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1. Circulating inflammatory cytokines predict severity disease in hospitalized COVID-19 patients: A prospective multicenter study of the European DRAGON consortium

Author

Polese, Barbara, Ernst, Marie, Henket, Monique, Ernst, Benoit, Winandy, Marie, Njock, Makon-Sébastien, Blockx, Céline, Kovacs, Stéphanie, Watar, Florence, Peired, Anna Julie, Tomassetti, Sara, Nardi, Cosimo, Gofflot, Stéphanie, Rahmouni, Souad, Schofield, James PR, Penrice-Randal, Rebekah, Skipp, Paul J., Strazzeri, Fabio, Parkinson, Erika, Darcis, Gilles, Misset, Benoit, Moutschen, Michel, Louis, Renaud, Cavalier, Etienne, and Guiot, Julien

Published
2024
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3. Genetic diversity of Echinococcus multilocularis specimens isolated from Belgian patients with alveolar echinococcosis using EmsB microsatellites analysis

Author

Sacheli, Rosalie, Knapp, Jenny, Pholien, Caroline, Egrek, Sabrina, Léonard, Philippe, Giot, Jean-Baptiste, Delaere, Bénédicte, Blétard, Noella, Gofflot, Stéphanie, Nollevaux, Marie-Cécile, Meunier, Paul, Lovinfosse, Pierre, Pirotte, Benoit, Truyens, Carine, Millon, Laurence, Detry, Olivier, and Hayette, Marie-Pierre

Published
2023
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4. Fibroblast-derived prolargin is a tumor suppressor in hepatocellular carcinoma

Author

Chiavarina, Barbara, Ronca, Roberto, Otaka, Yukihiro, Sutton, Roger Bryan, Rezzola, Sara, Yokobori, Takehiko, Chiodelli, Paola, Souche, Regis, Pourquier, Didier, Maraver, Antonio, Faa, Gavino, Khellaf, Lakhdar, Turtoi, Evgenia, Oyama, Tetsunari, Gofflot, Stephanie, Bellahcène, Akeila, Detry, Olivier, Delvenne, Philippe, Castronovo, Vincent, Nishiyama, Masahiko, and Turtoi, Andrei

Published
2022
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5. Surveillance of effects of HPV vaccination in Belgium

Author

Arbyn, Marc, Broeck, Davy Vanden, Benoy, Ina, Bogers, Johannes, Depuydt, Christophe, Praet, Marleen, Sutter, Philippe De, Hoorens, Anne, Hauben, Esther, Poppe, Willy, Ranst, Marc Van, Delvenne, Philippe, Gofflot, Stephanie, Pétein, Michel, Engelen, Frans, Vanneste, Alain, Beeck, Lode Op De, Damme, Pierre Van, Temmerman, Marleen, and Weyers, Steven

Published
2016
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6. Evaluation of Screening Program and Phylogenetic Analysis of SARS-CoV-2 Infections among Hospital Healthcare Workers in Liège, Belgium

Author

El Moussaoui, Majdouline, Maes, Nathalie, Hong, Samuel S.L., Lambert, Nicolas, Gofflot, Stephanie, Dellot, Patricia, Belhadj, Yasmine, Huynen, Pascale, Hayette, Marie-Pierre, Meex, Cécile, Bontems, Sébastien, Defêche, Justine, Godderis, Lode, Molenberghs, Geert, Meuris, Christelle C.M., Artesi, Maria, Durkin, Keith, Rahmouni, Souad, Grégoire, Céline, Beguin, Yves, Moutschen, Michel, Dellicour, Simon, Darcis, Gilles, El Moussaoui, Majdouline, Maes, Nathalie, Hong, Samuel S.L., Lambert, Nicolas, Gofflot, Stephanie, Dellot, Patricia, Belhadj, Yasmine, Huynen, Pascale, Hayette, Marie-Pierre, Meex, Cécile, Bontems, Sébastien, Defêche, Justine, Godderis, Lode, Molenberghs, Geert, Meuris, Christelle C.M., Artesi, Maria, Durkin, Keith, Rahmouni, Souad, Grégoire, Céline, Beguin, Yves, Moutschen, Michel, Dellicour, Simon, and Darcis, Gilles

Abstract

Healthcare workers (HCWs) are known to be at higher risk of developing severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infections although whether these risks are equal across all occupational roles is uncertain. Identifying these risk factors and understand SARS-CoV-2 transmission pathways in healthcare settings are of high importance to achieve optimal protection measures. We aimed to investigate the implementation of a voluntary screening program for SARS-CoV-2 infections among hospital HCWs and to elucidate potential transmission pathways though phylogenetic analysis before the vaccination era. HCWs of the University Hospital of Liège, Belgium, were invited to participate in voluntary reverse transcriptase-polymerase chain reaction (RT-PCR) assays performed every week from April to December 2020. Phylogenetic analysis of SARS-CoV-2 genomes were performed for a subgroup of 45 HCWs. 5095 samples were collected from 703 HCWs. 212 test results were positive, 15 were indeterminate, and 4868 returned negative. 156 HCWs (22.2%) tested positive at least once during the study period. All SARS-CoV-2 test results returned negative for 547 HCWs (77.8%). Nurses (p < 0.05), paramedics (p < 0.05), and laboratory staff handling respiratory samples (p < 0.01) were at higher risk for being infected compared to the control non-patient facing group. Our phylogenetic analysis revealed that most positive samples corresponded to independent introduction events into the hospital. Our findings add to the growing evidence of differential risks of being infected among HCWs and support the need to implement appropriate protection measures based on each individual’s risk profile to guarantee the protection of both HCWs and patients. Furthermore, our phylogenetic investigations highlight that most positive samples correspond to distinct introduction events into the hospital., SCOPUS: ar.j, info:eu-repo/semantics/published

Published
2022

7. Metastatic colorectal cancer cells maintain the TGFβ program and use TGFBI to fuel angiogenesis

Author

Chiavarina, Barbara, Costanza, Brunella, Ronca, Roberto, Blomme, Arnaud, Rezzola, Sara, Chiodelli, Paola, Giguelay, Ambre, Belthier, Guillame, Doumont, Gilles, Van Simaeys, Gaëtan, Lacroix, Simon, Yokobori, Takehiko, Erkhem-Ochir, Bilguun, Balaguer, Patrick, Cavailles, Vincent, Fabbrizio, Eric, Di Valentin, Emmanuel, Gofflot, Stephanie, Detry, Olivier, Jerusalem, Guy, Goldman, Serge, Delvenne, Philippe O, Bellahcène, Akeila, Pannequin, Julie, Castronovo, Vincent, Turtoi, Andrei, Chiavarina, Barbara, Costanza, Brunella, Ronca, Roberto, Blomme, Arnaud, Rezzola, Sara, Chiodelli, Paola, Giguelay, Ambre, Belthier, Guillame, Doumont, Gilles, Van Simaeys, Gaëtan, Lacroix, Simon, Yokobori, Takehiko, Erkhem-Ochir, Bilguun, Balaguer, Patrick, Cavailles, Vincent, Fabbrizio, Eric, Di Valentin, Emmanuel, Gofflot, Stephanie, Detry, Olivier, Jerusalem, Guy, Goldman, Serge, Delvenne, Philippe O, Bellahcène, Akeila, Pannequin, Julie, Castronovo, Vincent, and Turtoi, Andrei

Abstract

Colorectal cancer (CRC) cells are traditionally considered unresponsive to TGFβ due to mutations in the receptors and/or downstream signaling molecules. TGFβ influences CRC cells only indirectly via stromal cells, such as cancer-associated fibroblasts. However, CRC cell ability to directly respond to TGFβ currently remains unexplored. This represents a missed opportunity for diagnostic and therapeutic interventions. Methods: We examined whether cancer cells from primary CRC and liver metastases respond to TGFβ by inducing TGFβ-induced protein ig-h3 (TGFBI) expression, and the contribution of canonical and non-canonical TGFβ signaling pathways to this effect. We then investigated in vitro and in vivo TGFBI impact on metastasis formation and angiogenesis. Using patient serum samples and an orthotopic mouse model of CRC liver metastases we assessed the diagnostic/tumor targeting value of novel antibodies against TGFBI. Results: Metastatic CRC cells, such as circulating tumor cells, directly respond to TGFβ. These cells were characterized by the absence of TGFβ receptor mutations and the frequent presence of p53 mutations. The pro-tumorigenic program orchestrated by TGFβ in CRC cells was mediated through TGFBI, the expression of which was positively regulated by non-canonical TGFβ signaling cascades. TGFBI inhibition was sufficient to significantly reduce liver metastasis formation in vivo. Moreover, TGFBI pro-tumorigenic function was linked to its ability to stimulate angiogenesis. TGFBI levels were higher in serum samples from untreated patients with CRC than in patients who were receiving chemotherapy. A radiolabeled anti-TGFBI antibody selectively targeted metastatic lesions in vivo, underscoring its diagnostic and therapeutic potential. Conclusions: TGFβ signaling in CRC cells directly contributes to their metastatic potential and stromal cell-independence. Proteins downstream of activated TGFβ, such as TGFBI, represent novel diagnostic and therapeutic targets for, SCOPUS: ar.j, info:eu-repo/semantics/published

Published
2021

9. Pretreatment of adult bone marrow mesenchymal stem cells with cardiomyogenic growth factors and repair of the chronically infarcted myocardium

Author

Bartunek, Jozef, Croissant, Jeffrey D., Wijns, William, Gofflot, Stephanie, de Lavareille, Aurore, Vanderheyden, Marc, Kaluzhny, Yulia, Mazouz, Naima, Willemsen, Philippe, Penicka, Martin, Mathieu, Myrielle, Homsy, Christian, De Bruyne, Bernard, McEntee, Kathleen, Lee, Ike W., and Heyndrickx, Guy R.

Subjects
Hematopoietic stem cells -- Research, Heart attack -- Research, Biological sciences
Abstract

The in vivo cardiac differentiation and functional effects of unmodified adult bone marrow mesenchymal stem cells (MSCs) after myocardial infarction (MI) is controversial. We postulated that ex vivo pretreatment of autologous MSCs using cardiomyogenic growth factors will lead to cardiomyogenic specification and will result in superior biological and functional effects on cardiac regeneration of chronically infarcted myocardium. We used a chronic dog MI model generated by ligation of the coronary artery (n = 30). Autologous dog bone marrow MSCs were isolated, culture expanded, and specified into a cardiac lineage by adding growth factors, including basic FGF, IGF-1, and bone morphogenetic protein-2. Dogs underwent cell injection >8 wk after the infarction and were randomized into two groups. Group A dogs (n = 20) received MSCs specified with growth factors (147 [+ or -] 96 x [10.sup.6]), and group B (n = 10) received unmodified MSCs (168 [+ or -] 24 x [10.sup.6]). After the growth factor treatment, MSCs stained positive for the early muscle and cardiac markers desmin, antimyocyte enhancer factor-2, and Nkx2-5. In group A dogs, prespecified MSCs colocalized with troponin I and cardiac myosin. At 12 wk, group A dogs showed a significantly larger increase in regional wall thickening of the infarcted territory (from 22 [+ or -] 8 to 32 [+ or -] 6% in group A; P < 0.05 vs. baseline and group B, and from 19 [+ or -] 7 to 21 [+ or -] 7% in group B, respectively) and a decrease in the wall motion score index (from 1.60 [+ or -] 0.05 to 1.35 [+ or -] 0.03 in group A; P < 0.05 vs. baseline and group B, and from 1.58 [+ or -] 0.07 vs. 1.56 [+ or -] 0.08 in group B, respectively). The biological ex vivo cardiomyogenic specification of adult MSCs before their transplantation is feasible and appears to improve their in vivo cardiac differentiation as well as the functional recovery in a dog model of the chronically infarcted myocardium. cardiac repair; myogenesis; chronic myocardial infarction; heart failure

Published
2007

10. Tumor-Antagonizing Fibroblasts Secrete Prolargin as Tumor Suppressor in Hepatocellular Carcinoma

Author

Chiavarina, Barbara, primary, Ronca, Roberto, additional, Otaka, Yukihiro, additional, Sutton, Roger Bryan, additional, Rezzola, Sara, additional, Yokobori, Takehiko, additional, Chiodelli, Paola, additional, Souche, Regis, additional, Maraver, Antonio, additional, Faa, Gavino, additional, Oyama, Tetsunari, additional, Gofflot, Stephanie, additional, Bellahcène, Akeila, additional, Detry, Olivier, additional, Delvenne, Philippe, additional, Castronovo, Vincent, additional, Nishiyama, Masahiko, additional, and Turtoi, Andrei, additional

Published
2021
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11. Metastatic colorectal cancer cells maintain the TGFβ program and use TGFBI to fuel angiogenesis

Author

Chiavarina, Barbara, primary, Costanza, Brunella, additional, Ronca, Roberto, additional, Blomme, Arnaud, additional, Rezzola, Sara, additional, Chiodelli, Paola, additional, Giguelay, Ambre, additional, Belthier, Guillame, additional, Doumont, Gilles, additional, Van Simaeys, Gaetan, additional, Lacroix, Simon, additional, Yokobori, Takehiko, additional, Erkhem-Ochir, Bilguun, additional, Balaguer, Patrick, additional, Cavailles, Vincent, additional, Fabbrizio, Eric, additional, Di Valentin, Emmanuel, additional, Gofflot, Stephanie, additional, Detry, Olivier, additional, Jerusalem, Guy, additional, Goldman, Serge, additional, Delvenne, Philippe, additional, Bellahcène, Akeila, additional, Pannequin, Julie, additional, Castronovo, Vincent, additional, and Turtoi, Andrei, additional

Published
2021
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12. Asporin is a fibroblast-derived TGF-β1 inhibitor and a tumor suppressor associated with good prognosis in breast cancer

Author

Maris, Pamela, Blomme, Arnaud, Palacios, Ana Perez, Costanza, Brunella, Bellahcene, Akeila, Bianchi, Elettra, Gofflot, Stephanie, Drion, Pierre, Trombino, Giovanna Elvi, Di Valentin, Emmanuel, Cusumano, Pino G., Maweja, Sylvie, Jerusalem, Guy, Delvenne, Philippe, Lifrange, Eric, Castronovo, Vincent, and Turtoi, Andrei

Subjects
Transforming growth factors -- Health aspects -- Genetic aspects, Breast cancer -- Genetic aspects -- Prognosis, Biological sciences
Abstract

Background Breast cancer is a leading malignancy affecting the female population worldwide. Most morbidity is caused by metastases that remain incurable to date. TGF-β1 has been identified as a key driving force behind metastatic breast cancer, with promising therapeutic implications. Methods and Findings Employing immunohistochemistry (IHC) analysis, we report, to our knowledge for the first time, that asporin is overexpressed in the stroma of most human breast cancers and is not expressed in normal breast tissue. In vitro, asporin is secreted by breast fibroblasts upon exposure to conditioned medium from some but not all human breast cancer cells. While hormone receptor (HR) positive cells cause strong asporin expression, triple-negative breast cancer (TNBC) cells suppress it. Further, our findings show that soluble IL-1β, secreted by TNBC cells, is responsible for inhibiting asporin in normal and cancer-associated fibroblasts. Using recombinant protein, as well as a synthetic peptide fragment, we demonstrate the ability of asporin to inhibit TGF-β1-mediated SMAD2 phosphorylation, epithelial to mesenchymal transition, and stemness in breast cancer cells. In two in vivo murine models of TNBC, we observed that tumors expressing asporin exhibit significantly reduced growth (2-fold; p = 0.01) and metastatic properties (3-fold; p = 0.045). A retrospective IHC study performed on human breast carcinoma (n = 180) demonstrates that asporin expression is lowest in TNBC and HER2+ tumors, while HR+ tumors have significantly higher asporin expression (4-fold; p = 0.001). Assessment of asporin expression and patient outcome (n = 60; 10-y follow-up) shows that low protein levels in the primary breast lesion significantly delineate patients with bad outcome regardless of the tumor HR status (area under the curve = 0.87; 95% CI 0.78-0.96; p = 0.0001). Survival analysis, based on gene expression (n = 375; 25-y follow-up), confirmed that low asporin levels are associated with a reduced likelihood of survival (hazard ratio = 0.58; 95% CI 0.37-0.91; p = 0.017). Although these data highlight the potential of asporin to serve as a prognostic marker, confirmation of the clinical value would require a prospective study on a much larger patient cohort. Conclusions Our data show that asporin is a stroma-derived inhibitor of TGF-β1 and a tumor suppressor in breast cancer. High asporin expression is significantly associated with less aggressive tumors, stratifying patients according to the clinical outcome. Future pre-clinical studies should consider options for increasing asporin expression in TNBC as a promising strategy for targeted therapy., Introduction The tumor stroma, and especially cancer-associated fibroblasts (CAFs), is emerging as a key element of cancer growth and metastasis. CAFs supply cancer cells with a plethora of growth factors, [...]

Published
2015
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13. A specific immune and lymphatic profile characterizes the pre-metastatic state of the sentinel lymph node in patients with early cervical cancer.

Author

Balsat, Cédric, Blacher, Silvia, Herfs, Michael, Van de Velde, Maureen, Signolle, Nicolas, Sauthier, Philippe, Pottier, Charles, Gofflot, Stephanie, De Cuypere, Marjolein, Delvenne, Philippe, Goffin, Frédéric, Noël, Agnès, Kridelka, Frederic, Balsat, Cédric, Blacher, Silvia, Herfs, Michael, Van de Velde, Maureen, Signolle, Nicolas, Sauthier, Philippe, Pottier, Charles, Gofflot, Stephanie, De Cuypere, Marjolein, Delvenne, Philippe, Goffin, Frédéric, Noël, Agnès, and Kridelka, Frederic

Abstract

The lymph node (LN) pre-metastatic niche is faintly characterized in lymphophilic human neoplasia, although LN metastasis is considered as the strongest prognostic marker of patient survival. Due to its specific dissemination through a complex bilateral pelvic lymphatic system, early cervical cancer is a relevant candidate for investigating the early nodal metastatic process. In the present study, we analyzed in-depth both the lymphatic vasculature and the immune climate of pre-metastatic sentinel LN (SLN), in 48 cases of FIGO stage IB1 cervical neoplasms. An original digital image analysis methodology was used to objectively determine whole slide densities and spatial distributions of immunostained structures. We observed a marked increase in lymphatic vessel density (LVD) and a specific capsular and subcapsular distribution in pre-metastatic SLN when compared with non-sentinel counterparts. Such features persisted in the presence of nodal metastatic colonization. The inflammatory profile attested by CD8(+), Foxp3, CD20 and PD-1expression was also significantly increased in pre-metastatic SLN. Remarkably, the densities of CD20(+) B cells and PD-1 expressing germinal centers were positively correlated with LVD. All together, these data strongly support the existence of a pre-metastatic dialog between the primary tumor and the first nodal relay. Both lymphatic and immune responses contribute to the elaboration of a specific pre-metastatic microenvironment in human SLN. Moreover, this work provides evidence that, in the context of early cervical cancer, a pre-metastatic lymphangiogenesis occurs within the SLN (pre-metastatic niche) and is associated with a specific humoral immune response., info:eu-repo/semantics/published

Published
2017

14. Myoferlin regulates cellular lipid metabolism and promotes metastases in triple-negative breast cancer.

Author

Blomme, Adrien, Costanza, B, de Tullio, Pascal, Thiry, M., Van Simaeys, Gaëtan, Boutry, Sébastien, Doumont, Gilles, Di Valentin, E, Hirano, T, Yokobori, T, Gofflot, Stephanie, Peulen, Olivier, Bellahcene, Akeila, Sherer, Félicie, Le Goff, Carine, Cavalier, E, Mouithys-Mickalad, Ange, Jouret, François, Cusumano, P G, Lifrange, E, Muller, Robert N, Goldman, Serge, Delvenne, P, De Pauw, E, Nishiyama, M, Castronovo, V., Turtoi, Andrei, Blomme, Adrien, Costanza, B, de Tullio, Pascal, Thiry, M., Van Simaeys, Gaëtan, Boutry, Sébastien, Doumont, Gilles, Di Valentin, E, Hirano, T, Yokobori, T, Gofflot, Stephanie, Peulen, Olivier, Bellahcene, Akeila, Sherer, Félicie, Le Goff, Carine, Cavalier, E, Mouithys-Mickalad, Ange, Jouret, François, Cusumano, P G, Lifrange, E, Muller, Robert N, Goldman, Serge, Delvenne, P, De Pauw, E, Nishiyama, M, Castronovo, V., and Turtoi, Andrei

Abstract

Myoferlin is a multiple C2-domain-containing protein that regulates membrane repair, tyrosine kinase receptor function and endocytosis in myoblasts and endothelial cells. Recently it has been reported as overexpressed in several cancers and shown to contribute to proliferation, migration and invasion of cancer cells. We have previously demonstrated that myoferlin regulates epidermal growth factor receptor activity in breast cancer. In the current study, we report a consistent overexpression of myoferlin in triple-negative breast cancer cells (TNBC) over cells originating from other breast cancer subtypes. Using a combination of proteomics, metabolomics and electron microscopy, we demonstrate that myoferlin depletion results in marked alteration of endosomal system and metabolism. Mechanistically, myoferlin depletion caused impaired vesicle traffic that led to a misbalance of saturated/unsaturated fatty acids. This provoked mitochondrial dysfunction in TNBC cells. As a consequence of the major metabolic stress, TNBC cells rapidly triggered AMP activated protein kinase-mediated metabolic reprogramming to glycolysis. This reduced their ability to balance between oxidative phosphorylation and glycolysis, rendering TNBC cells metabolically inflexible, and more sensitive to metabolic drug targeting in vitro. In line with this, our in vivo findings demonstrated a significantly reduced capacity of myoferlin-deficient TNBC cells to metastasise to lungs. The significance of this observation was further supported by clinical data, showing that TNBC patients whose tumors overexpress myoferlin have worst distant metastasis-free and overall survivals. This novel insight into myoferlin function establishes an important link between vesicle traffic, cancer metabolism and progression, offering new diagnostic and therapeutic concepts to develop treatments for TNBC patients.Oncogene advance online publication, 24 October 2016; doi:10.1038/onc.2016.369., SCOPUS: ar.j, info:eu-repo/semantics/published

Published
2016

15. The flowing afterglow of the N2-O2 discharge as a means of decontaminating/sterilising through UV irradiation: Summary of the research achieved and recent results.

Author

Moisan, Michel, Levif, Pierre, Seguin, Jacynthe, Barbeau, Jean, Leduc, Annie, Elmoualij, Benaissa, Gofflot, Stephanie, Heinen, Ernst, Thellin, Olivier, and Zorzi, Willy

Abstract

The plasma systems for disinfection/sterilization that we have been working on are mainly based on UV irradiation while most plasma “sterilisers” are calling on ions and radicals. In the latter case, inactivation generally proceeds from erosion of the microorganisms while, in the former case, the UV photons create enough lesions to the DNA genetic material to prevent its repair. Inactivation of microorganisms through UV photons in the afterglow is, however, much slower than in the discharge itself. The UV photons stem from NO excited molecules, which are generated following the interaction of N and O atoms, in the flowing afterglow, which are coming from the dissociation of N2 and O2 in the (microwave) discharge. Since the N and O atoms can diffuse into crevices before joining into NO molecules, there is no limited accessibility of the UV photons as with a UV lamp. The NOγ molecular system shows band heads that cover almost continuously the 180–350 nm range. [ABSTRACT FROM PUBLISHER]

Published
2012
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