Life without dUTPase

Fine-tuned regulation of the cellular nucleotide pools is indispensable for faithful replication of DNA. The genetic information is also safeguarded by DNA damage recognition and repair processes. Uracil is one of the most frequently occurring erroneous bases in DNA; it can arise from cytosine deami...

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Main Authors: Csaba Kerepesi, Judit E Szabó, Veronika Papp-Kádár, Orsolya Dobay, Dóra Szabó, Vince Grolmusz, Beata G Vertessy
Format: Article
Language:English
Published: Frontiers Media S.A. 2016-11-01
Series:Frontiers in Microbiology
Subjects:
UNG
Online Access:http://journal.frontiersin.org/Journal/10.3389/fmicb.2016.01768/full
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spelling doaj-b4111ab7d87c4acd8bd6d46aac9a70d82020-11-24T22:33:29ZengFrontiers Media S.A.Frontiers in Microbiology1664-302X2016-11-01710.3389/fmicb.2016.01768227148Life without dUTPaseCsaba Kerepesi0Judit E Szabó1Judit E Szabó2Veronika Papp-Kádár3Veronika Papp-Kádár4Orsolya Dobay5Dóra Szabó6Vince Grolmusz7Beata G Vertessy8Beata G Vertessy9Eötvös UniversityBudapest University of Technology and EconomicsInstitute of Enzymology, Research Centre for Natural Sciences, Hungarian Academy of SciencesBudapest University of Technology and EconomicsInstitute of Enzymology, Research Centre for Natural Sciences, Hungarian Academy of SciencesInstitute of Medical Microbiology, Semmelweis UniversityInstitute of Medical Microbiology, Semmelweis UniversityEötvös UniversityBudapest University of Technology and EconomicsInstitute of Enzymology, Research Centre for Natural Sciences, Hungarian Academy of SciencesFine-tuned regulation of the cellular nucleotide pools is indispensable for faithful replication of DNA. The genetic information is also safeguarded by DNA damage recognition and repair processes. Uracil is one of the most frequently occurring erroneous bases in DNA; it can arise from cytosine deamination or thymine-replacing incorporation. Two enzyme activities are primarily involved in keeping DNA uracil-free: dUTPase activity that prevent thymine-replacing incorporation and uracil-DNA glycosylase activity that excise uracil from DNA and initiate uracil-excision repair. Both dUTPase and the most efficient uracil-DNA glycosylase (UNG) is thought to be ubiquitous in free-living organisms. In the present work, we have systematically investigated the genotype of deposited fully sequenced bacterial and Archaeal genomes. We have performed bioinformatic searches in these genomes using the already well described dUTPase and UNG gene sequences. For dUTPases, we have included the trimeric all-beta and the dimeric all-alpha families and also, the bifunctional dCTP deaminase-dUTPase sequences. Surprisingly, we have found that in contrast to the generally held opinion, a wide number of bacterial and Archaeal species lack all of the previously described dUTPase gene(s). The dut- genotype is present in diverse bacterial phyla indicating that loss of this (or these) gene(s) has occurred multiple times during evolution. We discuss potential survival strategies in lack of dUTPases, such as simultaneous lack or inhibition of UNG and possession of exogenous or alternate metabolic enzymes involved in uracil-DNA metabolism. The potential that genes previously not associated with dUTPase activity may still encode enzymes capable of hydrolyzing dUTP is also discussed. Our data indicate that several unicellular microorganisms may efficiently cope with a dut- genotype, lacking all of the previously described dUTPase genes, and potentially leading to an unusual uracil-enrichment in their genomic DNA.http://journal.frontiersin.org/Journal/10.3389/fmicb.2016.01768/fullBacteriaDNA RepairUracilhorizontal gene transferUNGdUTPase
collection DOAJ
language English
format Article
sources DOAJ
author Csaba Kerepesi
Judit E Szabó
Judit E Szabó
Veronika Papp-Kádár
Veronika Papp-Kádár
Orsolya Dobay
Dóra Szabó
Vince Grolmusz
Beata G Vertessy
Beata G Vertessy
spellingShingle Csaba Kerepesi
Judit E Szabó
Judit E Szabó
Veronika Papp-Kádár
Veronika Papp-Kádár
Orsolya Dobay
Dóra Szabó
Vince Grolmusz
Beata G Vertessy
Beata G Vertessy
Life without dUTPase
Frontiers in Microbiology
Bacteria
DNA Repair
Uracil
horizontal gene transfer
UNG
dUTPase
author_facet Csaba Kerepesi
Judit E Szabó
Judit E Szabó
Veronika Papp-Kádár
Veronika Papp-Kádár
Orsolya Dobay
Dóra Szabó
Vince Grolmusz
Beata G Vertessy
Beata G Vertessy
author_sort Csaba Kerepesi
title Life without dUTPase
title_short Life without dUTPase
title_full Life without dUTPase
title_fullStr Life without dUTPase
title_full_unstemmed Life without dUTPase
title_sort life without dutpase
publisher Frontiers Media S.A.
series Frontiers in Microbiology
issn 1664-302X
publishDate 2016-11-01
description Fine-tuned regulation of the cellular nucleotide pools is indispensable for faithful replication of DNA. The genetic information is also safeguarded by DNA damage recognition and repair processes. Uracil is one of the most frequently occurring erroneous bases in DNA; it can arise from cytosine deamination or thymine-replacing incorporation. Two enzyme activities are primarily involved in keeping DNA uracil-free: dUTPase activity that prevent thymine-replacing incorporation and uracil-DNA glycosylase activity that excise uracil from DNA and initiate uracil-excision repair. Both dUTPase and the most efficient uracil-DNA glycosylase (UNG) is thought to be ubiquitous in free-living organisms. In the present work, we have systematically investigated the genotype of deposited fully sequenced bacterial and Archaeal genomes. We have performed bioinformatic searches in these genomes using the already well described dUTPase and UNG gene sequences. For dUTPases, we have included the trimeric all-beta and the dimeric all-alpha families and also, the bifunctional dCTP deaminase-dUTPase sequences. Surprisingly, we have found that in contrast to the generally held opinion, a wide number of bacterial and Archaeal species lack all of the previously described dUTPase gene(s). The dut- genotype is present in diverse bacterial phyla indicating that loss of this (or these) gene(s) has occurred multiple times during evolution. We discuss potential survival strategies in lack of dUTPases, such as simultaneous lack or inhibition of UNG and possession of exogenous or alternate metabolic enzymes involved in uracil-DNA metabolism. The potential that genes previously not associated with dUTPase activity may still encode enzymes capable of hydrolyzing dUTP is also discussed. Our data indicate that several unicellular microorganisms may efficiently cope with a dut- genotype, lacking all of the previously described dUTPase genes, and potentially leading to an unusual uracil-enrichment in their genomic DNA.
topic Bacteria
DNA Repair
Uracil
horizontal gene transfer
UNG
dUTPase
url http://journal.frontiersin.org/Journal/10.3389/fmicb.2016.01768/full
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