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Literature DB >> 34097400

The 2-Aminopyridine Nucleobase Improves Triple-Helical Recognition of RNA and DNA When Used Instead of Pseudoisocytosine in Peptide Nucleic Acids.

Christopher A Ryan¹, Nikita Brodyagin¹, Justin Lok¹, Eriks Rozners¹.

Abstract

Pseudoisocytosine (J), a neutral analogue of protonated cytosine, is currently the gold standard modified nucleobase in peptide nucleic acids (PNAs) for the formation of J·G-C triplets that are stable at physiological pH. This study shows that triple-helical recognition of RNA and DNA is significantly improved by using 2-aminopyridine (M) instead of J. The positively charged M forms 3-fold stronger M+·G-C triplets than J with uncompromised sequence selectivity. Replacement of six Js with Ms in a PNA 9-mer increased its binding affinity by ∼2 orders of magnitude. M-modified PNAs prefer binding double-stranded RNA over DNA and disfavor off-target binding to single-stranded nucleic acids. Taken together, the results show that M is a promising modified nucleobase that significantly improves triplex-forming PNAs and may provide breakthrough developments for therapeutic and biotechnology applications.

Entities: Chemical

Mesh：

Substances：

Year: 2021 PMID： 34097400 PMCID： PMC8673193 DOI： 10.1021/acs.biochem.1c00275

Source DB: PubMed Journal: Biochemistry ISSN： 0006-2960 Impact factor: 3.321

35 in total

1. Combined triplex/duplex invasion of double-stranded DNA by "tail-clamp" peptide nucleic acid.

Authors: Thomas Bentin; H Jakob Larsen; Peter E Nielsen
Journal: Biochemistry Date: 2003-12-02 Impact factor: 3.162

Review 2. Sequence-selective targeting of duplex DNA by peptide nucleic acids.

Authors: Peter E Nielsen
Journal: Curr Opin Mol Ther Date: 2010-04

Review 3. Addressing the challenges of cellular delivery and bioavailability of peptide nucleic acids (PNA).

Authors: Peter E Nielsen
Journal: Q Rev Biophys Date: 2006-04-06 Impact factor: 5.318

4. Incorporating G-C Pair-Recognizing Guanidinium into PNAs for Sequence and Structure Specific Recognition of dsRNAs over dsDNAs and ssRNAs.

Authors: Manchugondanahalli S Krishna; Zhenzhang Wang; Liangzhen Zheng; Jogesh Bowry; Alan Ann Lerk Ong; Yuguang Mu; Mookkan Prabakaran; Gang Chen
Journal: Biochemistry Date: 2019-08-28 Impact factor: 3.162

5. 1,8-Naphthyridin-2,7-(1,8H)-dione is an effective mimic of protonated cytosine in peptide nucleic acid triplex recognition systems.

Authors: Caspar Christensen; Anne B Eldrup; Gerald Haaima; Peter E Nielsen
Journal: Bioorg Med Chem Lett Date: 2002-11-04 Impact factor: 2.823

6. Recognition of GC base pairs by triplex forming oligonucleotides containing nucleosides derived from 2-aminopyridine.

Authors: S A Cassidy; P Slickers; J O Trent; D C Capaldi; P D Roselt; C B Reese; S Neidle; K R Fox
Journal: Nucleic Acids Res Date: 1997-12-15 Impact factor: 16.971

7. Triple-helical recognition of RNA using 2-aminopyridine-modified PNA at physiologically relevant conditions.

Authors: Thomas Zengeya; Pankaj Gupta; Eriks Rozners
Journal: Angew Chem Int Ed Engl Date: 2012-11-04 Impact factor: 15.336

8. Sequence selective recognition of double-stranded RNA at physiologically relevant conditions using PNA-peptide conjugates.

Authors: Oluwatoyosi Muse; Thomas Zengeya; Juddy Mwaura; Dziyana Hnedzko; Dennis W McGee; Christof T Grewer; Eriks Rozners
Journal: ACS Chem Biol Date: 2013-06-12 Impact factor: 5.100

The 2-Aminopyridine Nucleobase Improves Triple-Helical Recognition of RNA and DNA When Used Instead of Pseudoisocytosine in Peptide Nucleic Acids.

1. Combined triplex/duplex invasion of double-stranded DNA by "tail-clamp" peptide nucleic acid.

Review 2. Sequence-selective targeting of duplex DNA by peptide nucleic acids.

Review 3. Addressing the challenges of cellular delivery and bioavailability of peptide nucleic acids (PNA).

4. Incorporating G-C Pair-Recognizing Guanidinium into PNAs for Sequence and Structure Specific Recognition of dsRNAs over dsDNAs and ssRNAs.

5. 1,8-Naphthyridin-2,7-(1,8H)-dione is an effective mimic of protonated cytosine in peptide nucleic acid triplex recognition systems.

6. Recognition of GC base pairs by triplex forming oligonucleotides containing nucleosides derived from 2-aminopyridine.

7. Triple-helical recognition of RNA using 2-aminopyridine-modified PNA at physiologically relevant conditions.

8. Sequence selective recognition of double-stranded RNA at physiologically relevant conditions using PNA-peptide conjugates.

9. Sequence-selective recognition of DNA by strand displacement with a thymine-substituted polyamide.

10. Role of Pseudoisocytidine Tautomerization in Triplex-Forming Oligonucleotides: In Silico and in Vitro Studies.

1. Fluorobenzene Nucleobase Analogues for Triplex-Forming Peptide Nucleic Acids.

2. Cellular uptake of 2-aminopyridine-modified peptide nucleic acids conjugated with cell-penetrating peptides.