AI Article Synopsis
- Increased expression of NUSAP1 serves as a strong prognostic biomarker in prostate cancer and promotes cancer invasion and metastasis regulated by E2F1.
- * Researchers identified 85 proteins that interact with NUSAP1, highlighting its role in maintaining R-loops and aiding in DNA damage response, particularly through interaction with ILF2.
- * Depleting ILF2 increases DNA damage, and NUSAP1's interaction with ILF2 is crucial in regulating R-loop formation, suggesting NUSAP1 as a potential target for cancer therapies.*
Article Abstract
Increased expression of NUSAP1 has been identified as a robust prognostic biomarker in prostate cancer and other malignancies. We have previously shown that NUSAP1 is positively regulated by E2F1 and promotes cancer invasion and metastasis. To further understand the biological function of NUSAP1, we used affinity purification and mass spectrometry proteomic analysis to identify NUSAP1 interactors. We identified 85 unique proteins in the NUSAP1 interactome, including ILF2, DHX9, and other RNA-binding proteins. Using proteomic approaches, we uncovered a function for NUSAP1 in maintaining R-loops and in DNA damage response through its interaction with ILF2. Co-immunoprecipitation and colocalization using confocal microscopy verified the interactions of NUSAP1 with ILF2 and DHX9, and RNA/DNA hybrids. We showed that the microtubule and charged helical domains of NUSAP1 were necessary for the protein-protein interactions. Depletion of ILF2 alone further increased camptothecin-induced R-loop accumulation and DNA damage, and NUSAP1 depletion abolished this effect. In human prostate adenocarcinoma, and mRNA expression levels are positively correlated, elevated, and associated with poor clinical outcomes. Our study identifies a novel role for NUSAP1 in regulating R-loop formation and accumulation in response to DNA damage through its interactions with ILF2 and hence provides a potential therapeutic target.
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|---|---|
| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10093842 | PMC |
| http://dx.doi.org/10.3390/ijms24076258 | DOI Listing |
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