Literature DB >> 21586796

A novel conserved targeting motif found in ABCA transporters mediates trafficking to early post-Golgi compartments.

Michael F Beers1, Arie Hawkins, Henry Shuman, Ming Zhao, Jennifer L Newitt, Jean Ann Maguire, Wenge Ding, Surafel Mulugeta.   

Abstract

The ATP binding cassette, class A (ABCA) proteins are homologous polytopic transmembrane transporters that function as lipid pumps at distinct subcellular sites in a variety of cells. Located within the N terminus of these transporters, there exists a highly conserved xLxxKN motif of unknown function. To define its role, human ABCA3 was employed as a primary model representing ABCA transporters, while mouse ABCA1 was utilized to support major findings. Transfection studies showed colocalization of both transporters with surfactant protein C (SP-C), a marker peptide for successful protein targeting to lysosomal-like organelles. In contrast, alanine mutation of xLxxKN resulted in endoplasmic reticulum retention. As proof of principle, swapping xLxxKN for the known lysosomal targeting motif of SP-C resulted in post-Golgi targeting of the SP-C chimera. However, these products failed to reach their terminal processing compartments, suggesting that the xLxxKN motif only serves as a Golgi exit signal. We propose a model whereby an N-terminal signal sequence, xLxxKN, directs ABCA transporters to a post-Golgi vesicular sorting station where additional signals may be required for selective delivery of individual transporters to final subcellular destinations.

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Year:  2011        PMID: 21586796      PMCID: PMC3139239          DOI: 10.1194/jlr.M013284

Source DB:  PubMed          Journal:  J Lipid Res        ISSN: 0022-2275            Impact factor:   5.922


  48 in total

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7.  Structural requirements for intracellular targeting of SP-C proprotein.

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Authors:  A F Kabore; W J Wang; S J Russo; M F Beers
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  11 in total

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7.  Cholesterol-binding molecules MLN64 and ORP1L mark distinct late endosomes with transporters ABCA3 and NPC1.

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