Q1M003 · Q1M003_9HIV1

Function

function

Bypasses host T-cell signaling by inducing a transcriptional program nearly identical to that of anti-CD3 cell activation. Interaction with TCR-zeta chain up-regulates the Fas ligand (FasL). Increasing surface FasL molecules and decreasing surface MHC-I molecules on infected CD4+ cells send attacking cytotoxic CD8+ T-lymphocytes into apoptosis.
Extracellular Nef protein targets CD4+ T-lymphocytes for apoptosis by interacting with CXCR4 surface receptors.
Factor of infectivity and pathogenicity, required for optimal virus replication. Alters numerous pathways of T-lymphocyte function and down-regulates immunity surface molecules in order to evade host defense and increase viral infectivity. Alters the functionality of other immunity cells, like dendritic cells, monocytes/macrophages and NK cells.
In infected CD4+ T-lymphocytes, down-regulates the surface MHC-I, mature MHC-II, CD4, CD28, CCR5 and CXCR4 molecules. Mediates internalization and degradation of host CD4 through the interaction of with the cytoplasmic tail of CD4, the recruitment of AP-2 (clathrin adapter protein complex 2), internalization through clathrin coated pits, and subsequent transport to endosomes and lysosomes for degradation. Diverts host MHC-I molecules to the trans-Golgi network-associated endosomal compartments by an endocytic pathway to finally target them for degradation. MHC-I down-regulation may involve AP-1 (clathrin adapter protein complex 1) or possibly Src family kinase-ZAP70/Syk-PI3K cascade recruited by PACS2. In consequence infected cells are masked for immune recognition by cytotoxic T-lymphocytes. Decreasing the number of immune receptors also prevents reinfection by more HIV particles (superinfection). Down-regulates host SERINC3 and SERINC5 thereby excluding these proteins from the viral particles. Virion infectivity is drastically higher when SERINC3 or SERINC5 are excluded from the viral envelope, because these host antiviral proteins impair the membrane fusion event necessary for subsequent virion penetration.
Plays a role in optimizing the host cell environment for viral replication without causing cell death by apoptosis. Protects the infected cells from apoptosis in order to keep them alive until the next virus generation is ready to strike. Inhibits the Fas and TNFR-mediated death signals by blocking MAP3K5/ASK1. Decreases the half-life of TP53, protecting the infected cell against p53-mediated apoptosis. Inhibits the apoptotic signals regulated by the Bcl-2 family proteins through the formation of a Nef/PI3-kinase/PAK2 complex that leads to activation of PAK2 and induces phosphorylation of host BAD.

Miscellaneous

HIV-1 lineages are divided in three main groups, M (for Major), O (for Outlier), and N (for New, or Non-M, Non-O). The vast majority of strains found worldwide belong to the group M. Group O seems to be endemic to and largely confined to Cameroon and neighboring countries in West Central Africa, where these viruses represent a small minority of HIV-1 strains. The group N is represented by a limited number of isolates from Cameroonian persons. The group M is further subdivided in 9 clades or subtypes (A to D, F to H, J and K).

Caution

Lacks conserved residue(s) required for the propagation of feature annotation.

Features

Showing features for site.

TypeIDPosition(s)Description
Site18Might play a role in AP-1 recruitment to the Nef-MHC-I complex
Site60-61Cleavage; by viral protease

GO annotations

AspectTerm
Cellular Componentextracellular region
Cellular Componenthost cell Golgi membrane
Cellular Componenthost cell plasma membrane
Cellular Componentmembrane
Cellular Componentvirion component
Molecular FunctionGTP binding
Molecular FunctionSH3 domain binding
Biological Processapoptotic process
Biological Processsuppression by virus of host autophagy
Biological Processsymbiont-mediated suppression of host antigen processing and presentation of peptide antigen via MHC class I
Biological Processsymbiont-mediated suppression of host antigen processing and presentation of peptide antigen via MHC class II
Biological Processvirus-mediated perturbation of host defense response

Keywords

Names & Taxonomy

Protein names

  • Recommended name
    Protein Nef
  • Alternative names
    • 3'ORF
    • Negative factor
      (F-protein
      )
  • Cleaved into 1 chains

Gene names

    • Name
      nef

Organism names

Accessions

  • Primary accession
    Q1M003

Proteomes

Subcellular Location

Host cell membrane
; Lipid-anchor
Virion
Secreted
Host Golgi apparatus membrane
Note: TGN localization requires PACS1. Associates with the inner plasma membrane through its N-terminal domain. Nef stimulates its own export via the release of exosomes. Incorporated in virions at a rate of about 10 molecules per virion, where it is cleaved.

Keywords

PTM/Processing

Features

Showing features for initiator methionine, lipidation, chain, modified residue.

TypeIDPosition(s)Description
Initiator methionine1Removed; by host
Lipidation2N-myristoyl glycine; by host
ChainPRO_50235205392-209Protein Nef
Modified residue6Phosphoserine; by host
ChainPRO_502352054061-209C-terminal core protein

Post-translational modification

Myristoylated.
Phosphorylated on serine residues, probably by host PKCdelta and theta.
The virion-associated Nef proteins are cleaved by the viral protease to release the soluble C-terminal core protein. Nef is probably cleaved concomitantly with viral structural proteins on maturation of virus particles.

Keywords

Expression

Induction

Expressed early in the viral replication cycle.

Keywords

Interaction

Subunit

Monomer; cytosolic form. Homodimer; membrane bound form. Interacts with Nef associated p21-activated kinase (PAK2); this interaction activates PAK2. Associates with the Nef-MHC-I-AP1 complex; this complex is required for MHC-I internalization. Interacts (via C-terminus) with host PI3-kinase. Interacts with host PACS1; this interaction seems to be weak. Interacts with host PACS2. Interacts with host LCK and MAPK3; these interactions inhibit the kinase activity of the latter. Interacts with host ATP6V1H; this interaction may play a role in CD4 endocytosis. Associates with the CD4-Nef-AP2 complex; this complex is required for CD4 internalization. Interacts with host AP2 subunit alpha and AP2 subunit sigma2. Interacts with TCR-zeta chain; this interaction up-regulates the Fas ligand (FasL) surface expression. Interacts with host HCK, LYN, and SRC; these interactions activate the Src family kinases. Interacts with MAP3K5; this interaction inhibits the Fas and TNFR-mediated death signals. Interacts with beta-COP and PTE1. Interacts with human RACK1; this increases Nef phosphorylation by PKC. Interacts with TP53; this interaction decreases the half-life of TP53, protecting the infected cell against p53-mediated apoptosis.

Family & Domains

Features

Showing features for region, motif.

TypeIDPosition(s)Description
Region1-26Disordered
Region73-82SH3-binding; interaction with Src family tyrosine kinases
Motif76-79PxxP; stabilizes the interaction of NEF/MHC-I with host AP1M1; necessary for MHC-I internalization
Region112-128Mediates dimerization, Nef-PTE1 interaction
Region152-184Binding to ATP6V1H
Motif168-169Dileucine internalization motif; necessary for CD4 internalization
Motif178-179Diacidic; necessary for CD4 internalization

Domain

The N-terminal domain is composed of the N-myristoyl glycine and of a cluster of positively charged amino acids. It is required for inner plasma membrane targeting of Nef and virion incorporation, and thereby for infectivity. This domain is also involved in binding to TP53.
The SH3-binding domain constituted of PxxP motifs mediates binding to several Src family proteins thereby regulating their tyrosine kinase activity. The same motifs also mediates the association with MAPK3, PI3-kinase and TCR-zeta.
The acidic region binds to the sorting protein PACS-2, which targets Nef to the paranuclear region, enabling the PxxP motif to direct assembly of an SFK/ZAP-70/PI3K complex that accelerates endocytosis of cell-surface MHC-I.
The dileucine internalization motif and a diacidic motif seem to be required for binding to AP-2.

Sequence similarities

Belongs to the lentivirus primate group Nef protein family.

Keywords

Family and domain databases

Sequence

  • Sequence status
    Complete
  • Length
    209
  • Mass (Da)
    23,622
  • Last updated
    2006-05-30 v1
  • Checksum
    2848DE2BC55D20AA
MGGKWSKNRGWANVRERMRQTPTTEGVQVADGVGAVSQELAARGAVTSSNTAANNPTCAWLEAQEEAEDVGFPVRPQVPLRPMTYKGAFDLGFFLKEKGGLDGLIWSQKRQDILDLWVYHTQGYFPDWQNYTPGPGTRFPLTFGWCFKLVPVNPSEVEEATEGENNCLLHPICQHGIEDPEKEVLKWVFDSSLARRHIARELHPEYYKN

Sequence databases

Nucleotide SequenceProtein SequenceMolecule TypeStatus
AY945739
EMBL· GenBank· DDBJ
AAY25809.1
EMBL· GenBank· DDBJ
Genomic DNA

Similar Proteins

Disclaimer

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