HIV-1 protease cleaves eukaryotic initiation factor 4G and inhibits cap-dependent translation

Several animal viruses inhibit host protein synthesis, but only some members of the picornavirus group are known to do so by cleaving translation initiation factor elF4G. Here we report that infection of human CD4(+) cells with HIV-1 also leads to proteolysis of elF4G and profound inhibition of cellular translation. Purified HIV-1 protease directly cleaves elF4GI at positions 678, 681, and 1086, separating the three domains of this initiation factor. Proteolysis of elF4GI by HIV-1 protease, as with poliovirus 2A protease, inhibits protein synthesis directed by capped mRNAs but allows internal ribosome entry site-driven translation. These findings indicate that HIV-1, a member of retrovirus group, shares with picornaviruses the capacity to proteolyze eIF4G.