Your search keyword '"Buffat L"' showing total 3 results

1. Mature IgM-expressing plasma cells sense antigen and develop competence for cytokine production upon antigenic challenge

Author

Blanc, P, Moro-Sibilot, L, Barthly, L, Jagot, F, This, S, de Bernard, S, Buffat, L, Dussurgey, S, Colisson, R, Hobeika, E, Fest, T, Taillardet, M, Thaunat, O, Sicard, A, Mondiere, P, Genestier, L, Nutt, SL, Defrance, T, Blanc, P, Moro-Sibilot, L, Barthly, L, Jagot, F, This, S, de Bernard, S, Buffat, L, Dussurgey, S, Colisson, R, Hobeika, E, Fest, T, Taillardet, M, Thaunat, O, Sicard, A, Mondiere, P, Genestier, L, Nutt, SL, and Defrance, T

Abstract

Dogma holds that plasma cells, as opposed to B cells, cannot bind antigen because they have switched from expression of membrane-bound immunoglobulins (Ig) that constitute the B-cell receptor (BCR) to production of the secreted form of immunoglobulins. Here we compare the phenotypical and functional attributes of plasma cells generated by the T-cell-dependent and T-cell-independent forms of the hapten NP. We show that the nature of the secreted Ig isotype, rather than the chemical structure of the immunizing antigen, defines two functionally distinct populations of plasma cells. Fully mature IgM-expressing plasma cells resident in the bone marrow retain expression of a functional BCR, whereas their IgG+ counterparts do not. Antigen boost modifies the gene expression profile of IgM+ plasma cells and initiates a cytokine production program, characterized by upregulation of CCL5 and IL-10. Our results demonstrate that IgM-expressing plasma cells can sense antigen and acquire competence for cytokine production upon antigenic challenge.

Published

2016

2. Early diet-induced non-alcoholic steatohepatitis in APOE2 knock-in mice and its prevention by fibrates

Author

Shiri-Sverdlov, R., Shiri-Sverdlov, R., Wouters, Kristiaan, van Gorp, P.J.J., Gijbels, M.J.J., Noel, B., Buffat, L., Staels, B., Maeda, N., van Bilsen, M., Hofker, M.H., Shiri-Sverdlov, R., Shiri-Sverdlov, R., Wouters, Kristiaan, van Gorp, P.J.J., Gijbels, M.J.J., Noel, B., Buffat, L., Staels, B., Maeda, N., van Bilsen, M., and Hofker, M.H.

Abstract

BACKGROUND/AIMS: The molecular mechanisms leading to Non-Alcoholic Steatohepatitis (NASH) are not fully understood. In mice, NASH can be inhibited by fenofibrate, a synthetic agonist for the nuclear receptor peroxisome proliferator activated receptor alpha, which regulates hepatic triglyceride metabolism. This study aimed to elucidate the relation between steatosis and inflammation in NASH in a human-like hyperlipidemic mouse model. METHODS: Liver phenotype and gene expression were assessed in APOE2 knock-in mice that were fed a western-type high fat diet with or without co-administration of fenofibrate. RESULTS: In response to a western diet, APOE2 knock-in mice developed NASH characterized by steatosis and inflammation. Strikingly, macrophage accumulation in the liver preceded the steatosis during progression of the disease. This phenotype was in line with gene expression patterns, which showed regulation of two major groups of genes, i.e. inflammatory and lipid genes. Fenofibrate treatment decreased hepatic macrophage accumulation and abolished steatosis. Moreover, a marked reduction in the expression of inflammatory genes occurred immediately after fibrate treatment. CONCLUSIONS: These data indicate that inflammation might play an instrumental role during the development of NASH in this mouse model. Inhibition of NASH by fenofibrate may be due, at least in part, to its inhibitory effect on pro-inflammatory genes.

Published

2006

3. Early diet-induced non-alcoholic steatohepatitis in APOE2 knock-in mice and its prevention by fibrates

Author

Shiri-Sverdlov, R., Wouters, Kristiaan, van Gorp, P.J.J., Gijbels, M.J.J., Noel, B., Buffat, L., Staels, B., Maeda, N., van Bilsen, M., Hofker, M.H., Shiri-Sverdlov, R., Wouters, Kristiaan, van Gorp, P.J.J., Gijbels, M.J.J., Noel, B., Buffat, L., Staels, B., Maeda, N., van Bilsen, M., and Hofker, M.H.

Abstract

BACKGROUND/AIMS: The molecular mechanisms leading to Non-Alcoholic Steatohepatitis (NASH) are not fully understood. In mice, NASH can be inhibited by fenofibrate, a synthetic agonist for the nuclear receptor peroxisome proliferator activated receptor alpha, which regulates hepatic triglyceride metabolism. This study aimed to elucidate the relation between steatosis and inflammation in NASH in a human-like hyperlipidemic mouse model. METHODS: Liver phenotype and gene expression were assessed in APOE2 knock-in mice that were fed a western-type high fat diet with or without co-administration of fenofibrate. RESULTS: In response to a western diet, APOE2 knock-in mice developed NASH characterized by steatosis and inflammation. Strikingly, macrophage accumulation in the liver preceded the steatosis during progression of the disease. This phenotype was in line with gene expression patterns, which showed regulation of two major groups of genes, i.e. inflammatory and lipid genes. Fenofibrate treatment decreased hepatic macrophage accumulation and abolished steatosis. Moreover, a marked reduction in the expression of inflammatory genes occurred immediately after fibrate treatment. CONCLUSIONS: These data indicate that inflammation might play an instrumental role during the development of NASH in this mouse model. Inhibition of NASH by fenofibrate may be due, at least in part, to its inhibitory effect on pro-inflammatory genes.

Published

2006