Issue 37, 2013

Targeting folded RNA: a branched peptideboronic acid that binds to a large surface area of HIV-1 RRE RNA

Abstract

On-bead high-throughput screening of a medium-sized (1000–2000 Da) branched peptideboronic acid (BPBA) library consisting of 46 656 unique sequences against HIV-1 RRE RNA generated peptides with binding affinities in the low micromolar range. In particular, BPBA1 had a Kd of 1.4 μM with RRE IIB, preference for RNA over DNA (27 fold), and selectivity of up to >75 fold against a panel of RRE IIB variants. Structure–activity studies suggest that the boronic acid moiety and “branching” in peptides are key structural features for efficient binding and selectivity for the folded RNA target. BPBA1 was efficiently taken up by HeLa and A2780 cells. RNA-footprinting studies revealed that the BPBA1 binding site encompasses a large surface area that spans both the upper stem as well as the internal loop regions of RRE IIB.

Graphical abstract: Targeting folded RNA: a branched peptideboronic acid that binds to a large surface area of HIV-1 RRE RNA

Supplementary files

Article information

Article type
Paper
Submitted
21 May 2013
Accepted
01 Aug 2013
First published
02 Aug 2013
This article is Open Access
Creative Commons BY-NC license

Org. Biomol. Chem., 2013,11, 6263-6271

Targeting folded RNA: a branched peptideboronic acid that binds to a large surface area of HIV-1 RRE RNA

W. Zhang, D. I. Bryson, J. B. Crumpton, J. Wynn and W. L. Santos, Org. Biomol. Chem., 2013, 11, 6263 DOI: 10.1039/C3OB41053F

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