A Model of HIV-I Reverse Transcriptase: Possible Mechanisms for AZT Resistance

摘要

In this report we present our preliminary results on the explanation of possible roles that mutations at positions 41, 67, 70, 215, and 219 of the p66 subunit of HIV-I reverse transcriptase play in AZT resistance. These explanations stem from molecular modeling studies of AZT in both the active site of our full-coordinate model, and in the channel to the active site. These results suggest the following: (a) that mutant residues Arg 70, Tyr 215, and possibly Leu 41, slerically block the opening to theactive site and help reverse transcriptase selectively exclude AZT due to its larger 3' group compared to normal nucleotides, (b) the loss of the positively charged lysine ammonium head group in the Lys 219 —> Gln mutation removes a favorable monopole-dipole interaction with the 3' azido group of AZT, and (c) the mutant residue Asn 67 can hydrogen bond to the single-stranded template of the template-primer complex and constrains the p3-p4 loop into a conformation which disallows AZT uptake.