An ultra-high affinity ligand of HIV-1 TAR reveals the RNA structure recognized by P-TEFb

The HIV-1 trans-activator protein Tat binds the trans-activation response element (TAR) to facilitate recruitment of the super elongation complex (SEC) to enhance transcription of the integrated pro-viral genome. The Tat–TAR interaction is critical for viral replication and the emergence of the viru...

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Autores principales: Shortridge, Matthew D, Wille, Paul T, Jones, Alisha N, Davidson, Amy, Bogdanovic, Jasmina, Arts, Eric, Karn, Jonathan, Robinson, John A, Varani, Gabriele
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2019
Materias:
RNA and RNA-protein complexes
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6379670/
https://www.ncbi.nlm.nih.gov/pubmed/30481318
http://dx.doi.org/10.1093/nar/gky1197
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author Shortridge, Matthew D
Wille, Paul T
Jones, Alisha N
Davidson, Amy
Bogdanovic, Jasmina
Arts, Eric
Karn, Jonathan
Robinson, John A
Varani, Gabriele
author_facet Shortridge, Matthew D
Wille, Paul T
Jones, Alisha N
Davidson, Amy
Bogdanovic, Jasmina
Arts, Eric
Karn, Jonathan
Robinson, John A
Varani, Gabriele
author_sort Shortridge, Matthew D
collection PubMed
description The HIV-1 trans-activator protein Tat binds the trans-activation response element (TAR) to facilitate recruitment of the super elongation complex (SEC) to enhance transcription of the integrated pro-viral genome. The Tat–TAR interaction is critical for viral replication and the emergence of the virus from the latent state, therefore, inhibiting this interaction has long been pursued to discover new anti-viral or latency reversal agents. However, discovering active compounds that directly target RNA with high affinity and selectivity remains a significant challenge; limiting pre-clinical development. Here, we report the rational design of a macrocyclic peptide mimic of the arginine rich motif of Tat, which binds to TAR with low pM affinity and 100-fold selectivity against closely homologous RNAs. Despite these unprecedented binding properties, the new ligand (JB181) only moderately inhibits Tat-dependent reactivation in cells and recruitment of positive transcription elongation factor (P-TEFb) to TAR. The NMR structure of the JB181–TAR complex revealed that the ligand induces a structure in the TAR loop that closely mimics the P-TEFb/Tat1:57/AFF4/TAR complex. These results strongly suggest that high-affinity ligands which bind the UCU bulge are not likely to inhibit recruitment of the SEC and suggest that targeting of the TAR loop will be an essential feature of effective Tat inhibitors.
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spelling pubmed-63796702019-02-22 An ultra-high affinity ligand of HIV-1 TAR reveals the RNA structure recognized by P-TEFb Shortridge, Matthew D Wille, Paul T Jones, Alisha N Davidson, Amy Bogdanovic, Jasmina Arts, Eric Karn, Jonathan Robinson, John A Varani, Gabriele Nucleic Acids Res RNA and RNA-protein complexes The HIV-1 trans-activator protein Tat binds the trans-activation response element (TAR) to facilitate recruitment of the super elongation complex (SEC) to enhance transcription of the integrated pro-viral genome. The Tat–TAR interaction is critical for viral replication and the emergence of the virus from the latent state, therefore, inhibiting this interaction has long been pursued to discover new anti-viral or latency reversal agents. However, discovering active compounds that directly target RNA with high affinity and selectivity remains a significant challenge; limiting pre-clinical development. Here, we report the rational design of a macrocyclic peptide mimic of the arginine rich motif of Tat, which binds to TAR with low pM affinity and 100-fold selectivity against closely homologous RNAs. Despite these unprecedented binding properties, the new ligand (JB181) only moderately inhibits Tat-dependent reactivation in cells and recruitment of positive transcription elongation factor (P-TEFb) to TAR. The NMR structure of the JB181–TAR complex revealed that the ligand induces a structure in the TAR loop that closely mimics the P-TEFb/Tat1:57/AFF4/TAR complex. These results strongly suggest that high-affinity ligands which bind the UCU bulge are not likely to inhibit recruitment of the SEC and suggest that targeting of the TAR loop will be an essential feature of effective Tat inhibitors. Oxford University Press 2019-02-20 2018-11-27 /pmc/articles/PMC6379670/ /pubmed/30481318 http://dx.doi.org/10.1093/nar/gky1197 Text en © The Author(s) 2018. Published by Oxford University Press on behalf of Nucleic Acids Research. http://creativecommons.org/licenses/by/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted reuse, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle RNA and RNA-protein complexes
Shortridge, Matthew D
Wille, Paul T
Jones, Alisha N
Davidson, Amy
Bogdanovic, Jasmina
Arts, Eric
Karn, Jonathan
Robinson, John A
Varani, Gabriele
An ultra-high affinity ligand of HIV-1 TAR reveals the RNA structure recognized by P-TEFb
title An ultra-high affinity ligand of HIV-1 TAR reveals the RNA structure recognized by P-TEFb
title_full An ultra-high affinity ligand of HIV-1 TAR reveals the RNA structure recognized by P-TEFb
title_fullStr An ultra-high affinity ligand of HIV-1 TAR reveals the RNA structure recognized by P-TEFb
title_full_unstemmed An ultra-high affinity ligand of HIV-1 TAR reveals the RNA structure recognized by P-TEFb
title_short An ultra-high affinity ligand of HIV-1 TAR reveals the RNA structure recognized by P-TEFb
title_sort ultra-high affinity ligand of hiv-1 tar reveals the rna structure recognized by p-tefb
topic RNA and RNA-protein complexes
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6379670/
https://www.ncbi.nlm.nih.gov/pubmed/30481318
http://dx.doi.org/10.1093/nar/gky1197
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