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Literature DB >> 27595347

A molecular code for endosomal recycling of phosphorylated cargos by the SNX27-retromer complex.

Thomas Clairfeuille¹, Caroline Mas¹, Audrey S M Chan², Zhe Yang¹, Maria Tello-Lafoz³, Mintu Chandra¹, Jocelyn Widagdo⁴, Markus C Kerr¹, Blessy Paul¹, Isabel Mérida³, Rohan D Teasdale¹, Nathan J Pavlos², Victor Anggono⁴, Brett M Collins¹.

Abstract

Recycling of internalized receptors from endosomal compartments is essential for the receptors' cell-surface homeostasis. Sorting nexin 27 (SNX27) cooperates with the retromer complex in the recycling of proteins containing type I PSD95-Dlg-ZO1 (PDZ)-binding motifs. Here we define specific acidic amino acid sequences upstream of the PDZ-binding motif required for high-affinity engagement of the human SNX27 PDZ domain. However, a subset of SNX27 ligands, such as the β2 adrenergic receptor and N-methyl-D-aspartate (NMDA) receptor, lack these sequence determinants. Instead, we identified conserved sites of phosphorylation that substitute for acidic residues and dramatically enhance SNX27 interactions. This newly identified mechanism suggests a likely regulatory switch for PDZ interaction and protein transport by the SNX27-retromer complex. Defining this SNX27 binding code allowed us to classify more than 400 potential SNX27 ligands with broad functional implications in signal transduction, neuronal plasticity and metabolite transport.

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Year: 2016 PMID： 27595347 DOI： 10.1038/nsmb.3290

Source DB: PubMed Journal: Nat Struct Mol Biol ISSN： 1545-9985 Impact factor: 15.369

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