DNA polymerase delta interacting protein 3 facilitates the activation and maintenance of DNA damage checkpoint in response to replication stress

Author(s)

Zhang, S., Lee, E. Y. C., Lee, M. Y. W. T., & Zhang, D.

Title

DNA polymerase delta interacting protein 3 facilitates the activation and maintenance of DNA damage checkpoint in response to replication stress

Date

2022

Publisher

Wiley

Subject

DNA Damage
DNA Polymerase III metabolism
DNA Replication
DNA damage checkpoint
DNA polymerase delta
Index Medicus
POLDIP3
Replication stress

Language

English

Abstract

Background

Replication stress response is crucial for the maintenance of a stable genome. POLDIP3 (DNA polymerase delta interacting protein 3) was initially identified as one of the DNA polymerase δ (Pol δ) interacting proteins almost 20 years ago. Using a variety of in vitro biochemical assays, we previously established that POLDIP3 is a key regulator of the enzymatic activity of Pol δ. However, the in vivo function of POLDIP3 in DNA replication and DNA damage response has been elusive.

Methods

We first generated POLDIP3 knockout (KO) cells using the CRISPR/Cas9 technology. We then investigated its biological functions in vivo using a variety of biochemical and cell biology assays.

Results

We showed that although the POLDIP3-KO cells manifest no pronounced defect in global DNA synthesis under nonstress conditions, they are sensitive to a variety of replication fork blockers. Intriguingly, we found that POLDIP3 plays a crucial role in the activation and maintenance of the DNA damage checkpoint in response to exogenous as well as endogenous replication stress.

Conclusion

Our results indicate that when the DNA replication fork is blocked, POLDIP3 can be recruited to the stalled replication fork and functions to bridge the early DNA damage checkpoint response and the later replication fork repair/restart.

Source

Animal Models and Experimental Medicine, Volume 5, Issue 5, September 2022, pages 461-469

Rights

This is an open access article under the terms of the Creative Commons Attribution-NonCommercial-NoDerivs License, which permits use and distribution in any medium, provided the original work is properly cited, the use is non-commercial and no modifications or adaptations are made.

Bibliographic Citation

Zhang, S., Lee, E. Y. C., Lee, M. Y. W. T., & Zhang, D. (2022). <scp>DNA</scp> polymerase delta interacting protein 3 facilitates the activation and maintenance of <scp>DNA</scp> damage checkpoint in response to replication stress. In Animal Models and Experimental Medicine (Vol. 5, Issue 5, pp. 461–469). Wiley. https://doi.org/10.1002/ame2.12274

Files

Anim Models and Exp Med - 2022 - Zhang.pdf

Citation

Zhang, S., Lee, E. Y. C., Lee, M. Y. W. T., & Zhang, D., DNA polymerase delta interacting protein 3 facilitates the activation and maintenance of DNA damage checkpoint in response to replication stress. Animal Models and Experimental Medicine, Volume 5, Issue 5, September 2022, pages 461-469, New York Tech Institutional Repository, accessed April 27, 2024, https://repository.nyitlibrary.org/items/show/3756

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