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Featured researches published by Claude Lambert.


Journal of Immunology | 2004

Recruitment of STAT3 for Production of IL-10 by Colon Carcinoma Cells Induced by Macrophage-Derived IL-6

Jean-Philippe Herbeuval; Eric Lelièvre; Claude Lambert; Michel Dy; Christian Genin

The immunosuppressive cytokine IL-10 is associated with poor prognosis in colon cancer. Although macrophages are involved in antitumor defenses, production of IL-10 by tumor cells may permit malignant cells escape to cell-mediated immune defenses. To investigate interactions between macrophages and tumor cells in humans, we cultured macrophages isolated from patients and tested the effect of these macrophages on the production of IL-10 by several tumor cell lines. Macrophages were isolated from pleural effusions of patients with malignancy and from noncancer control patients. We demonstrated that culture supernatants of macrophages from both sources strongly stimulated IL-10 production by the three different human colon adenocarcinoma cell lines, Colo 205, Colo 320, and HT29. Recombinant IL-6, but not IL-10, TNF-α, and IFN-α, stimulated the secretion of IL-10 by colon tumor cells. mAbs against IL-6 and IL-6R prevented the effect of macrophage culture supernatants and of rIL-6, respectively, on the production of IL-10 by the three cell lines. Cocultures of macrophages and colon cancer cells showed that these tumor cells first stimulated macrophages to produce IL-6, which was then followed by IL-6-induced IL-10 production by colon cancer cells. Finally, we showed that IL-10 gene regulation was mediated by STAT3, which was phosphorylated after the binding of IL-6 to IL-6R. This is the first demonstration that IL-6, secreted by macrophages, can induce a STAT3-mediated IL-10 production by colon tumor cells.


Immunology Letters | 2003

Technique for obtaining highly enriched, quiescent immature Langerhans cells suitable for ex vivo assays

Isabelle Tchou; Odile Sabido; Claude Lambert; Laurent Misery; Olivier Garraud; Christian Genin

Epidermis and surface epithelium-dendritic cells comprise of immature cells termed Langerhans cells (LCs), which express characteristically the Birbeck granules, along with surface markers such as CD1a. These cells can capture a pathogen and then migrate and differentiate to a more mature stage. During this maturation process, dentritic cells express surface markers differentially. In physio-pathological models of infection where LCs are involved, it is critically important to ensure that the LCs tested in vitro are still immature and are not artefactually matured-dentritic cells. For experimental purposes, LCs were isolated from skin epidermis obtained from patients undergoing plastic surgery. This work thus aimed at collecting fresh LCs ex vivo and at testing the cells for phenotypic and functional characteristics of the immature stage. After mechanic disruption of the epidermis and proceeding for single cell suspension obtaining, two methods for purification were tested in parallel: (a) a positive immuno-magnetic separation by anti-CD1a-coated beads and (b) a purely mechanic purification system based on a three-step Ficoll floatation process. Both systems were equally efficient in terms of purification and yield. By using flow cytometry phenotyping, we have demonstrated that the use of magnetic beads led to some degree of maturation of CD1a(+) LCs, contrary to the repeated Ficoll floatation. This work calls attention for the use of certain monoclonal antibodies such as anti-CD1a to purify immature dendritic cells as they pre-activate these cells. Pre-activation would render a number of assays on the early events of LC physiology invalid, contrary to the purification of fresh skin epidermis LCs by means of a repeated Ficoll floatation.


Journal of the National Cancer Institute | 2003

Macrophages from cancer patients: analysis of TRAIL, TRAIL receptors, and colon tumor cell apoptosis

Jean-Philippe Herbeuval; Claude Lambert; Odile Sabido; Michèle Cottier; Pierre Fournel; Michel Dy; Christian Genin


Clinical Cancer Research | 2001

The Expression of G250/MN/CA9 Antigen by Flow Cytometry: Its Possible Implication for Detection of Micrometastatic Renal Cancer Cells

Guorong Li; Karine Passebosc-Faure; Claude Lambert; Anne Gentil-Perret; François Blanc; Egbert Oosterwijk; Jean-François Mosnier; Christian Genin; Jacques Tostain


Clinical Cancer Research | 2003

Rapid and sensitive detection of messenger RNA expression for molecular differential diagnosis of renal cell carcinoma

Guorong Li; Muriel Cuilleron; Anne Gentil-Perret; Michèle Cottier; Karine Passebosc-Faure; Claude Lambert; Christian Genin; Jacques Tostain


Anticancer Research | 2000

Flow cytometric analysis of antigen expression in malignant and normal renal cells.

Guorong Li; Karine Passebosc-Faure; Claude Lambert; Anne Gentil-Perret; François Blanc; Egbert Oosterwijk; Jean-François Mosnier; Christian Genin; Jacques Tostain


European Urology Supplements | 2002

Cadherin-6 gene expression in conventional renal cell carcinomas: implication for detection of circulating renal cancer cells

Guorong Li; Karine Passebosc-Faure; Claude Lambert; Anne Gentil-Perret; Christian Genin; Jacques Tostain


The Journal of Urology | 2004

1756: Combination of MN/CA9 Gene Expression and Cytological Examination in fine Needle Aspiration Biopsy for Differential Diagnosis of the Imaging-Indeterminate Renal Tumors

Guorong Li; Muriel Cuilleron; Michèle Cottier; Anne Gentil-Perret; Karine Passebosc-Faure; Claude Lambert; Christian Genin; Jacques Tostain; Saint Etienne


European Urology Supplements | 2004

381 RT-PCR of urine survivin and MN/CA9 for non-invasive diagnosis of transitional cell carcinoma (TCC) of urinary bladder

Guorong Li; Karine Passebosc-Faure; Anne Gentil-Perret; Claude Lambert; Christian Genin; Jacques Tostain


European Urology Supplements | 2004

494 Evaluation of MN/CA9 gene expression in fine needle aspiration (FNA) biopsy for differential diagnosis of conventional renal cell carcinoma (RCC) among the imaging-indeterminate renal tumours

Guorong Li; M. Cuilleron; Michèle Cottier; Anne Gentil-Perret; Karine Passebosc-Faure; Claude Lambert; Christian Genin; Jacques Tostain

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Michel Dy

Centre national de la recherche scientifique

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