Your search keyword '"Huppertz, Christine"' showing total 4 results

1. Autocrine Loop Involving IL-6 Family Member LIF, LIF Receptor, and STAT4 Drives Sustained Fibroblast Production of Inflammatory Mediators.

Author

Nguyen, Hung N., Noss, Erika H., Mizoguchi, Fumitaka, Huppertz, Christine, Wei, Kevin S., Watts, Gerald F.M., and Brenner, Michael B.

Subjects

*INFLAMMATORY mediators, *FIBROBLASTS, *LEUCOCYTES, *AUTOCRINE mechanisms, *INTERLEUKIN-6, *GENES

Abstract

Summary Fibroblasts are major contributors to and regulators of inflammation and dominant producers of interleukin-6 (IL-6) in inflammatory diseases like rheumatoid arthritis. Yet, compared to leukocytes, the regulation of inflammatory pathways in fibroblasts is largely unknown. Here, we report that analyses of genes coordinately upregulated with IL-6 pointed to STAT4 and leukemia inhibitory factor (LIF) as potentially linked. Gene silencing revealed that STAT4 was required for IL-6 transcription. STAT4 was recruited to the IL-6 promoter after fibroblast activation, and LIF receptor (LIFR) and STAT4 formed a molecular complex that, together with JAK1 and TYK2 kinases, controlled STAT4 activation. Importantly, a positive feedback loop involving autocrine LIF, LIFR, and STAT4 drove sustained IL-6 transcription. Besides IL-6, this autorine loop also drove the production of other key inflammatory factors including IL-8, granulocyte-colony stimulating factor (G-CSF), IL-33, IL-11, IL-1α, and IL-1β. These findings define the transcriptional regulation of fibroblast-mediated inflammation as distinct from leukocytes. [ABSTRACT FROM AUTHOR]

Published

2017

2. In vivo and in vitro SAR of tetracyclic MAPKAP-K2 (MK2) inhibitors. Part I

Author

Revesz, Laszlo, Schlapbach, Achim, Aichholz, Reiner, Feifel, Roland, Hawtin, Stuart, Heng, Richard, Hiestand, Peter, Jahnke, Wolfgang, Koch, Guido, Kroemer, Markus, Möbitz, Henrik, Scheufler, Clemens, Velcicky, Juraj, and Huppertz, Christine

Subjects

*CLINICAL drug trials, *STRUCTURE-activity relationship in pharmacology, *MITOGEN-activated protein kinases, *CYCLIC compounds, *THERAPEUTIC use of amino acids, *LACTAMS, *KETONES, *BLOOD cells

Abstract

Abstract: Pyrrolo[2,3-f]isoquinoline based amino acids, tetracyclic lactams and cyclic ketone analogues are described as novel MK2 inhibitors with IC50 as low as 5nM and good selectivity profiles against a number of related kinases including ERK, p38α and JNKs. TNFα release was suppressed from human peripheral blood mononuclear cells (hPBMCs), and a representative compound inhibited LPS induced TNFα release in mice illustrating the potential of this series to provide orally active MK2 inhibitors. [Copyright &y& Elsevier]

Published

2010

3. In vivo and in vitro SAR of tetracyclic MAPKAP-K2 (MK2) inhibitors. Part II

Author

Revesz, Laszlo, Schlapbach, Achim, Aichholz, Reiner, Dawson, Janet, Feifel, Roland, Hawtin, Stuart, Littlewood-Evans, Amanda, Koch, Guido, Kroemer, Markus, Möbitz, Henrik, Scheufler, Clemens, Velcicky, Juraj, and Huppertz, Christine

Subjects

*CLINICAL drug trials, *STRUCTURE-activity relationship in pharmacology, *CYCLIC compounds, *MITOGEN-activated protein kinases, *CHEMICAL inhibitors, *CYCLOPROPANE, *ORAL drug administration, *DRUG absorption

Abstract

Abstract: Spirocyclopropane- and spiroazetidine-substituted tetracycles 13D–E and 16A are described as orally active MK2 inhibitors. The spiroazetidine derivatives are potent MK2 inhibitors with IC50 <3nM and inhibit the release of TNFα (IC50<0.3μM) from hPBMCs and hsp27 phosphorylation in anisomycin stimulated THP-1 cells. The spirocyclopropane analogues are less potent against MK2 (IC50 =0.05–0.23μM), less potent in cells (IC50 <1.1μM), but show good oral absorption. Compound 13E (100mg/kg po; bid) showed oral activity in rAIA and mCIA, with significant reduction of swelling and histological score. [Copyright &y& Elsevier]

Published

2010

4. Pyrrolo-pyrimidones: A novel class of MK2 inhibitors with potent cellular activity

Author

Schlapbach, Achim, Feifel, Roland, Hawtin, Stuart, Heng, Richard, Koch, Guido, Moebitz, Henrik, Revesz, Laszlo, Scheufler, Clemens, Velcicky, Juraj, Waelchli, Rudolf, and Huppertz, Christine

Subjects

*ENZYME inhibitors, *RHEUMATOID arthritis, *PHOSPHORYLATION, *HEAT shock proteins, *TUMOR necrosis factors

Abstract

Abstract: Pyrrolo-pyrimidones of the general structure 1 were synthesized and evaluated for their potential as MK2 inhibitors. Potent derivatives were discovered which inhibit MK2 in the nanomolar range and show potent inhibition of cytokine release from LPS-stimulated monocytes. These derivatives were shown to inhibit phosphorylation of hsp27, a downstream target of MK2 and are modestly selective in a panel of 28 kinases. [Copyright &y& Elsevier]

Published

2008