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  5. Evolutionary Origins of DNA Repair Pathways: Role of Oxygen Catastrophe in the Emergence of DNA Glycosylases
 
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2021
Zweitveröffentlichung
Artikel
Verlagsversion

Evolutionary Origins of DNA Repair Pathways: Role of Oxygen Catastrophe in the Emergence of DNA Glycosylases

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Hauptpublikation
cells-10-01591.pdf
CC BY 4.0 International
Format: Adobe PDF
Size: 5.26 MB
TUDa URI
tuda/7485
URN
urn:nbn:de:tuda-tuprints-195692
DOI
10.26083/tuprints-00019569
Autor:innen
Prorok, Paulina ORCID 0000-0002-1427-1528
Grin, Inga R.
Matkarimov, Bakhyt T.
Ishchenko, Alexander A. ORCID 0000-0002-0488-8858
Laval, Jacques
Zharkov, Dmitry O. ORCID 0000-0001-5013-0194
Saparbaev, Murat ORCID 0000-0002-4630-1074
Kurzbeschreibung (Abstract)

It was proposed that the last universal common ancestor (LUCA) evolved under high temperatures in an oxygen-free environment, similar to those found in deep-sea vents and on volcanic slopes. Therefore, spontaneous DNA decay, such as base loss and cytosine deamination, was the major factor affecting LUCA’s genome integrity. Cosmic radiation due to Earth’s weak magnetic field and alkylating metabolic radicals added to these threats. Here, we propose that ancient forms of life had only two distinct repair mechanisms: versatile apurinic/apyrimidinic (AP) endonucleases to cope with both AP sites and deaminated residues, and enzymes catalyzing the direct reversal of UV and alkylation damage. The absence of uracil–DNA N-glycosylases in some Archaea, together with the presence of an AP endonuclease, which can cleave uracil-containing DNA, suggests that the AP endonuclease-initiated nucleotide incision repair (NIR) pathway evolved independently from DNA glycosylase-mediated base excision repair. NIR may be a relic that appeared in an early thermophilic ancestor to counteract spontaneous DNA damage. We hypothesize that a rise in the oxygen level in the Earth’s atmosphere ~2 Ga triggered the narrow specialization of AP endonucleases and DNA glycosylases to cope efficiently with a widened array of oxidative base damage and complex DNA lesions.

Freie Schlagworte

DNA repair

DNA glycosylases

AP endonucleases

protein folds

structural homology

Sprache
Englisch
Fachbereich/-gebiet
10 Fachbereich Biologie > Cell Biology and Epigenetics
DDC
500 Naturwissenschaften und Mathematik > 570 Biowissenschaften, Biologie
600 Technik, Medizin, angewandte Wissenschaften > 610 Medizin, Gesundheit
Institution
Universitäts- und Landesbibliothek Darmstadt
Ort
Darmstadt
Titel der Zeitschrift / Schriftenreihe
Cells
Jahrgang der Zeitschrift
10
Heftnummer der Zeitschrift
7
ISSN
2073-4409
Verlag
MDPI
Ort der Erstveröffentlichung
Basel
Publikationsjahr der Erstveröffentlichung
2021
Verlags-DOI
10.3390/cells10071591
PPN
516174622
Zusätzliche Infomationen
This article belongs to the Special Issue DNA Repair, Genome Stability/Diversity, and Oxidative Stress and Aging, from Bacteria to Human Cells: A Themed Issue in Honor of Prof. Miroslav Radman

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