Werner helicase interacting protein 1 contributes to G-quadruplex processing in human cells

Lili Hegedus; Agnes Toth; Gabor M. Harami; Janos Palinkas; Nargis Karatayeva; Eniko Sajben-Nagy; Szabolcs Bene; Sara Afzali Jaktajdinani; Mihaly Kovacs; Szilvia Juhasz; Peter Burkovics

doi:10.1038/s41598-024-66425-y

Scientific Reports (Jul 2024)

Werner helicase interacting protein 1 contributes to G-quadruplex processing in human cells

Lili Hegedus,
Agnes Toth,
Gabor M. Harami,
Janos Palinkas,
Nargis Karatayeva,
Eniko Sajben-Nagy,
Szabolcs Bene,
Sara Afzali Jaktajdinani,
Mihaly Kovacs,
Szilvia Juhasz,
Peter Burkovics

Affiliations

Lili Hegedus: Institute of Genetics, Biological Research Centre, HUN-REN Szeged
Agnes Toth: Institute of Genetics, Biological Research Centre, HUN-REN Szeged
Gabor M. Harami: ELTE-MTA Momentum Motor Enzymology Research Group, Department of Biochemistry, Eötvös Loránd University
Janos Palinkas: ELTE-MTA Momentum Motor Enzymology Research Group, Department of Biochemistry, Eötvös Loránd University
Nargis Karatayeva: Institute of Genetics, Biological Research Centre, HUN-REN Szeged
Eniko Sajben-Nagy: Institute of Genetics, Biological Research Centre, HUN-REN Szeged
Szabolcs Bene: Institute of Genetics, Biological Research Centre, HUN-REN Szeged
Sara Afzali Jaktajdinani: Institute of Genetics, Biological Research Centre, HUN-REN Szeged
Mihaly Kovacs: ELTE-MTA Momentum Motor Enzymology Research Group, Department of Biochemistry, Eötvös Loránd University
Szilvia Juhasz: HCEMM Cancer Microbiome Core Group
Peter Burkovics: Institute of Genetics, Biological Research Centre, HUN-REN Szeged

DOI: https://doi.org/10.1038/s41598-024-66425-y
Journal volume & issue: Vol. 14, no. 1
pp. 1 – 12

Abstract

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Abstract Genome replication is frequently impeded by highly stable DNA secondary structures, including G-quadruplex (G4) DNA, that can hinder the progression of the replication fork. Human WRNIP1 (Werner helicase Interacting Protein 1) associates with various components of the replication machinery and plays a crucial role in genome maintenance processes. However, its detailed function is still not fully understood. Here we show that human WRNIP1 interacts with G4 structures and provide evidence for its contribution to G4 processing. The absence of WRNIP1 results in elevated levels of G4 structures, DNA damage and chromosome aberrations following treatment with PhenDC3, a G4-stabilizing ligand. Additionally, we establish a functional and physical relationship between WRNIP1 and the PIF1 helicase in G4 processing. In summary, our results suggest that WRNIP1 aids genome replication and maintenance by regulating G4 processing and this activity relies on Pif1 DNA helicase.

Published in Scientific Reports

ISSN: 2045-2322 (Online)
Publisher: Nature Portfolio
Country of publisher: United Kingdom
LCC subjects: Medicine; Science
Website: https://www.nature.com/srep/

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Abstract

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