Your search keyword '"Lehours, Philippe"' showing total 17 results

1. Targeting metastasis-initiating cancer stem cells in gastric cancer with leukaemia inhibitory factor.

Author

Seeneevassen, Lornella, Zaafour, Anissa, Sifré, Elodie, Genevois, Coralie, Nguyen, Tra Ly, Pobiedonoscew, Yasmine, Giese, Alban, Guignard, Jérôme, Tiffon, Camille, Rousseau, Benoit, Raymond, Anne-Aurélie, Belleannée, Geneviève, Boeuf, Hélène, Gronnier, Caroline, Martin, Océane C. B., Giraud, Julie, Lehours, Philippe, Dubus, Pierre, and Varon, Christine

Published

2024

2. RIDA®GENE Helicobacter pylori PCR on the ELITe InGenius System.

Author

Bénéjat, Lucie, Ducournau, Astrid, Martins, Chloé Domingues, Bessède, Emilie, and Lehours, Philippe

Subjects

HELICOBACTER pylori, HELICOBACTER pylori infections, BACTERIAL mutation

Abstract

PCR detection of Helicobacter pylori infection in gastric biopsies allows the detection of this bacterium and the mutations associated with macrolide resistance. The aim of this study was to evaluate the performance of RIDA®GENE H. pylori PCR (r-Biopharm) on the ELITe InGenius System (Elitech). Two hundred gastric biopsies were obtained. These biopsies were ground in nutrient broth. Two hundred microliters of this suspension was treated with proteinase K, and then, 200 µL was transferred to an ELITe InGenius sample tube and tested using RIDA®GENE H. pylori PCR reagents. In-house H. pylori PCR was used as a reference. The sensitivity of RIDA®GENE H. pylori PCR with ELITe InGenius was 100%, the specificity was 98% (95% confidence interval (CI), 95.3–100%), the PPV was 98% (95% CI, 95.3–100%), and the NPV was 100% for the detection of H. pylori. All of these parameters were 100% for the categorization of macrolide resistance. The adaptation of RIDA®GENE H. pylori PCR reagents on the ELITe InGenius System was successful. This PCR is easy to use on this system. [ABSTRACT FROM AUTHOR]

Published

2023

3. CD44v3 is a marker of invasive cancer stem cells driving metastasis in gastric carcinoma.

Author

Giraud, Julie, Seeneevassen, Lornella, Rousseau, Benoit, Bouriez, Damien, Sifré, Elodie, Giese, Alban, Nguyen, Tra Ly, Tiffon, Camille, Lippi, Yannick, Azzi-Martin, Lamia, Pannequin, Julie, Ménard, Armelle, Bessède, Emilie, Staedel, Cathy, Mégraud, Francis, Belleannée, Geneviève, Lehours, Philippe, Gronnier, Caroline, Dubus, Pierre, and Varon, Christine

Subjects

CANCER stem cells, CANCER invasiveness, STOMACH cancer, TUMOR markers, PRECANCEROUS conditions

Abstract

Background: Cancer stem cells (CSCs) are at the origin of tumour initiation and progression in gastric adenocarcinoma (GC). However, markers of metastasis-initiating cells remain unidentified in GC. In this study, we characterized CD44 variants expressed in GC and evaluated the tumorigenic and metastatic properties of CD44v3+ cells and their clinical significance in GC patients. Methods: Using GC cell lines and patient-derived xenografts, we evaluated CD44+ and CD44v3+ GC cells molecular signature and their tumorigenic, chemoresistance, invasive and metastatic properties, and expression in patients-derived tissues. Results: CD44v3+ cells, which represented a subpopulation of CD44+ cells, were detected in advanced preneoplastic lesions and presented CSCs chemoresistance and tumorigenic properties in vitro and in vivo. Molecular and functional analyses revealed two subpopulations of gastric CSCs: CD44v3+ CSCs with an epithelial-mesenchymal transition (EMT)-like signature, and CD44+/v3– CSCs with an epithelial-like signature; both were tumorigenic but CD44v3+ cells showed higher invasive and metastatic properties in vivo. CD44v3+ cells detected in the primary tumours of GC patients were associated with a worse prognosis. Conclusion: CD44v3 is a marker of a subpopulation of CSCs with metastatic properties in GC. The identification of metastasis-initiating cells in GC represents a major advance for further development of anti-metastatic therapeutic strategies. [ABSTRACT FROM AUTHOR]

Published

2023

4. Autophagy induced by Helicobacter pylori infection is necessary for gastric cancer stem cell emergence

Author

Ligue Nationale contre le Cancer (France), Courtois, Sarah, Haykal, Maria, Bodineau, Clément, Sifré, Elodie, Azzi-Martin, Lamia, Ménard, Armelle, Mégraud, Francis, Lehours, Philippe, Durán, Raúl V., Varon, Christine, Bessède, Emilie, Ligue Nationale contre le Cancer (France), Courtois, Sarah, Haykal, Maria, Bodineau, Clément, Sifré, Elodie, Azzi-Martin, Lamia, Ménard, Armelle, Mégraud, Francis, Lehours, Philippe, Durán, Raúl V., Varon, Christine, and Bessède, Emilie

Abstract

Background: The main cause of gastric cancer is the infection by the bacterium Helicobacter pylori which induces a chronic inflammation and an epithelial-to-mesenchymal transition (EMT) leading to the emergence of cells with cancer stem cell (CSC) properties. However, the underlying mechanisms have not been fully characterized. Moreover, H. pylori modulates the host cell autophagic process, but a few studies have investigated the role of this process in tumoral transformation. The aim of this study was to determine whether H. pylori-induced autophagy has a role in CSC emergence. Methods: Autophagic flux in response to H. pylori infection was characterized in AGS cell line expressing the tandem-tagged mCherry-GFP-LC3 protein and using a ratiometric flow cytometry analysis. Then, AGS and MKN45 cell lines were treated with bafilomycin or chloroquine, two pharmaceutical well-known inhibitors of autophagy, and different EMT and CSC characteristics were analyzed. Results: First, a co-expression of the gastric CSC marker CD44 and the autophagic marker LC3 in mice and human stomach tissues infected with H. pylori was observed. Then, we demonstrated in vitro that H. pylori was able to activate the autophagy process with a reduced autophagic flux. Finally, infected cells were treated with autophagy inhibitors, which reduced (i) appearance of mesenchymal phenotypes and migration ability related to EMT and (ii) CD44 expression as well as tumorsphere formation capacities reflecting CSC properties. Conclusion: In conclusion, all these data show that H. pylori-induced autophagy is implicated in gastric CSC emergence and could represent an interesting therapeutic target.

Published

2021

5. Automation of RIDA®GENE Helicobacter pylori PCR on the BD MAX™ System.

Author

Bénéjat, Lucie, Giese, Alban, Lescaudron, Zoé, Bonnac, Julien, Ducournau, Astrid, Bessède, Emilie, and Lehours, Philippe

Subjects

HELICOBACTER pylori, HELICOBACTER pylori infections, BACTERIAL mutation, AUTOMATION

Abstract

PCR detection of Helicobacter pylori infection in gastric biopsies allows the detection of this bacterium and the mutations associated with macrolide resistance. The aim of this study was to evaluate the performance of RIDA®GENE H. pylori PCR (r-Biopharm) on a BD MAX™ System (Becton Dickinson). Two hundred ten gastric biopsies obtained were included. These biopsies were ground in nutrient broth. Two hundred microliters of this suspension was treated with proteinase K; 200 µL was transferred to a BD MAX™ sample tube then tested using RIDA®GENE H. pylori PCR reagents. In-house H. pylori PCR was used as a reference. The sensitivity of RIDA®GENE H. pylori PCR with BD MAX™ was 100%, the specificity was 99.08% (95% confidence interval (CI), 97.21–100%), the PPV was 99.02% (95% CI, 97.09–100%), and the NPV was 100% for the detection of H. pylori. The sensitivity was 97.14% (95% CI, 93.87–100%), the specificity was 100%, the PPV was 100%, and the NPV was 98.48% (95% CI, 96.08–100%) for categorization of macrolides resistance. The adaptation of RIDA®GENE H. pylori PCR on the BD MAX™ System is of considerable interest for microbiologists who seek to establish this assay in their laboratories. [ABSTRACT FROM AUTHOR]

Published

2022

6. Leukaemia inhibitory factor in gastric cancer: friend or foe?

Author

Seeneevassen, Lornella, Martin, Océane C. B., Lehours, Philippe, Dubus, Pierre, and Varon, Christine

Subjects

STOMACH cancer, LEUKEMIA, CELLULAR signal transduction

Abstract

IL-6 family cytokine leukaemia inhibitory factor (LIF) study has deciphered a variety of effects, in physiology as well as pathology. Despite the sudden arousal in LIF interest in cancers, its study in the gastric cancer (GC) context has been put aside. Only few related studies can be found in literature, most of them investigating IL-6/STAT3 signalling in GC, and not the particular LIF/LIFRβ signalisation. LIF/LIFR has opposing effects depending on the signalling pathways involved. This review relates the pro- and anti-tumorigenic aspects of LIF/LIFR in GC, taking also into account facts from other types of cancer. A better understanding of these issues would undoubtedly help postulate interesting hypotheses and perspectives for future LIF/LIFR study and its use in GC therapies, where options tend to be limited in number and efficiency. [ABSTRACT FROM AUTHOR]

Published

2022

7. Autophagy induced by Helicobacter pylori infection is necessary for gastric cancer stem cell emergence.

Author

Courtois, Sarah, Haykal, Maria, Bodineau, Clément, Sifré, Elodie, Azzi-Martin, Lamia, Ménard, Armelle, Mégraud, Francis, Lehours, Philippe, Durán, Raúl V., Varon, Christine, and Bessède, Emilie

Subjects

HELICOBACTER pylori infections, CANCER stem cells, STOMACH cancer, AUTOPHAGY, EPITHELIAL-mesenchymal transition, H2 receptor antagonists

Abstract

Background: The main cause of gastric cancer is the infection by the bacterium Helicobacter pylori which induces a chronic inflammation and an epithelial-to-mesenchymal transition (EMT) leading to the emergence of cells with cancer stem cell (CSC) properties. However, the underlying mechanisms have not been fully characterized. Moreover, H. pylori modulates the host cell autophagic process, but a few studies have investigated the role of this process in tumoral transformation. The aim of this study was to determine whether H. pylori-induced autophagy has a role in CSC emergence. Methods: Autophagic flux in response to H. pylori infection was characterized in AGS cell line expressing the tandem-tagged mCherry-GFP-LC3 protein and using a ratiometric flow cytometry analysis. Then, AGS and MKN45 cell lines were treated with bafilomycin or chloroquine, two pharmaceutical well-known inhibitors of autophagy, and different EMT and CSC characteristics were analyzed. Results: First, a co-expression of the gastric CSC marker CD44 and the autophagic marker LC3 in mice and human stomach tissues infected with H. pylori was observed. Then, we demonstrated in vitro that H. pylori was able to activate the autophagy process with a reduced autophagic flux. Finally, infected cells were treated with autophagy inhibitors, which reduced (i) appearance of mesenchymal phenotypes and migration ability related to EMT and (ii) CD44 expression as well as tumorsphere formation capacities reflecting CSC properties. Conclusion: In conclusion, all these data show that H. pylori-induced autophagy is implicated in gastric CSC emergence and could represent an interesting therapeutic target. [ABSTRACT FROM AUTHOR]

Published

2021

8. The therapeutic potential of metformin in gastric cancer.

Author

Courtois, Sarah, Lehours, Philippe, and Bessède, Emilie

Subjects

*STOMACH cancer, *CANCER stem cells, *TYPE 2 diabetes, *CELL lines, *CANCER cells

Abstract

Metformin is a biguanide molecule used since 1957 to treat type 2 diabetes patients. In addition to its hypoglycemic effects, epidemiological studies have shown that metformin can be associated with a decrease in cancer development risk in diabetic populations. Thus, since 2005 this molecule is largely studied for its antitumoural properties in different types of cancer. The potential antitumoural effect of metformin in gastric cancer has been poorly studied. Here, we detailed the different described mechanisms implicated in the antitumoural effect of metformin in gastric cancer, from the signalling pathways to the functional effects on gastric cancer cell lines and gastric cancer stem cells. [ABSTRACT FROM AUTHOR]

Published

2019

9. Evaluation of RIDASCREEN® and RIDA®QUICK Helicobacter kits for Helicobacter pylori detection in stools.

Author

Bénéjat, Lucie, Buissonnière, Alice, Ducournau, Astrid, Mégraud, Francis, Bessède, Emilie, and Lehours, Philippe

Subjects

HELICOBACTER pylori, FECES, HELICOBACTER, HELICOBACTER pylori infections, BACTERIAL antigens, PYLORUS

Abstract

The diagnosis of Helicobacter pylori infection can be made by using noninvasive tests. The detection of bacterial antigens in stool samples is a technique proposed by some suppliers. The objective of this study was to evaluate retrospectively the performances of the commercially available RIDA®QUICK Helicobacter and RIDASCREEN® Helicobacter (R-Biopharm) kits in detecting H. pylori antigens in stool samples. A collection of 132 stools was used in this study: 94 stools obtained from H. pylori-negative patients and 38 stools from H. pylori-positive patients. The performances (sensitivity, specificity, positive predictive value (PPV), negative predictive value (NPV)) were evaluated for the RIDA®QUICK Helicobacter and RIDASCREEN® Helicobacter kits in comparison with real-time PCR results performed on gastric biopsies as well as culture. Discordant results, with respect to H. pylori status, were checked on the same day as the test by repeating the procedure. All of the readings concerning the RIDA®QUICK Helicobacter tests were concordant between 3 users, i.e., 94/94 negative tests and 34/38 positive tests. RIDASCREEN® Helicobacter tests were negative for all 94 H. pylori-negative samples and positive for 35/38 positive stools. Reading of the RIDA®QUICK Helicobacter tests was not a problem in routine practice. The RIDA®QUICK Helicobacter and RIDASCREEN® Helicobacter kits show good performances and can be included in the armamentarium of diagnostic tests for H. pylori infection. [ABSTRACT FROM AUTHOR]

Published

2020

10. Distinct Campylobacter fetus lineages adapted as livestock pathogens and human pathobionts in the intestinal microbiota.

Author

Iraola, Gregorio, Forster, Samuel C., Kumar, Nitin, Lehours, Philippe, Bekal, Sadjia, García-Peña, Francisco J., Paolicchi, Fernando, Morsella, Claudia, Hotzel, Helmut, Po-Ren Hsueh, Vidal, Ana, Lévesque, Simon, Wataru Yamazaki, Balzan, Claudia, Vargas, Agueda, Piccirillo, Alessandra, Chaban, Bonnie, Hill, Janet E., Betancor, Laura, and Collado, Luis

Subjects

GUT microbiome, CAMPYLOBACTER jejuni, FETUS, CAMPYLOBACTER, LIVESTOCK, EPIDEMIOLOGICAL research

Abstract

Campylobacter fetus is a venereal pathogen of cattle and sheep, and an opportunistic human pathogen. It is often assumed that C. fetus infection occurs in humans as a zoonosis through food chain transmission. Here we show that mammalian C. fetus consists of distinct evolutionary lineages, primarily associated with either human or bovine hosts. We use whole-genome phylogenetics on 182 strains from 17 countries to provide evidence that C. fetus may have originated in humans around 10,500 years ago and may have “jumped” into cattle during the livestock domestication period. We detect C. fetus genomes in 8% of healthy human fecal metagenomes, where the human-associated lineages are the dominant type (78%). Thus, our work suggests that C. fetus is an unappreciated human intestinal pathobiont likely spread by human to human transmission. This genome-based evolutionary framework will facilitate C. fetus epidemiology research and the development of improved molecular diagnostics and prevention schemes for this neglected pathogen. [ABSTRACT FROM AUTHOR]

Published

2017

11. Epidemiology of Helicobacter pylori and Mechanisms of Carcinogenesis.

Author

Lehours, Philippe, Bessède, Emilie, Mégraud, Francis, and Varon, Christine

Published

2015

12. A new kit to detect Campylobacter species in stool specimens: the Orion GenRead Campylobacter®.

Author

Buissonnière, Alice, Bénéjat, Lucie, Charron, Paul, Bessède, Emilie, Lehours, Philippe, Valdenaire, Guillaume, Richer, Olivier, and Mégraud, Francis

Subjects

CAMPYLOBACTER, POLYMERASE chain reaction, ENZYME-linked immunosorbent assay, MEDICAL care, INFANT diseases

Abstract

Campylobacter enteritis is the most frequent bacterial enteritis including in children. Its diagnosis suffers from the lack of sensitivity and delayed result of culture. Our aim was to test a new PCR-derived method for Campylobacter diagnosis in comparison to a composite reference. Patients presenting to the emergency ward of our hospital with enteric symptoms during the 2016 summer season were included. In addition to culture, an ELISA and an in-house real-time PCR were performed, as well as the new method (Orion GenRead Campylobacter) on all stool specimens. The composite reference used to consider a case positive for Campylobacter was either culture positive and in case of negative culture both the ELISA and real-time PCR positive. One hundred fifty patients were included, 64 being infants or children. There were 29 cases positive by the composite reference, with 19 of the 64 children (29.7%) and 10 of the 86 adults (11.6%). If performed alone, culture would have missed six cases. The Orion GenRead Campylobacter detected all the positives by the composite reference but also 12 cases negative by the composite reference (sensitivity 100%, specificity 90.1%). Given the characteristics of the new method, it can be used as a screening method for Campylobacter detection. [ABSTRACT FROM AUTHOR]

Published

2018

13. Gastric Carcinogenesis and Helicobacter pylori Infection.

Author

Varon, Christine, Mosnier, Jean-François, Lehours, Philippe, Matysiak-Budnik, Tamara, and Mégraud, Francis

Published

2009

14. Which test to use to detect Helicobacter pylori infection in patients with low-grade gastric mucosa-associated lymphoid tissue lymphoma?

Author

Lehours, Philippe, Ruskone-Fourmestraux, Agnès, Lavergne, Anne, Cantet, Franck, and Mégraud, Francis

Subjects

*HELICOBACTER pylori, *LYMPHOMAS

Abstract

Helicobacter pylori is involved in the pathogenesis of lymphoma of the gastric mucosa-associated lymphoid tissue (MALT). Because gastric MALT lymphoma is a rare disease, few studies comparing the accuracy of diagnostic tests in this group of patients have been carried out, and only a limited number of tests (essentially histological) were performed. The aim of our study was to compare the results of four different diagnostic methods used to detect H. pylori (histology, culture, polymerase chain reaction, and serology) in a prospective multicenter study. A patient was considered to be H. pylori positive if culture or histology was positive. During the period 1995–2000, a total of 90 patients with low-grade gastric MALT lymphoma were enrolled. Results for the four tests were available for 56 patients (62.2%). Among these patients, the four tests were concordant in 35 cases (62.5%), i.e., were positive in 19 cases (33.9%) and negative in 16 patients (17.8%). Histology (39/40 positive, 97.5%) and serology (38/40 positive, 95.0%) were the most sensitive tests. Polymerase chain reaction (PCR) and culture were positive in 52.5% and 50%, respectively. The cagA gene was detected in 47.4% of the strains. [Copyright &y& Elsevier]

Published

2003

15. APRIL-producing eosinophils are involved in gastric MALT lymphomagenesis induced by Helicobacter sp infection.

Author

Blosse, Alice, Peru, Sara, Levy, Michael, Marteyn, Benoit, Floch, Pauline, Sifré, Elodie, Giese, Alban, Prochazkova-Carlotti, Martine, Azzi Martin, Lamia, Dubus, Pierre, Mégraud, Francis, Ruskone Fournestraux, Agnès, Fabiani, Bettina, Copie Bergman, Christiane, Robe, Cyrielle, Hahne, Michael, Huard, Bertrand, and Lehours, Philippe

Subjects

CYTOKINES, MUCOSA-associated lymphoid tissue lymphoma, HELICOBACTER diseases, EOSINOPHILS, GASTRITIS, LABORATORY mice

Abstract

The roles of the inflammatory response and production of a proliferation-inducing ligand (APRIL) cytokine in gastric mucosa-associated lymphoid tissue (MALT) lymphomagenesis induced by Helicobacter species infection are not clearly understood. We characterized the gastric mucosal inflammatory response associated with gastric MALT lymphoma (GML) and identified APRIL-producing cells in two model systems: an APRIL transgenic mouse model of GML induced by Helicobacter infection (Tg-hAPRIL) and human gastric biopsy samples from Helicobacter pylori-infected GML patients. In the mouse model, polarization of T helper 1 (tbet), T helper 2 (gata3), and regulatory T cell (foxp3) responses was evaluated by quantitative PCR. In humans, a significant increase in april gene expression was observed in GML compared to gastritis. APRIL-producing cells were eosinophilic polynuclear cells located within lymphoid infiltrates, and tumoral B lymphocytes were targeted by APRIL. Together, the results of this study demonstrate that the Treg-balanced inflammatory environment is important for gastric lymphomagenesis induced by Helicobacter species, and suggest the pro-tumorigenic potential of APRIL-producing eosinophils. [ABSTRACT FROM AUTHOR]

Published

2020

16. Source attribution of Campylobacter jejuni shows variable importance of chicken and ruminants reservoirs in non-invasive and invasive French clinical isolates.

Author

Berthenet, Elvire, Thépault, Amandine, Chemaly, Marianne, Rivoal, Katell, Ducournau, Astrid, Buissonnière, Alice, Bénéjat, Lucie, Bessède, Emilie, Mégraud, Francis, Sheppard, Samuel K., and Lehours, Philippe

Published

2019

17. Genomic structure and insertion sites of Helicobacter pylori prophages from various geographical origins.

Author

Vale, Filipa F., Nunes, Alexandra, Oleastro, Mónica, Gomes, João P., Sampaio, Daniel A., Rocha, Raquel, Vítor, Jorge M. B., Engstrand, Lars, Pascoe, Ben, Berthenet, Elvire, Sheppard, Samuel K., Hitchings, Matthew D., Mégraud, Francis, Vadivelu, Jamuna, and Lehours, Philippe

Abstract

Helicobacter pylori genetic diversity is known to be influenced by mobile genomic elements. Here we focused on prophages, the least characterized mobile elements of H. pylori. We present the full genomic sequences, insertion sites and phylogenetic analysis of 28 prophages found in H. pylori isolates from patients of distinct disease types, ranging from gastritis to gastric cancer, and geographic origins, covering most continents. The genome sizes of these prophages range from 22.6-33.0 Kbp, consisting of 27-39 open reading frames. A 36.6% GC was found in prophages in contrast to 39% in H. pylori genome. Remarkably a conserved integration site was found in over 50% of the cases. Nearly 40% of the prophages harbored insertion sequences (IS) previously described in H. pylori. Tandem repeats were frequently found in the intergenic region between the prophage at the 3′ end and the bacterial gene. Furthermore, prophage genomes present a robust phylogeographic pattern, revealing four distinct clusters: one African, one Asian and two European prophage populations. Evidence of recombination was detected within the genome of some prophages, resulting in genome mosaics composed by different populations, which may yield additional H. pylori phenotypes. [ABSTRACT FROM AUTHOR]

Published

2017