Literature DB >> 28031466

Cell-based Fluorescence Complementation Reveals a Role for HIV-1 Nef Protein Dimerization in AP-2 Adaptor Recruitment and CD4 Co-receptor Down-regulation.

Sherry T Shu1, Lori A Emert-Sedlak1, Thomas E Smithgall2.   

Abstract

The HIV-1 Nef accessory factor enhances viral infectivity, immune evasion, and AIDS progression. Nef triggers rapid down-regulation of CD4 via the endocytic adaptor protein 2 (AP-2) complex, a process linked to enhanced viral infectivity and immune escape. Here, we describe a bimolecular fluorescence complementation (BiFC) assay to visualize the interaction of Nef with AP-2 and CD4 in living cells. Interacting protein pairs were fused to complementary non-fluorescent fragments of YFP and co-expressed in 293T cells. Nef interactions with both CD4 and AP-2 resulted in complementation of YFP and a bright fluorescent signal by confocal microcopy that localized to the cell periphery. Co-expression of the AP-2 α subunit enhanced the Nef·AP-2 σ2 subunit BiFC signal and vice versa, suggesting that the AP-2 α-σ2 hemicomplex interacts cooperatively with Nef. Mutagenesis of Nef amino acids Arg-134, Glu-174, and Asp-175, which stabilize Nef for AP-2 α-σ2 binding in a recent co-crystal structure, substantially reduced AP-2 interaction without affecting CD4 binding. A dimerization-defective mutant of Nef failed to interact with either CD4 or AP-2 in the BiFC assay, indicating that Nef quaternary structure is required for CD4 and AP-2 recruitment as well as CD4 down-regulation. A small molecule previously shown to bind the Nef dimerization interface also reduced Nef interactions with AP-2 and CD4 and restored CD4 expression to the surface of HIV-infected cells. Our findings provide a mechanistic explanation for previous observations that dimerization-defective Nef mutants fail to down-regulate CD4 and validate the Nef dimerization interface as a target site for antiretroviral drug development.
© 2017 by The American Society for Biochemistry and Molecular Biology, Inc.

Entities:  

Keywords:  AP-2; Nef; bimolecular fluorescence complementation; cluster of differentiation 4 (CD4); dimerization; endocytosis; human immunodeficiency virus (HIV); protein-protein interaction

Mesh:

Substances:

Year:  2016        PMID: 28031466      PMCID: PMC5314165          DOI: 10.1074/jbc.M116.770016

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  41 in total

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Authors:  K L Collins; B K Chen; S A Kalams; B D Walker; D Baltimore
Journal:  Nature       Date:  1998-01-22       Impact factor: 49.962

Review 5.  Cargo adaptors: structures illuminate mechanisms regulating vesicle biogenesis.

Authors:  Jon E Paczkowski; Brian C Richardson; J Christopher Fromme
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Authors:  S Arold; P Franken; M P Strub; F Hoh; S Benichou; R Benarous; C Dumas
Journal:  Structure       Date:  1997-10-15       Impact factor: 5.006

7.  A new reporter cell line to monitor HIV infection and drug susceptibility in vitro.

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8.  HIV-1 Nef dimerization is required for Nef-mediated receptor downregulation and viral replication.

Authors:  Jerrod A Poe; Thomas E Smithgall
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Review 6.  Plasma Membrane-Associated Restriction Factors and Their Counteraction by HIV-1 Accessory Proteins.

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7.  Structural basis of CD4 downregulation by HIV-1 Nef.

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9.  A single β-octyl glucoside molecule induces HIV-1 Nef dimer formation in the absence of partner protein binding.

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  9 in total

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