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Your search keyword '"Mariette Barthelmebs"' showing total 11 results
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11 results on '"Mariette Barthelmebs"'

1. Antitumor effect of parathyroid hormone-related protein neutralizing antibody in human renal cell carcinoma in vitro and in vivo.

Author

Isabelle Talon, Véronique Lindner, Carole Sourbier, Eric Schordan, Sylvie Rothhut, Mariette Barthelmebs, Hervé Lang, Jean-Jacques Helwig, and Thierry Massfelder

Abstract

Functional inactivation of the von Hippel-Lindau (VHL) tumor suppressor gene occurs in 40–80% of human conventional renal cell carcinomas (RCCs). We showed recently that VHL-deficient RCCs expressed large amounts of parathyroid hormone-related protein (PTHrP), and that PTHrP, acting through the PTH1 receptor (PTH1R), plays an essential role in tumor growth. We also showed that PTHrP expression is negatively regulated by the VHL gene products (pVHL). Our goal was to determine whether blocking the PTHrP/PTH1R system might be of therapeutic value against RCC, independent of VHL status and PTHrP expression levels. The antitumor activity of PTHrP neutralizing antibody and of PTH1R antagonist were evaluated in vitro and in vivo in a panel of human RCC lines expressing or not pVHL. PTHrP is upregulated compared with normal tubular cells. In vitro, tumor cell growth and viability was decreased by up to 80% by the antibody in all cell lines. These effects resulted from apoptosis. Exogenously added PTHrP had no effect on cell growth and viability, but reversed the inhibitory effects of the antibody. The growth inhibition was reproduced by a specific PTH1R antagonist in all cell lines. In vivo, the treatment of nude mice bearing the Caki-1 RCC tumor with the PTHrP antibody inhibited tumor growth by 80%, by inducing apoptosis. Proliferation and neovascularization were not affected by the antiserum. Anti-PTHrP treatment induced no side effects as assessed by animal weight and blood chemistries. Current therapeutic strategies are only marginally effective against metastatic RCC, and adverse effects are common. This study provides a rationale for evaluating the blockade of PTHrP signaling as therapy for human RCC in a clinical setting. [ABSTRACT FROM AUTHOR]

Published
2006

2. Vitamin D3 triggers antitumor activity through targeting hedgehog signaling in human renal cell carcinoma.

Author

Dormoy, Valérian, Béraud, Claire, Lindner, Véronique, Coquard, Catherine, Barthelmebs, Mariette, Brasse, David, Jacqmin, Didier, Lang, Hervé, and Massfelder, Thierry

Subjects
CHOLECALCIFEROL, ANTINEOPLASTIC agents, HEDGEHOG signaling proteins, RENAL cell carcinoma, LABORATORY mice, CARCINOGENESIS, DRUG efficacy
Abstract

Human clear cell renal cell carcinoma (CCC) remains resistant to treatments despite the progress in targeted therapies. Several signaling pathways acting during renal development are reactivated during kidney tumorigenesis; this is the case of the sonic hedgehog (SHH)-Gli. Interestingly, the precursor of active vitamin D3 (VD3), cholecalciferol, has been demonstrated to be a strong inhibitor of SHH-Gli signaling. Here, we show the preclinical efficacy of cholecalciferol in CCC both in vitro and in vivo. A panel of CCC cell lines, tumors and normal corresponding tissues from CCC patients were used to evaluate the expression of the VD3 receptor and metabolizing enzymes and the effects of cholecalciferol treatment. Subsequently, xenografted mice were treated with cholecalciferol in a prophylactic or therapeutic manner; their response and the adverse effects were evaluated on the basis of weekly monitoring, followed by blood collection procedures and X-ray micro-computed tomography. VD3 receptor and metabolizing enzymes are dramatically decreased in human cell lines and tumors. Cholecalciferol decreases cell proliferation and increases cell death by inhibition of the SHH-Gli pathway. Xenografted mice treated with cholecalciferol exhibit absence of tumor development or substantial growth inhibition. The treatment was shown to be safe; it did not induce calcification or calcium reabsorption. These findings establish that, although VD3 receptors and metabolizing enzymes are absent in CCC, cholecalciferol supplementation is a strong tool to block the reactivation of SHH-Gli pathway in this pathology, leading ultimately to tumor regression. Cholecalciferol may have highly therapeutic potential in CCC. [ABSTRACT FROM AUTHOR]

Published
2012
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3. Contribution of angiotensin II internalization to intrarenal angiotensin II levels in rats.

Author

Ingert, Catherine, Grima, Michèle, Coquard, Catherine, Barthelmebs, Mariette, and Imbs, Jean-Louis

Subjects
ANGIOTENSINS, SALT deposits
Abstract

Examines the contribution of angiotensin II (ANG II) internalization to intrarenal angiotensin II levels in rats. Regulation of renal hemodynamics and sodium excretion; Effects of salt depletion; Components of renin-angiotensin system in plasma; Administration of losartan to rats causing 90 percent fall in intrarenal ANG II.

Published
2002
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4. Effects of dietary salt changes on renal renin-angiotensin system in rats.

Author

Ingert, Catherine, Grima, Michèle, Coquard, Catherine, Barthelmebs, Mariette, and Imbs, Jean-Louis

Subjects
ANGIOTENSINS, HEMODYNAMICS
Abstract

Examines the effects of dietary salt changes on renal-angiotensin system in rats. Regulation of renal hemodynamics and tubular transport function; Details on the steps for enzymatic cascade; Localization of angiotensinogen.

Published
2002
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