Publication

Lack of synergy for inhibitors targeting a multi-drug-resistant HIV-1 protease

King, Nancy M.
Melnick, Laurence
Prabu-Jeyabalan, Moses
Nalivaika, Ellen A.
Yang, Shiow-Shong
Gao, Yun
Nie, Xiaoyi
Zepp, Charles
Heefner, Donald L.
Schiffer, Celia A.
Embargo Expiration Date
Abstract

The three-dimensional structures of indinavir and three newly synthesized indinavir analogs in complex with a multi-drug-resistant variant (L63P, V82T, I84V) of HIV-1 protease were determined to approximately 2.2 A resolution. Two of the three analogs have only a single modification of indinavir, and their binding affinities to the variant HIV-1 protease are enhanced over that of indinavir. However, when both modifications were combined into a single compound, the binding affinity to the protease variant was reduced. On close examination, the structural rearrangements in the protease that occur in the tightest binding inhibitor complex are mutually exclusive with the structural rearrangements seen in the second tightest inhibitor complex. This occurs as adaptations in the S1 pocket of one monomer propagate through the dimer and affect the conformation of the S1 loop near P81 of the other monomer. Therefore, structural rearrangements that occur within the protease when it binds to an inhibitor with a single modification must be accounted for in the design of inhibitors with multiple modifications. This consideration is necessary to develop inhibitors that bind sufficiently tightly to drug-resistant variants of HIV-1 protease to potentially become the next generation of therapeutic agents.

Source

Protein Sci. 2002 Feb;11(2):418-29. Link to article on publisher's website

Year of Medical School at Time of Visit
Sponsors
Dates of Travel
DOI
10.1110/ps.25502
PubMed ID
11790852
Other Identifiers
Notes
Funding and Acknowledgements
Corresponding Author
Related Resources
Related Resources
Repository Citation
Rights
Distribution License