About this item:

107 Views | 60 Downloads

Author Notes:

karen.anderson@yale.edu; Tel.: +1-203-785-4526

We thank Sheida Amiralaei for assisting with the synthesis and characterization of the FTC nucleotides. The authors are grateful to Stefan G. Sarafianos for providing access to the RT construct.

Conceptualization, N.B. and K.S.A.; methodology, N.B. and A.H.C.; validation, N.B., A.H.C., R.F.S. and K.S.A.; formal analysis, N.B.; investigation, N.B. and A.H.C.; resources, R.F.S. and K.S.A.; writing—original draft preparation, N.B.; writing—review and editing, K.S.A. and R.F.S.; visualization, N.B.; supervision, K.S.A.; funding acquisition, K.S.A. and R.F.S. All authors have read and agreed to the published version of the manuscript.

The authors declare no conflict of interest

Subjects:

Research Funding:

Crystals screening was conducted with support from the Yale Macromolecular X-ray Core Facility (1S10OD018007-01). This research used resources FMX of the National Synchrotron Light Source II, a U.S. Department of Energy (DOE) Office of Science User Facility operated for the DOE Office of Science by Brookhaven National Laboratory under contract no. DE-SC0012704. The Life Science Biomedical Technology Research resource is primarily supported by the National Institute of Health, National Institute of General Medical Sciences (NIGMS) through a Center Core P30 Grant (P30GM133893), and by the DOE Office of Biological and Environmental Research (KP1605010). This work is also based upon research conducted at the Northeastern Collaborative Access Team beamlines, which are funded by the National Institute of General Medical Sciences from the National Institutes of Health (P30 GM124165). The Eiger 16M detector on the 24-ID-E beam line is funded by a NIH-ORIP HEI grant (S10OD021527). This research used resources of the Advanced Photon Source, a U.S. Department of Energy (DOE) Office of Science User Facility operated for the DOE Office of Science by Argonne National Laboratory under contract no. DE-AC02-06CH11357.

This research was funded by National Institutes of Health (NIH), grant number AI155072 and 5P30-AI-50409.

Keywords:

  • Science & Technology
  • Life Sciences & Biomedicine
  • Physical Sciences
  • Biochemistry & Molecular Biology
  • Chemistry, Multidisciplinary
  • Chemistry
  • nucleoside reverse transcriptase inhibitors
  • emtricitabine
  • stavudine
  • inhibitor-protein complexes
  • macromolecular X-ray crystallography
  • STRUCTURAL BASIS
  • INHIBITION
  • TRANSLOCATION
  • AZT
  • DNA

Post-Catalytic Complexes with Emtricitabine or Stavudine and HIV-1 Reverse Transcriptase Reveal New Mechanistic Insights for Nucleotide Incorporation and Drug Resistance

Tools:

Share

Journal Title:

MOLECULES

Volume:

Volume 25, Number 20

Publisher:

Type of Work:

Article | Final Publisher PDF

Abstract:

Human immunodeficiency virus 1 (HIV-1) infection is a global health issue since neither a cure nor a vaccine is available. However, the highly active antiretroviral therapy (HAART) has improved the life expectancy for patients with acquired immunodeficiency syndrome (AIDS). Nucleoside reverse transcriptase inhibitors (NRTIs) are in almost all HAART and target reverse transcriptase (RT), an essential enzyme for the virus. Even though NRTIs are highly effective, they have limitations caused by RT resistance. The main mechanisms of RT resistance to NRTIs are discrimination and excision. Understanding the molecular mechanisms for discrimination and excision are essential to develop more potent and selective NRTIs. Using protein X-ray crystallography, we determined the first crystal structure of RT in its post-catalytic state in complex with emtricitabine, (-)FTC or stavudine (d4T). Our structural studies provide the framework for understanding how RT discriminates between NRTIs and natural nucleotides, and for understanding the requirement of (-)FTC to undergo a conformation change for successful incorporation by RT. The crystal structure of RT in post-catalytic complex with d4T provides a “snapshot” for considering the possible mechanism of how RT develops resistance for d4T via excision. The findings reported herein will contribute to the development of next generation NRTIs.

Copyright information:

© 2020 by the authors.

This is an Open Access work distributed under the terms of the Creative Commons Attribution 4.0 International License (https://creativecommons.org/licenses/by/4.0/rdf).
Export to EndNote
Site Statistics

Copyright © 2016 Emory University - All Rights Reserved
540 Asbury Circle, Atlanta, GA 30322-2870
(404) 727-6861
Privacy Policy | Terms & Conditions

v2.2.8-dev

Contact Us
Download now