Leonie Müller scite author profile

Background: 8-OxoG is a major oxidative lesion in DNA and is associated with cancer. Results: Kinetic and mass spectrometric studies demonstrate that human polymerase bypasses 8-oxoG in a largely error-free manner. Conclusion: Arginine 61 from the finger domain plays a key role in error-free bypass at the insertion stage. Significance: In addition to photo-adducts and cisplatinated DNA, polymerase might also be involved in accurate bypass of 8-oxoG in vivo.

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p53 Activity Results in DNA Replication Fork Processivity

Ina

Rodewald

Müller

et al. 2016

Cell Reports

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p53 induces cell death upon DNA damage, but this may not confer all of its tumor suppressor activity. We report that p53 activation enhances the processivity of DNA replication, as monitored by multi-label fiber assays, whereas removal of p53 reduces fork progression. This is observed in tumor-derived U2OS cells but also in murine embryonic fibroblasts with heterozygous or homozygous p53 deletion and in freshly isolated thymocytes from mice with differential p53 status. Mdm2, a p53-inducible gene product, similarly supports DNA replication even in p53-deficient cells, suggesting that sustained Mdm2-expression is at least one of the mechanisms allowing p53 to prevent replicative stress. Thus, p53 helps to protect the genome during S phase, by preventing the occurrence of stalled or collapsed replication forks. These results expand p53's tumor-suppressive functions, adding to the ex-post model (elimination of damaged cells) an ex-ante activity; i.e., the prevention of DNA damage during replication.

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A dimer-monomer switch controls CHIP-dependent substrate ubiquitylation and processing

et al. 2022

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<em>In Vitro</em> Analysis of E3 Ubiquitin Ligase Function

Müller

Kutzner

Balaji

et al. 2021

JoVE

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Leonie Müller

Kinetics, Structure, and Mechanism of 8-Oxo-7,8-dihydro-2′-deoxyguanosine Bypass by Human DNA Polymerase η

p53 Activity Results in DNA Replication Fork Processivity

A dimer-monomer switch controls CHIP-dependent substrate ubiquitylation and processing

<em>In Vitro</em> Analysis of E3 Ubiquitin Ligase Function

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