INVESTIGADORES
CACERES Alfredo Oscar
artículos
Título:
Polarized traffic of LRP1 involves AP1B and SNX17 operating upon Y-dependent sorting motifs in different pathways.
Autor/es:
DONOSO, M., CANCINO, J., LE, J., VAN KERHOF, P., RETAMAL, C., BU, G., GONZALEZ, A., CÁCERES, A., MARZOLO, M. P.
Revista:
MOLECULAR BIOLOGY OF THE CELL
Editorial:
AMER SOC CELL BIOLOGY
Referencias:
Año: 2009 vol. 20 p. 481 - 497
ISSN:
1059-1524
Resumen:
Low-density lipoprotein receptor–related protein 1 (LRP1) is an endocytic recycling receptor with two cytoplasmic tyrosine-based basolateral sorting signals. Here we show that during biosynthetic trafficking LRP1 uses AP1B adaptor complex to move from a post-TGN recycling endosome (RE) to the basolateral membrane. Then it recycles basolaterally from the basolateral sorting endosome (BSE) involving recognition by sorting nexin 17 (SNX17). In the biosyntheticpathway, Y29 but not N26 from a proximal NPXY directs LRP1 basolateral sorting from the TGN. A N26A mutant revealed that this NPXY motif recognized by SNX17 is required for the receptor’s exit from BSE. An endocytic Y63ATL66 motif also functions in basolateral recycling, in concert with an additional endocytic motif (LL86,87), by preventing LRP1 entry intothe transcytotic apical pathway. All this sorting information operates similarly in hippocampal neurons to mediate LRP1 somatodendritic distribution regardless of the absence of AP1B in neurons. LRP1 basolateral distribution results then from spatially and temporally segregation steps mediated by recognition of distinct tyrosine-based motifs. We also demonstrate a novel function of SNX17 in basolateral/somatodendritic recycling from a different compartment than AP1Bendosomes.