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2 research outputs found

Identification of lysine residues critical for the transcriptional activity and polyubiquitination of the NF-κB family member RelB

Author: Adhikary
Baumann
Carmody
Chen
Croxton
Dietmar Fischer
Duran
Ghosh
Haglund
Hayden
Ikeda
Julia Leidner
Lawrence
Lernbecher
Lernbecher
Lysann Palkowitsch
Maier
Maine
Marienfeld
Marienfeld
Oeckinghaus
Palkowitsch
Ralf Marienfeld
Saccani
Senftleben
Tang
Uta Marienfeld
Weih
Zhong
Publication venue: 'Portland Press Ltd.'
Publication date
Field of study

The Ca2+-dependent Phosphatase Calcineurin Controls the Formation of the Carma1-Bcl10-Malt1 Complex during T Cell Receptor-induced NF-κB Activation*

Author: Andrea Eitelhuber
Bidère
Brenner
Cornelia Brunner
Daniel Krappmann
Edin
Hinz
Hughes
Inesi
Ishiguro
Ishiguro
Lysann Palkowitsch
Marienfeld
Marienfeld
Moreno-García
Moreno-García
Oeckinghaus
Oh-hora
Palkowitsch
Ralf B. Marienfeld
Scharschmidt
Schulze-Luehrmann
Serfling
Shibasaki
Shinohara
Sommer
Thome
Trushin
Trushin
Uta Marienfeld
Wegener
Welteke
Werlen
Zeng
Publication venue: American Society for Biochemistry and Molecular Biology
Publication date: 01/01/2011
Field of study

T cell receptor (TCR) ligation induces increased diacylglycerol and Ca2+ levels in T cells, and both secondary messengers are crucial for TCR-induced nuclear factor of activated T cells (NF-AT) and NF-κB signaling pathways. One prominent calcium-dependent enzyme involved in the regulation of NF-AT and NF-κB signaling pathways is the protein phosphatase calcineurin. However, in contrast to NF-AT, which is directly dephosphorylated by calcineurin, the molecular basis of the calcium-calcineurin dependence of the TCR-induced NF-κB activity remains largely unknown. Here, we demonstrate that calcineurin regulates TCR-induced NF-κB activity by controlling the formation of a protein complex composed of Carma1, Bcl10, and Malt1 (CBM complex). For instance, increased calcium levels induced by ionomycin or thapsigargin augmented the phorbol 12-myristate 13-acetate-induced formation of the CBM complex and activation of NF-κB, whereas removal of calcium by the calcium chelator EGTA-acetoxymethyl ester (AM) attenuated both processes. Furthermore, inhibition of the calcium-dependent phosphatase calcineurin with the immunosuppressive agent cyclosporin A (CsA) or FK506 as well as siRNA-mediated knockdown of calcineurin A strongly affected the PMA + ionomycin- or anti-CD3 + CD28-induced CBM complex assembly. Mechanistically, the positive effect of calcineurin on the CBM complex formation seems to be linked to a dephosphorylation of Bcl10. For instance, Bcl10 was found to be hyperphosphorylated in Jurkat T cells upon treatment with CsA or EGTA-AM, and calcineurin dephosphorylated Bcl10 in vivo and in vitro. Furthermore, we show here that calcineurin A interacts with the CBM complex. In summary, the evidence provided here argues for a previously unanticipated role of calcineurin in CBM complex formation as a molecular basis of the inhibitory function of CsA or FK506 on TCR-induced NF-κB activity

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PubMed Central

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