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Research Article

A simple ligand that selectively targets CUG trinucleotide repeats and inhibits MBNL protein binding

Jonathan F. Arambula, Sreenivasa Rao Ramisetty, Anne M. Baranger, and Steven C. Zimmerman
PNAS first published September 8, 2009; https://doi.org/10.1073/pnas.0901824106
Jonathan F. Arambula
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Sreenivasa Rao Ramisetty
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Anne M. Baranger
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  • For correspondence: baranger@illinois.edu sczimmer@illinois.edu
Steven C. Zimmerman
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  • For correspondence: baranger@illinois.edu sczimmer@illinois.edu
  1. Edited by Gregory A. Petsko, Brandeis University, Waltham, MA, and approved July 16, 2009 (received for review February 19, 2009)

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Abstract

This work describes the rational design, synthesis, and study of a ligand that selectively complexes CUG repeats in RNA (and CTG repeats in DNA) with high nanomolar affinity. This sequence is considered a causative agent of myotonic dystrophy type 1 (DM1) because of its ability to sequester muscleblind-like (MBNL) proteins. Ligand 1 was synthesized in two steps from commercially available compounds, and its binding to CTG and CUG repeats in oligonucleotides studied. Isothermal titration calorimetry studies of 1 with various sequences showed a preference toward the T-T mismatch (Kd of 390 ± 80 nM) with a 13-, 169-, and 85-fold reduction in affinity toward single C-C, A-A, and G-G mismatches, respectively. Binding and Job analysis of 1 to multiple CTG step sequences revealed high affinity binding to every other T-T mismatch with negative cooperativity for proximal T-T mismatches. The affinity of 1 for a (CUG)4 step provided a Kd of 430 nM with a binding stoichiometry of 1:1. The preference for the U-U in RNA was maintained with a 6-, >143-, and >143-fold reduction in affinity toward single C-C, A-A, and G-G mismatches, respectively. Ligand 1 destabilized the complexes formed between MBNL1N and (CUG)4 and (CUG)12 with IC50 values of 52 ± 20 μM and 46 ± 7 μM, respectively, and Ki values of 6 ± 2 μM and 7 ± 1 μM, respectively. These values were only minimally altered by the addition of competitor tRNA. Ligand 1 does not destabilize the unrelated RNA-protein complexes the U1A-SL2 RNA complex and the Sex lethal-tra RNA complex. Thus, ligand 1 selectively destabilizes the MBNL1N-poly(CUG) complex.

  • inhibition
  • MBNL1
  • molecular recognition
  • myotonic dystrophy
  • RNA

Footnotes

  • 1To whom correspondence may be addressed. E-mail: baranger{at}illinois.edu or sczimmer{at}illinois.edu
  • Author contributions: J.F.A., S.R.R., A.M.B., and S.C.Z. designed research; J.F.A. and S.R.R. performed research; J.F.A., S.R.R., A.M.B., and S.C.Z. analyzed data; and J.F.A., A.M.B., and S.C.Z. wrote the paper.

  • The authors declare no conflict of interest.

  • This article is a PNAS Direct Submission.

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A simple ligand that selectively targets CUG trinucleotide repeats and inhibits MBNL protein binding
Jonathan F. Arambula, Sreenivasa Rao Ramisetty, Anne M. Baranger, Steven C. Zimmerman
Proceedings of the National Academy of Sciences Sep 2009, pnas.0901824106; DOI: 10.1073/pnas.0901824106

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A simple ligand that selectively targets CUG trinucleotide repeats and inhibits MBNL protein binding
Jonathan F. Arambula, Sreenivasa Rao Ramisetty, Anne M. Baranger, Steven C. Zimmerman
Proceedings of the National Academy of Sciences Sep 2009, pnas.0901824106; DOI: 10.1073/pnas.0901824106
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