Human endonuclease III/NTH1: focusing on the [4Fe-4S] cluster and the N-terminal domain.

Elin Moe,Célia M Silveira,Meike Stelter,Lidia Zuccarello,Smilja Todorovic,Peter Hildebrandt,Joanna Timmins,Ingo Zebger,Filipe Rollo,Sagie Katz,Salvatore De Bonis,Catharina Kulka-Peschke

doi:10.1039/d2cc03643f

Human endonuclease III/NTH1: focusing on the [4Fe-4S] cluster and the N-terminal domain.

Elin Moe, Célia M Silveira + Show 10 more

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https://doi.org/10.1039/d2cc03643f

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Journal: Chemical Communications	Publication Date: Jan 1, 2022
Citations: 3	License type: CC BY-NC 3.0

Affiliation: Universidade Nova de Lisboa, Institut de Biologie Structurale, French National Centre for Scientific Research, CEA Grenoble, Atomic Energy and Alternative Energies Commission, Université Grenoble Alpes, Technische Universität Berlin

#Damaged DNA Substrate #4Fe 4S + Show 8 more

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Abstract

Human Endonuclease III (EndoIII), hNTH1, is an FeS containing enzyme which repairs oxidation damaged bases in DNA. We report here the first comparative biophysical study of full-length and an N-terminally truncated hNTH1, with a domain architecture homologous to bacterial EndoIII. Vibrational spectroscopy, spectroelectrochemistry and SAXS experiments reveal distinct properties of the two enzyme forms, and indicate that the N-terminal domain is important for DNA binding at the onset of damage recognition.

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