Literature DB >> 29243925

In Vitro Bypass of Thymidine Glycol by DNA Polymerase θ Forms Sequence-Dependent Frameshift Mutations.

Daniel J Laverty1, Marc M Greenberg1.   

Abstract

Unrepaired DNA lesions block replication and threaten genomic stability. Several specialized translesion polymerases, including polymerase θ (Pol θ), contribute to replicative bypass of these lesions. The role of Pol θ in double-strand break repair is well-understood, but its contribution to translesion synthesis is much less so. We describe the action of Pol θ on templates containing thymidine glycol (Tg), a major cytotoxic, oxidative DNA lesion that blocks DNA replication. Unrepaired Tg lesions are bypassed in human cells by specialized translesion polymerases by one of two distinct pathways: high-fidelity bypass by the combined action of Pol κ and Pol ζ or weakly mutagenic bypass by Pol θ. Here we report that in vitro bypass of Tg by Pol θ results in frameshift mutations (deletions) in a sequence-dependent fashion. Steady-state kinetic analysis indicated that one- and two-nucleotide deletions are formed 9- and 6-fold more efficiently, respectively, than correct, full-length bypass products. Sequencing of in vitro bypass products revealed that bypass preference decreased in the following order on a template where all three outcomes were possible: two-nucleotide deletion > correct bypass > one-nucleotide deletion. These results suggest that bypass of Tg by Pol θ results in mutations opposite the lesion, as well as frameshift mutations.

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Year:  2017        PMID: 29243925      PMCID: PMC5743609          DOI: 10.1021/acs.biochem.7b01093

Source DB:  PubMed          Journal:  Biochemistry        ISSN: 0006-2960            Impact factor:   3.162


  39 in total

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2.  Human DNA polymerase kappa encircles DNA: implications for mismatch extension and lesion bypass.

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6.  Oxidative damage to DNA: relation to species metabolic rate and life span.

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Authors:  Karl E Zahn; April M Averill; Pierre Aller; Richard D Wood; Sylvie Doublié
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8.  Interconversion of the cis-5R,6S- and trans-5R,6R-thymine glycol lesions in duplex DNA.

Authors:  Kyle L Brown; Travis Adams; Vijay P Jasti; Ashis K Basu; Michael P Stone
Journal:  J Am Chem Soc       Date:  2008-08-06       Impact factor: 15.419

9.  Novel nuclear and mitochondrial glycosylases revealed by disruption of the mouse Nth1 gene encoding an endonuclease III homolog for repair of thymine glycols.

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Journal:  EMBO J       Date:  2002-07-01       Impact factor: 11.598

10.  Homologous-recombination-deficient tumours are dependent on Polθ-mediated repair.

Authors:  Raphael Ceccaldi; Jessica C Liu; Ravindra Amunugama; Ildiko Hajdu; Benjamin Primack; Mark I R Petalcorin; Kevin W O'Connor; Panagiotis A Konstantinopoulos; Stephen J Elledge; Simon J Boulton; Timur Yusufzai; Alan D D'Andrea
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  4 in total

1.  Mechanistic Insight through Irreversible Inhibition: DNA Polymerase θ Uses a Common Active Site for Polymerase and Lyase Activities.

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2.  Translesion Synthesis Past 5-Formylcytosine-Mediated DNA-Peptide Cross-Links by hPolη Is Dependent on the Local DNA Sequence.

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3.  Dynamics of 5R-Tg Base Flipping in DNA Duplexes Based on Simulations─Agreement with Experiments and Beyond.

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4.  TEB/POLQ plays dual roles in protecting Arabidopsis from NO-induced DNA damage.

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  4 in total

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