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The full-length interleukin-33 (FLIL33)-importin-5 interaction does not regulate nuclear localization of FLIL33 but controls its intracellular degradation.

J. Biol. Chem.. 2017; 
ClermanAndrew,NoorZahid,FishelevichRita,LockatellVirginia,HamptonBrian S,ShahNirav G,SalcedoMariah V,ToddNevins W,AtamasSergei P,LuzinaIri
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摘要

Human mature IL-33 is a member of the IL-1 family and a potent regulator of immunity through its pro-T helper cell 2 activity. Its precursor form, full-length interleukin-33 (FLIL33), is an intranuclear protein in many cell types, including fibroblasts, and its intracellular levels can change in response to stimuli. However, the mechanisms controlling the nuclear localization of FLIL33 or its stability in cells are not understood. Here, we identified importin-5 (IPO5), a member of the importin family of nuclear transport proteins, as an intracellular binding partner of FLIL33. By overexpressing various FLIL33 protein segments and variants in primary human lung fibroblasts and HEK293T cells, we... More

关键词

fibroblast,interleukin-33,nuclear translocation,proteasome,protein degradation,protein-protein interac
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