Two independent regions of HIV-1 Nef are required for connection with the endocytic pathway through binding to the mu 1 chain of AP1 complex

Two independent regions of HIV-1 Nef are required for connection with the endocytic pathway through binding to the mu 1 chain of AP1 complex

The Nef protein from the human immunodeficiency virus (HIV) induces down-regulation of the CD4 and major histocompatibility complex class I molecules from the cell surface by interfering with the endocytic machinery. This work focuses on the interaction of HIV-1 Nef with the mu 1 chain of adaptor pr...

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Bibliographic Details
Published in:Traffic (Copenhagen, Denmark) Vol. 1; no. 11; pp. 871 - 883
Main Authors: Erdtmann, L, Janvier, K, Raposo, G, Craig, H M, Benaroch, P, Berlioz-Torrent, C, Guatelli, J C, Benarous, R, Benichou, S
Format: Journal Article
Language:English
Published: England 01-11-2000
Subjects:
Adaptor Protein Complex 1
Adaptor Protein Complex alpha Subunits
Adaptor Proteins, Vesicular Transport
Amino Acid Sequence
Binding Sites - genetics
CD4 Antigens - metabolism
CD8 Antigens - genetics
CD8 Antigens - metabolism
Cell Compartmentation
Cell Nucleus - metabolism
Down-Regulation
Endocytosis - physiology
Endosomes - metabolism
Genes, nef
HeLa Cells
HIV-1 - genetics
HIV-1 - physiology
Human immunodeficiency virus 1
Humans
Membrane Proteins - metabolism
Microscopy, Immunoelectron
Molecular Sequence Data
Point Mutation
Recombinant Fusion Proteins - genetics
Recombinant Fusion Proteins - metabolism
Transfection
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Summary:The Nef protein from the human immunodeficiency virus (HIV) induces down-regulation of the CD4 and major histocompatibility complex class I molecules from the cell surface by interfering with the endocytic machinery. This work focuses on the interaction of HIV-1 Nef with the mu 1 chain of adaptor protein type 1 (AP1) complex and its contribution to the Nef-induced alterations of membrane trafficking. Two independent regions surrounding a disordered loop located in the C-terminal part of Nef are involved in mu 1 binding. Each region can separately interact with mu 1, and simultaneous point mutations within both regions are needed to abolish binding. We used CD8 chimeras in which the cytoplasmic tail was replaced by Nef mutants to show that these mu 1-binding sites contain determinants required to induce CD4 down-regulation and to target the chimera to the endocytic pathway by promoting AP1 complex recruitment. Ultrastructural analysis revealed that the CD8-Nef chimera provokes morphological alterations of the endosomal compartments and co-localizes with AP1 complexes. These data indicate that the recruitment by Nef of AP1 via binding to mu 1 participates in the connection of Nef with the endocytic pathway.
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ISSN:1398-9219
1600-0854
DOI:10.1034/j.1600-0854.2000.011106.x