Membrane anchorage of gp160 is necessary and sufficient to prevent CD4 transport to the cell surface.

The HIV envelope glycoprotein gp160 plays a major role in the posttranslational down-regulation of its receptor, CD4. In this report we have analyzed the requirements of both CD4 and gp160 involved in transport block of the gp160-CD4 complex causing the down-regulation of cell surface CD4. Using a transient expression system we observed that both soluble and membrane-bound CD4 were equally blocked by the wild-type gp160, indicating that neither the transmembrane domain nor the cytoplasmic tail of CD4 affected its interaction with gp160 or exocytic transport block of the complex. Similarly, deletions of the gp160 cytoplasmic domain or mutation in the transmembrane domain had little effect on its transport, or its ability to down-regulate CD4 surface expression. Furthermore, substitution of the gp160 transmembrane domain and cytoplasmic tail with that of the influenza virus hemagglutinin or with a glycophosphatidylinositol moiety did not affect its ability to bind CD4 and block its transport. However, soluble envelope glycoprotein constructs (either gp120 or soluble gp160) were unable to block CD4 transport to the cell surface despite their binding to CD4 within the ER. Taken together these results demonstrate that neither the gp160 cytoplasmic tail nor the specific sequences of the transmembrane region of gp160 nor the membrane anchoring of CD4 were involved in ER retention of the CD4-gp160 complex and that anchoring of gp160 to the ER membrane was responsible for gp160-mediated cell surface down-regulation of CD4.