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C5-Substituted 2-Selenouridines Ensure Efficient Base Pairing with Guanosine; Consequences for Reading the NNG-3′ Synonymous mRNA Codons

5-Substituted 2-selenouridines (R5Se2U) are post-transcriptional modifications present in the first anticodon position of transfer RNA. Their functional role in the regulation of gene expression is elusive. Here, we present efficient syntheses of 5-methylaminomethyl-2-selenouridine (1, mnm5Se2U), 5-...

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Autores principales: Leszczynska, Grazyna, Cypryk, Marek, Gostynski, Bartlomiej, Sadowska, Klaudia, Herman, Paulina, Bujacz, Grzegorz, Lodyga-Chruscinska, Elzbieta, Sochacka, Elzbieta, Nawrot, Barbara
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7216251/
https://www.ncbi.nlm.nih.gov/pubmed/32326096
http://dx.doi.org/10.3390/ijms21082882
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author Leszczynska, Grazyna
Cypryk, Marek
Gostynski, Bartlomiej
Sadowska, Klaudia
Herman, Paulina
Bujacz, Grzegorz
Lodyga-Chruscinska, Elzbieta
Sochacka, Elzbieta
Nawrot, Barbara
author_facet Leszczynska, Grazyna
Cypryk, Marek
Gostynski, Bartlomiej
Sadowska, Klaudia
Herman, Paulina
Bujacz, Grzegorz
Lodyga-Chruscinska, Elzbieta
Sochacka, Elzbieta
Nawrot, Barbara
author_sort Leszczynska, Grazyna
collection PubMed
description 5-Substituted 2-selenouridines (R5Se2U) are post-transcriptional modifications present in the first anticodon position of transfer RNA. Their functional role in the regulation of gene expression is elusive. Here, we present efficient syntheses of 5-methylaminomethyl-2-selenouridine (1, mnm5Se2U), 5-carboxymethylaminomethyl-2-selenouridine (2, cmnm5Se2U), and Se2U (3) alongside the crystal structure of the latter nucleoside. By using pH-dependent potentiometric titration, pKa values for the N3H groups of 1–3 were assessed to be significantly lower compared to their 2-thio- and 2-oxo-congeners. At physiological conditions (pH 7.4), Se2-uridines 1 and 2 preferentially adopted the zwitterionic form (ZI, ca. 90%), with the positive charge located at the amino alkyl side chain and the negative charge at the Se2-N3-O4 edge. As shown by density functional theory (DFT) calculations, this ZI form efficiently bound to guanine, forming the so-called “new wobble base pair”, which was accepted by the ribosome architecture. These data suggest that the tRNA anticodons with wobble R5Se2Us may preferentially read the 5′-NNG-3′ synonymous codons, unlike their 2-thio- and 2-oxo-precursors, which preferentially read the 5′-NNA-3′ codons. Thus, the interplay between the levels of U-, S2U- and Se2U-tRNA may have a dominant role in the epitranscriptomic regulation of gene expression via reading of the synonymous 3′-A- and 3′-G-ending codons.
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spelling pubmed-72162512020-05-22 C5-Substituted 2-Selenouridines Ensure Efficient Base Pairing with Guanosine; Consequences for Reading the NNG-3′ Synonymous mRNA Codons Leszczynska, Grazyna Cypryk, Marek Gostynski, Bartlomiej Sadowska, Klaudia Herman, Paulina Bujacz, Grzegorz Lodyga-Chruscinska, Elzbieta Sochacka, Elzbieta Nawrot, Barbara Int J Mol Sci Article 5-Substituted 2-selenouridines (R5Se2U) are post-transcriptional modifications present in the first anticodon position of transfer RNA. Their functional role in the regulation of gene expression is elusive. Here, we present efficient syntheses of 5-methylaminomethyl-2-selenouridine (1, mnm5Se2U), 5-carboxymethylaminomethyl-2-selenouridine (2, cmnm5Se2U), and Se2U (3) alongside the crystal structure of the latter nucleoside. By using pH-dependent potentiometric titration, pKa values for the N3H groups of 1–3 were assessed to be significantly lower compared to their 2-thio- and 2-oxo-congeners. At physiological conditions (pH 7.4), Se2-uridines 1 and 2 preferentially adopted the zwitterionic form (ZI, ca. 90%), with the positive charge located at the amino alkyl side chain and the negative charge at the Se2-N3-O4 edge. As shown by density functional theory (DFT) calculations, this ZI form efficiently bound to guanine, forming the so-called “new wobble base pair”, which was accepted by the ribosome architecture. These data suggest that the tRNA anticodons with wobble R5Se2Us may preferentially read the 5′-NNG-3′ synonymous codons, unlike their 2-thio- and 2-oxo-precursors, which preferentially read the 5′-NNA-3′ codons. Thus, the interplay between the levels of U-, S2U- and Se2U-tRNA may have a dominant role in the epitranscriptomic regulation of gene expression via reading of the synonymous 3′-A- and 3′-G-ending codons. MDPI 2020-04-20 /pmc/articles/PMC7216251/ /pubmed/32326096 http://dx.doi.org/10.3390/ijms21082882 Text en © 2020 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Leszczynska, Grazyna
Cypryk, Marek
Gostynski, Bartlomiej
Sadowska, Klaudia
Herman, Paulina
Bujacz, Grzegorz
Lodyga-Chruscinska, Elzbieta
Sochacka, Elzbieta
Nawrot, Barbara
C5-Substituted 2-Selenouridines Ensure Efficient Base Pairing with Guanosine; Consequences for Reading the NNG-3′ Synonymous mRNA Codons
title C5-Substituted 2-Selenouridines Ensure Efficient Base Pairing with Guanosine; Consequences for Reading the NNG-3′ Synonymous mRNA Codons
title_full C5-Substituted 2-Selenouridines Ensure Efficient Base Pairing with Guanosine; Consequences for Reading the NNG-3′ Synonymous mRNA Codons
title_fullStr C5-Substituted 2-Selenouridines Ensure Efficient Base Pairing with Guanosine; Consequences for Reading the NNG-3′ Synonymous mRNA Codons
title_full_unstemmed C5-Substituted 2-Selenouridines Ensure Efficient Base Pairing with Guanosine; Consequences for Reading the NNG-3′ Synonymous mRNA Codons
title_short C5-Substituted 2-Selenouridines Ensure Efficient Base Pairing with Guanosine; Consequences for Reading the NNG-3′ Synonymous mRNA Codons
title_sort c5-substituted 2-selenouridines ensure efficient base pairing with guanosine; consequences for reading the nng-3′ synonymous mrna codons
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7216251/
https://www.ncbi.nlm.nih.gov/pubmed/32326096
http://dx.doi.org/10.3390/ijms21082882
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