AI Article Synopsis
- L-selectin plays a key role in leukocyte adhesion and rolling by interacting with various proteins through its cytoplasmic tail.
- The study identified μ1A, part of the clathrin-coated vesicle AP-1 complex, as a novel binding protein for the L-selectin tail, suggesting that this interaction is influenced by the phosphorylation state of μ1A and L-selectin.
- Overall, the findings highlight the importance of L-selectin transport mechanisms and the regulatory role of phosphorylation in determining its interaction with μ1A and retrograde transport processes within cells.
Article Abstract
L-selectin regulates leukocyte adhesion and rolling along the endothelium. Proteins binding to the cytoplasmic tail of L-selectin regulate L-selectin functions. We used L-selectin cytoplasmic tail peptide pulldown assays combined with high sensitivity liquid chromatography/mass spectrometry to identify novel L-selectin tail-binding proteins. Incubation of the L-selectin tail with cell extracts from phorbol 12-myristate 13-acetate-stimulated Raw 264.7 macrophages resulted in the binding of μ1A of the clathrin-coated vesicle AP-1 complex. Furthermore, full-length GST-μ1A and the GST-μ1A C-terminal domain, but not the GST-μ1A N-terminal domain, bind to L-selectin tail peptide, and the intracellular pool of L-selectin colocalizes with AP-1 at the -Golgi network. We identified a novel basic protein motif consisting of a cluster of three dibasic residues (RR, KK, and KK) in the membrane-proximal domain of the L-selectin tail as well as a doublet of aspartic acid residues (DD) in the membrane-distal end of the L-selectin tail involved in μ1A binding. Stimulation of Raw 264.7 macrophages with PMA augmented the amount of μ1A associated with anti-L-selectin immunoprecipitates. However, full-length GST-μ1A did not bind to the phospho-L-selectin tail or phospho-mimetic S364D L-selectin tail. Accordingly, we propose that phosphorylation of μ1A is required for interaction with the L-selectin tail and that L-selectin tail phosphorylation may regulate this interaction Molecular docking of the L-selectin tail to μ1A was used to identify the μ1A surface domain binding the L-selectin tail and to explain how phosphorylation of the L-selectin tail abrogates μ1A interaction. Our findings indicate that L-selectin is transported constitutively by the AP-1 complex, leading to the formation of a -Golgi network reserve pool and that phosphorylation of the L-selectin tail blocks AP-1-dependent retrograde transport of L-selectin.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5399118 | PMC |
| http://dx.doi.org/10.1074/jbc.M116.768598 | DOI Listing |
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