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CLIC4 interacts with histamine H3 receptor and enhances the receptor cell surface expression.

Biochemical and biophysical research communications (2008-02-28)
Kay Maeda, Mitsuya Haraguchi, Atsuo Kuramasu, Takeya Sato, Kyohei Ariake, Hiroyuki Sakagami, Hisatake Kondo, Kazuhiko Yanai, Kohji Fukunaga, Teruyuki Yanagisawa, Jun Sukegawa
ZUSAMMENFASSUNG

Histamine H3 receptor (H3R), one of G protein-coupled receptors (GPCRs), has been known to regulate neurotransmitter release negatively in central and peripheral nervous systems. Recently, a variety of intracellular proteins have been identified to interact with carboxy (C)-termini of GPCRs, and control their intracellular trafficking and signal transduction efficiencies. Screening for such proteins that interact with the C-terminus of H3R resulted in identification of one of the chloride intracellular channel (CLIC) proteins, CLIC4. The association of CLIC4 with H3R was confirmed in in vitro pull-down assays, coimmunoprecipitation from rat brain lysate, and immunofluorescence microscopy of rat cerebellar neurons. The data from flowcytometric analysis, radioligand receptor binding assay, and cell-based ELISA indicated that CLIC4 enhanced cell surface expression of wild-type H3R, but not a mutant form of the receptor that failed to interact with CLIC4. These results indicate that, by binding to the C-terminus of H3R, CLIC4 plays a critical role in regulation of the receptor cell surface expression.