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Ubiquitylation of the initiator caspase DREDD is required for innate immune signalling
Authors:Meinander Annika  Runchel Christopher  Tenev Tencho  Chen Li  Kim Chan-Hee  Ribeiro Paulo S  Broemer Meike  Leulier Francois  Zvelebil Marketa  Silverman Neal  Meier Pascal
Affiliation:The Breakthrough Toby Robins Breast Cancer Research Centre, Institute of Cancer Research, Chester Beatty Laboratories, London, UK.
Abstract:Caspases have been extensively studied as critical initiators and executioners of cell death pathways. However, caspases also take part in non-apoptotic signalling events such as the regulation of innate immunity and activation of nuclear factor-κB (NF-κB). How caspases are activated under these conditions and process a selective set of substrates to allow NF-κB signalling without killing the cell remains largely unknown. Here, we show that stimulation of the Drosophila pattern recognition protein PGRP-LCx induces DIAP2-dependent polyubiquitylation of the initiator caspase DREDD. Signal-dependent ubiquitylation of DREDD is required for full processing of IMD, NF-κB/Relish and expression of antimicrobial peptide genes in response to infection with Gram-negative bacteria. Our results identify a mechanism that positively controls NF-κB signalling via ubiquitin-mediated activation of DREDD. The direct involvement of ubiquitylation in caspase activation represents a novel mechanism for non-apoptotic caspase-mediated signalling.
Keywords:caspase  Drosophila  IAP  innate immunity  ubiquitin
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