AI Article Synopsis
- PARP1 is a key sensor for cellular damage, specifically DNA strand breaks, which helps in DNA repair by recruiting XRCC1 and forming repair complexes.
- The study shows that the recruitment of PARP1 and XRCC1 to DNA damage sites is mutually dependent, emphasizing their collaboration in responding to genotoxic stress.
- Experiments using various cell types revealed that XRCC1 KO cells are more sensitive to certain DNA-damaging treatments, and this sensitivity can be mitigated by further genetic modifications or pharmacological interventions targeting PARP1.
Article Abstract
PARP1 (aka ARTD1) acts as a prime sensor of cellular genotoxic stress response. PARP1 detects DNA strand breaks and subsequently catalyzes the formation of poly(ADP-ribose) (PAR), which leads to the recruitment of the scaffold protein XRCC1 during base excision and single strand break repair and the assembly of multi-protein complexes to promote DNA repair. Here, we reveal that the recruitment of either protein to sites of DNA damage is impeded in the absence of the other, indicating a strong reciprocal relationship between the two DNA repair factors during genotoxic stress response. We further analyzed several cellular and molecular endpoints in HeLa PARP1 KO, XRCC1 KO, and PARP1/XRCC1 double KO (DKO) cells after genotoxic treatments, i.e., PARylation response, NAD levels, clonogenic survival, cell cycle progression, cell death, and DNA repair. The analysis of NAD levels and cytotoxicity after treatment with the topoisomerase I inhibitor camptothecin revealed a hypersensitivity phenotype of XRCC1 KO cells compared to PARP1 KO cells-an effect that could be rescued by the additional genetic deletion of PARP1 as well as by pharmacological PARP inhibition. Moreover, impaired repair of hydrogen peroxide and CPT-induced DNA damage in XRCC1 KO cells could be partially rescued by additional deletion of PARP1. Our results therefore highlight important reciprocal regulatory functions of XRCC1 and PARP1 during genotoxic stress response.
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|---|---|
| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10042965 | PMC |
| http://dx.doi.org/10.1007/s10565-022-09739-9 | DOI Listing |
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