Identification of 34 novel proinflammatory proteins in a genome-wide macrophage functional screen |
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Authors: | David H Wyllie Karen C Søgaard Karen Holland Xu Yaobo Migena Bregu Adrian V S Hill Endre Kiss-Toth |
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Affiliation: | Jenner Institute, Old Road Campus Research Building, Oxford University, Oxford, United Kingdom. |
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Abstract: | Signal transduction pathways activated by Toll-like Receptors and the IL-1 family of cytokines are fundamental to mounting an innate immune response and thus to clearing pathogens and promoting wound healing. Whilst mechanistic understanding of the regulation of innate signalling pathways has advanced considerably in recent years, there are still a number of critical controllers to be discovered. In order to characterise novel regulators of macrophage inflammation, we have carried out an extensive, cDNA-based forward genetic screen and identified 34 novel activators, based on their ability to induce the expression of cxcl2. Many are physiologically expressed in macrophages, although the majority of genes uncovered in our screen have not previously been linked to innate immunity. We show that expression of particular activators has profound but distinct impacts on LPS-induced inflammatory gene expression, including switch-type, amplifier and sensitiser behaviours. Furthermore, the novel genes identified here interact with the canonical inflammatory signalling network via specific mechanisms, as demonstrated by the use of dominant negative forms of IL1/TLR signalling mediators. |
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