using the FinHER and the integrated GEO datasets, the thesis demonstrated a potential interaction between microtubule targeting agents and immune response to clinical outcomes in adjuvant and neoadjuvant breast cancer settings. This interaction’s clinical relevance is discussed.I, Doctorat en Sciences biomédicales et pharmaceutiques (Médecine), info:eu-repo/semantics/nonPublished

Published
2023

33. Transcriptome analysis reveals tumor microenvironment changes in glioblastoma

Author

Research UMC Utrecht, Opleiding Neurochirurgie, Neurochirurgie, Brain, Cancer, Hoogstrate, Youri, Draaisma, Kaspar, Ghisai, Santoesha A., van Hijfte, Levi, Barin, Nastaran, de Heer, Iris, Coppieters, Wouter, van den Bosch, Thierry P.P., Bolleboom, Anne, Gao, Zhenyu, Vincent, Arnaud J.P.E., Karim, Latifa, Deckers, Manon, Taphoorn, Martin J.B., Kerkhof, Melissa, Weyerbrock, Astrid, Sanson, Marc, Hoeben, Ann, Lukacova, Slávka, Lombardi, Giuseppe, Leenstra, Sieger, Hanse, Monique, Fleischeuer, Ruth E.M., Watts, Colin, Angelopoulos, Nicos, Gorlia, Thierry, Golfinopoulos, Vassilis, Bours, Vincent, van den Bent, Martin J., Robe, Pierre A., French, Pim J., Research UMC Utrecht, Opleiding Neurochirurgie, Neurochirurgie, Brain, Cancer, Hoogstrate, Youri, Draaisma, Kaspar, Ghisai, Santoesha A., van Hijfte, Levi, Barin, Nastaran, de Heer, Iris, Coppieters, Wouter, van den Bosch, Thierry P.P., Bolleboom, Anne, Gao, Zhenyu, Vincent, Arnaud J.P.E., Karim, Latifa, Deckers, Manon, Taphoorn, Martin J.B., Kerkhof, Melissa, Weyerbrock, Astrid, Sanson, Marc, Hoeben, Ann, Lukacova, Slávka, Lombardi, Giuseppe, Leenstra, Sieger, Hanse, Monique, Fleischeuer, Ruth E.M., Watts, Colin, Angelopoulos, Nicos, Gorlia, Thierry, Golfinopoulos, Vassilis, Bours, Vincent, van den Bent, Martin J., Robe, Pierre A., and French, Pim J.

Published
2023

36. Rapid Whole Genome Sequencing Diagnoses and Guides Treatment in Critically Ill Children in Belgium in Less than 40 Hours

Author

Lumaka, Aimé, primary, Fasquelle, Corinne, additional, Debray, Francois-Guillaume, additional, Alkan, Serpil, additional, Jacquinet, Adeline, additional, Harvengt, Julie, additional, Boemer, François, additional, Mulder, André, additional, Vaessen, Sandrine, additional, Viellevoye, Renaud, additional, Palmeira, Leonor, additional, Charloteaux, Benoit, additional, Brysse, Anne, additional, Bulk, Saskia, additional, Rigo, Vincent, additional, and Bours, Vincent, additional

Published
2023
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37. The Role of MCM9 in the Etiology of Sertoli Cell-Only Syndrome and Premature Ovarian Insufficiency

Author

Potorac, Iulia, primary, Laterre, Marie, additional, Malaise, Olivier, additional, Nechifor, Vlad, additional, Fasquelle, Corinne, additional, Colleye, Orphal, additional, Detrembleur, Nancy, additional, Verdin, Hannah, additional, Symoens, Sofie, additional, De Baere, Elfride, additional, Daly, Adrian F., additional, Bours, Vincent, additional, Pétrossians, Patrick, additional, and Pintiaux, Axelle, additional

Published
2023
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39. EP150/#325 Endometrial cancer: agreement between P53 immunohistochemistry and TP53 mutational analysis?

Author

Salmon, Alixe, primary, Dheur, Adriane, additional, Bours, Vincent, additional, Delbecque, Katty, additional, Gonne, Élodie, additional, Pleyers, Clémence, additional, Cuypere, Marjolein De, additional, Goffin, Frédéric, additional, Lovinfosse, Pierre, additional, Kakkos, Athanasios, additional, Kridelka, Frédéric, additional, and Gennigens, Christine, additional

Published
2022
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40. EP107/#235 Defining prognostic risk groups amongst patients with endometrial cancer: respective role of 2009 FIGO stage and molecular profile

Author

Dheur, Adriane, primary, Bours, Vincent, additional, Cuypere, Marjolein De, additional, Delbecque, Katty, additional, Gennigens, Christine, additional, Goffin, Frédéric, additional, Gonne, Élodie, additional, Hermesse, Johanne, additional, Kakkos, Athanasios, additional, Lovinfosse, Pierre, additional, Pleyers, Clémence, additional, Salmon, Alixe, additional, and Kridelka, Frédéric, additional

Published
2022
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41. Two Years of Genomic Surveillance in Belgium during the SARS-CoV-2 Pandemic to Attain Country-Wide Coverage and Monitor the Introduction and Spread of Emerging Variants

Author

COVID-19 Genomics Belgium Consortium, Cuypers, Lize, Dellicour, Simon, Hong, Samuel L, Potter, Barney I, Verhasselt, Bruno, Vereecke, Nick, Lambrechts, Laurens, Durkin, Keith, Bours, Vincent, Klamer, Sofieke, Bayon-Vicente, Guillaume, Vael, Carl, Ariën, Kevin K, De Mendonca, Ricardo, Soetens, Oriane, Michel, Charlotte, Bearzatto, Bertrand, Naesens, Reinout, Gras, Jeremie, Vankeerberghen, Anne, Matheeussen, Veerle, Martens, Geert, Obbels, Dagmar, Lemmens, Ann, Van den Poel, Bea, Van Even, Ellen, De Rauw, Klara, Waumans, Luc, Reynders, Marijke, Degosserie, Jonathan, Maes, Piet, André, Emmanuel, Baele, Guy, Department of Bio-engineering Sciences, Supporting clinical sciences, Microbiology and Infection Control, Clinical Biology, Department of Clinical Microbiology, Faculty of Physical Education and Physical Therapy, Diabetes Pathology & Therapy, UCL - SSS/IREC/MONT - Pôle Mont Godinne, UCL - (MGD) Laboratoire de biologie clinique, and COVID-19 Genomics Belgium Consortium

Subjects
SARS-CoV-2, Biology and Life Sciences, COVID-19, High-Throughput Nucleotide Sequencing, Genomics, Genome, Viral, variants of concern, genomic surveillance, Infectious Diseases, Belgium, SARS-CoV-2/genetics, Virology, Medicine and Health Sciences, genomics, Humans, next-generation sequencing, Human medicine, Belgium/epidemiology, Pandemics, COVID-19/epidemiology
Abstract

An adequate SARS-CoV-2 genomic surveillance strategy has proven to be essential for countries to obtain a thorough understanding of the variants and lineages being imported and successfully established within their borders. During 2020, genomic surveillance in Belgium was not structurally implemented but performed by individual research laboratories that had to acquire the necessary funds themselves to perform this important task. At the start of 2021, a nationwide genomic surveillance consortium was established in Belgium to markedly increase the country's genomic sequencing efforts (both in terms of intensity and representativeness), to perform quality control among participating laboratories, and to enable coordination and collaboration of research projects and publications. We here discuss the genomic surveillance efforts in Belgium before and after the establishment of its genomic sequencing consortium, provide an overview of the specifics of the consortium, and explore more details regarding the scientific studies that have been published as a result of the increased number of Belgian SARS-CoV-2 genomes that have become available. ispartof: VIRUSES-BASEL vol:14 issue:10 ispartof: location:Switzerland status: published

Published
2022

42. Red blood cell alloimmunisation in sickle cell disease patients in the Democratic Republic of the Congo

Author

Kambale‐Kombi, Paul, primary, Djang'eing'a, Roland Marini, additional, Alworong'a Opara, Jean‐Pierre, additional, Minon, Jean‐Marc, additional, Sepulchre, Edith, additional, Bours, Vincent, additional, Floch, Aline, additional, Pirenne, France, additional, Tshilumba, Charles Kayembe, additional, and Batina‐Agasa, Salomon, additional

Published
2022
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43. Two Years of Genomic Surveillance in Belgium during the SARS-CoV-2 Pandemic to Attain Country-Wide Coverage and Monitor the Introduction and Spread of Emerging Variants

Author

Cuypers, Lize, primary, Dellicour, Simon, additional, Hong, Samuel L., additional, Potter, Barney I., additional, Verhasselt, Bruno, additional, Vereecke, Nick, additional, Lambrechts, Laurens, additional, Durkin, Keith, additional, Bours, Vincent, additional, Klamer, Sofieke, additional, Bayon-Vicente, Guillaume, additional, Vael, Carl, additional, Ariën, Kevin K., additional, De Mendonca, Ricardo, additional, Soetens, Oriane, additional, Michel, Charlotte, additional, Bearzatto, Bertrand, additional, Naesens, Reinout, additional, Gras, Jeremie, additional, Vankeerberghen, Anne, additional, Matheeussen, Veerle, additional, Martens, Geert, additional, Obbels, Dagmar, additional, Lemmens, Ann, additional, Van den Poel, Bea, additional, Van Even, Ellen, additional, De Rauw, Klara, additional, Waumans, Luc, additional, Reynders, Marijke, additional, Degosserie, Jonathan, additional, Maes, Piet, additional, André, Emmanuel, additional, and Baele, Guy, additional

Published
2022
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44. Reconstruction of SARS-CoV-2 outbreaks in a primary school using epidemiological and genomic data

Author

Kremer, Cécile, primary, Torneri, Andrea, additional, Libin, Pieter J. K., additional, Meex, Cécile, additional, Hayette, Marie-Pierre, additional, Bontems, Sébastien, additional, Durkin, Keith, additional, Artesi, Maria, additional, Bours, Vincent, additional, Lemey, Philippe, additional, Darcis, Gilles, additional, Hens, Niel, additional, and Meuris, Christelle, additional

Published
2022
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45. 2022-RA-193-ESGO Cost-effectiveness of molecular profiling for endometrial neoplasia: a single institution experience

Author

Dheur, Adriane, primary, Bours, Vincent, additional, De Cuypere, Marjolein, additional, Delbecque, Katty, additional, Gennigens, Christine, additional, Goffin, Frédéric, additional, Gonne, Elodie, additional, Hermesse, Johanne, additional, Kridelka, Frédéric, additional, Lovinfosse, Pierre, additional, Pleyers, Clémence, additional, Salmon, Alixe, additional, and Kakkos, Athanasios, additional

Published
2022
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46. 2022-RA-967-ESGO Endometrial cancer: agreement between microsatellite instability in immunohistochemistry and molecular biology?

Author

Gennigens, Christine, primary, Dheur, Adriane, additional, Bours, Vincent, additional, Delbecque, Katty, additional, Gonne, Elodie, additional, Pleyers, Clemence, additional, Seidel, Laurence, additional, Streel, Sylvie, additional, de Cuypere, Marjolein, additional, Goffin, Frederic, additional, Lovinfosse, Pierre, additional, Kakkos, Athanasios, additional, Kridelka, Frederic, additional, and Salmon, Alixe, additional

Published
2022
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47. 2022-RA-955-ESGO Endometrial cancer: lymphovascular space invasion is a negative prognostic factor

Author

Salmon, Alixe, primary, Dheur, Adriane, additional, Bours, Vincent, additional, Delbecque, Katty, additional, Gonne, Elodie, additional, Pleyers, Clemence, additional, de Cuypere, Marjolein, additional, Goffin, Frederic, additional, Lovinfosse, Pierre, additional, Kridelka, Frederic, additional, Kakkos, Athanasios, additional, and Gennigens, Christine, additional

Published
2022
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48. Coinheritance of pathogenic variants in ATM and BRCA2 in families with multiple cancers: a case series

Author

Freire, Maria Valeria, primary, Martin, Marie, additional, Segers, Karin, additional, Sepulchre, Edith, additional, Leroi, Natacha, additional, Kalantari, Hassan, additional, Wolter, Pascal, additional, Collignon, Joëlle, additional, Polus, Marc, additional, Plomteux, Olivier, additional, Josse, Claire, additional, and Bours, Vincent, additional

Published
2022
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