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Your search keyword '"Pipy, Bernard"' showing total 5 results
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5 results on '"Pipy, Bernard"'

1. Comparative study of the effects of ziram and disulfiram on human monocyte-derived macrophage functions and polarization: involvement of zinc.

Author

Parny, Melissa, Bernad, José, Prat, Mélissa, Salon, Marie, Aubouy, Agnès, Bonnafé, Elsa, Coste, Agnès, Pipy, Bernard, and Treilhou, Michel

Subjects
DISULFIRAM, ZINC, GENE expression profiling, MACROPHAGES, PHAGOCYTOSIS
Abstract

Ziram, a zinc dithiocarbamate is widely used worldwide as a fungicide in agriculture. In order to investigate ziram-induced changes in macrophage functions and polarization, human monocytes-derived macrophages in culture were treated with ziram at 0.01–10 μmol.L−1 for 4–24 h. To characterize zinc involvement in these changes, we also determined the effects of disulfiram alone (dithiocarbamate without zinc) or in co-incubation with ZnSO4. We have shown that ziram and disulfiram at 0.01 μmol.L−1 increased zymosan phagocytosis. In contrast, ziram at 10 μmol.L−1 completely inhibited this phagocytic process, the oxidative burst triggered by zymosan and the production of TNF-α, IL-1β, IL-6, and CCL2 triggered by LPS. Disulfiram had the same effects on these macrophages functions only when combined with zinc (10 μmol.L−1). In contrast, at 10 μmol.L−1 ziram and zinc associated-disulfiram induced expression of several antioxidants genes HMOX1, SOD2, and catalase, which could suggest the induction of oxidative stress. This oxidative stress could be involved in the increase in late apoptosis induced by ziram (10 μmol.L−1) and zinc associated-disulfiram. Concerning gene expression profiles of membrane markers of macrophage polarization, ziram at 10 μmol.L−1 had two opposite effects. It inhibited the gene expression of M2 markers (CD36, CD163) in the same way as the disulfiram-zinc co-treatment. Conversely, ziram induced gene expression of other M2 markers CD209, CD11b, and CD16 in the same way as treatment with zinc alone. Disulfiram-zinc association had no significant effects on these markers. These results taken together show that ziram via zinc modulates macrophages to M2-like anti-inflammatory phenotype which is often associated with various diseases. [ABSTRACT FROM AUTHOR]

Published
2021
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2. Immunohistochemical distribution of activated nuclear factor κB and peroxisome proliferator-activated receptors in carbon tetrachloride-induced chronic liver injury in rats.

Author

Orfila, Claudine, Lepert, Jean-Claude, Alric, Laurent, Carrera, Georges, Béraud, Maryse, and Pipy, Bernard

Subjects
LIVER cells, BILIARY tract, MACROPHAGES, TRANSCRIPTION factors, PROTEINS, REACTIVE oxygen species, ABSORPTION (Physiology)
Abstract

We investigated the immunohistochemical distribution of active NF-κB p65 and peroxisome proliferator-activated receptor (PPAR) subtypes alpha and gamma in the different phases of liver steatonecrosis and cirrhosis induced in rats after 3 and 9 weeks of carbon tetrachloride (CCl4) intoxication. CCl4 treatment can induce changes in the expression of NF-κB and PPARs. Immunohistochemical analysis of liver tissue sections from rats with steatonecrosis or cirrhosis demonstrated a significant increase in the number of NF-κB-positive and TNF-α-positive hepatocytes and Kupffer cells. In healthy controls, no expression of active NF-κB was detected. In previous studies, we have demonstrated that Kupffer cells isolated from rats with CCl4-induced steatonecrosis produced more reactive oxygen intermediates than cells isolated from normal rats. These oxidants could activate NF-κB and lead to an overexpression of TNF-α, observed in liver tissue sections. After CCl4 ingestion, the rat livers demonstrated a significantly decreased number of hepatocytes expressing PPARα and PPARγ and a significantly increased number of ED2-positive Kupffer cells expressing these transcription factors, compared to normal. The activation of the p65 isoform of NF-κB correlates negatively with transcription of the alpha and gamma isoforms of PPAR in hepatocytes, and positively in Kupffer cells. These results suggest that the regulation and the role of these two transcription factors differ in the two cell types studied. [ABSTRACT FROM AUTHOR]

Published
2005
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3. Hepatic metallothionein in patients with chronic hepatitis C: relationship with severity of liver disease and response to treatment

Author

Carrera, Georges, Paternain, Jose Luis, Carrere, Nicolas, Folch, Jaume, Courtade-Saïdi, Monique, Orfila, Claudine, Vinel, Jean Pierre, Alric, Laurent, and Pipy, Bernard

Subjects
REACTIVE oxygen species, HEPATITIS C virus
Abstract

: ObjectivesReactive oxygen species may be involved in the pathogenesis of chronic hepatitis C virus infection. Metallothionein (MT) is an essential protein for the protection of cells against reactive oxygen species. The aim of this prospective study was to assess the influence of the hepatic level and cellular distribution of MT in hepatitis C virus (HCV) infection and in the liver disease outcome.: MethodsIn liver biopsy samples of 32 patients with chronic HCV infection and of 12 control subjects, quantification of MT was performed by radioimmunoassay, MT, interleukin (IL)-1 and -6, and tumor necrosis factor (INF)–α mRNA by reverse transcription–polymerase chain reaction (PCR) and cellular distribution by immunohistochemistry.: ResultsIn HCV-infected patients, MT liver protein level was 3-fold lower than in control specimens. A significant inverse linear regression between MT protein or mRNA expression and the Histological Activity Index, the necroinflammatory grade, and the stage of fibrosis was observed. MT immunostaining was located in the nucleus and cytoplasm in hepatocytes of control subjects, whereas it was mainly cytoplasmic in HCV-infected patients. Before interferon (IFN) therapy, the hepatic MT level in patients that were nonsustained responders was half that of sustained responders. Intrahepatic IL-6 and MT were simultaneously down-regulated, but no correlation was found between MT and intrahepatic cytokine mRNA expression in patients with chronic HCV infection.: ConclusionsThis study shows that hepatic MT expression could reflect the severity of chronic HCV infection and could be one of the factors associated with a favorable clinical outcome in the response to interferon therapy. [Copyright &y& Elsevier]

Published
2003
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4. Opioids prevent regeneration in adult mammals through inhibition of ROS production.

Author

Labit, Elodie, Rabiller, Lise, Rampon, Christine, Guissard, Christophe, André, Mireille, Barreau, Corinne, Cousin, Béatrice, Carrière, Audrey, Eddine, Mohamad Ala, Pipy, Bernard, Pénicaud, Luc, Lorsignol, Anne, Vriz, Sophie, Dromard, Cécile, and Casteilla, Louis

Abstract

Inhibition of regeneration and induction of tissue fibrosis are classic outcomes of tissue repair in adult mammals. Here, using a newly developed model of regeneration in adult mammals i.e. regeneration after massive resection of an inguinal fat pad, we demonstrate that both endogenous and exogenous opioids prevent tissue regeneration in adults, by inhibiting the early production of reactive oxygen species (ROS) that generally occurs after lesion and is required for regeneration. These effects can be overcome and regeneration induced by the use of an opioid antagonist. The results obtained in both our new model and the gold standard adult zebrafish demonstrate that this mechanism can be considered as a general paradigm in vertebrates. This work clearly demonstrates that ROS is required for tissue regeneration in adult mammals and shows the deleterious effect of opioids on tissue regeneration through the control of this ROS production. It thus raises questions about opioid-based analgesia in perioperative care. [ABSTRACT FROM AUTHOR]

Published
2018
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