Roles of homologous recombination in response to ionizing radiation-induced DNA damage

Jac A Nickoloff; Neelam Sharma; Christopher P Allen; Lynn Taylor; Sage J Allen; Aruna S Jaiswal; Robert Hromas

doi:10.1080/09553002.2021.1956001

Roles of homologous recombination in response to ionizing radiation-induced DNA damage

Int J Radiat Biol. 2023;99(6):903-914. doi: 10.1080/09553002.2021.1956001. Epub 2021 Aug 4.

Authors

Jac A Nickoloff¹, Neelam Sharma¹, Christopher P Allen^{1

2}, Lynn Taylor¹, Sage J Allen¹, Aruna S Jaiswal³, Robert Hromas³

Affiliations

¹ Department of Environmental and Radiological Health Sciences, Colorado State University, Fort Collins, CO, USA.
² Department of Microbiology, Immunology and Pathology, Flow Cytometry and Cell Sorting Facility, Colorado State University, Fort Collins, CO, USA.
³ Division of Hematology and Medical Oncology, Department of Medicine and the Mays Cancer Center, University of Texas Health Science Center, San Antonio, TX, USA.

Abstract

Purpose: Ionizing radiation induces a vast array of DNA lesions including base damage, and single- and double-strand breaks (SSB, DSB). DSBs are among the most cytotoxic lesions, and mis-repair causes small- and large-scale genome alterations that can contribute to carcinogenesis. Indeed, ionizing radiation is a 'complete' carcinogen. DSBs arise immediately after irradiation, termed 'frank DSBs,' as well as several hours later in a replication-dependent manner, termed 'secondary' or 'replication-dependent DSBs. DSBs resulting from replication fork collapse are single-ended and thus pose a distinct problem from two-ended, frank DSBs. DSBs are repaired by error-prone nonhomologous end-joining (NHEJ), or generally error-free homologous recombination (HR), each with sub-pathways. Clarifying how these pathways operate in normal and tumor cells is critical to increasing tumor control and minimizing side effects during radiotherapy.

Conclusions: The choice between NHEJ and HR is regulated during the cell cycle and by other factors. DSB repair pathways are major contributors to cell survival after ionizing radiation, including tumor-resistance to radiotherapy. Several nucleases are important for HR-mediated repair of replication-dependent DSBs and thus replication fork restart. These include three structure-specific nucleases, the 3' MUS81 nuclease, and two 5' nucleases, EEPD1 and Metnase, as well as three end-resection nucleases, MRE11, EXO1, and DNA2. The three structure-specific nucleases evolved at very different times, suggesting incremental acceleration of replication fork restart to limit toxic HR intermediates and genome instability as genomes increased in size during evolution, including the gain of large numbers of HR-prone repetitive elements. Ionizing radiation also induces delayed effects, observed days to weeks after exposure, including delayed cell death and delayed HR. In this review we highlight the roles of HR in cellular responses to ionizing radiation, and discuss the importance of HR as an exploitable target for cancer radiotherapy.

Keywords: DNA double-strand breaks; DNA repair; cancer radiotherapy; homologous recombination; ionizing radiation; replication stress.

Publication types

Review
Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Cell Cycle
DNA Breaks, Double-Stranded*
DNA Damage
DNA Repair*
Homologous Recombination
Radiation, Ionizing

Abstract

Publication types

MeSH terms

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