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Oncotarget

A Multiplex Assay to Assess Activated p300/CBP in Circulating Prostate Tumor Cells

Jul 22, 2023
New research paper on assessing p300/CBP in circulating tumor cells. Connection between SIRT2 deacetylation and p300 acetylation in prostate cancer. Use of Exclusion-based Sample Preparation to isolate CTCs. Staining optimization reveals expression of acetyl-p300 and acetyl-H3K18.
04:13

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Quick takeaways

  • Altered P300/CBP acetylation in circulating tumor cells may serve as biomarkers for assessing treatment response to androgen deprivation therapy (ADT).
  • Increased p300/CBP activity in castration-resistant prostate cancer patients could indicate potential candidates for CBP/P300 acetylation inhibitors in clinical development.

Deep dives

Development of a Multiplex Estate to Assess Activated P300/CBP in Circulating Prostate Tumor Cells

Researchers at the University of Wisconsin conducted a study focusing on altered P300/CBP acetylation in circulating tumor cells (CTCs) from patients with sensitivity or resistance to androgen deprivation therapy (ADT). By isolating CTCs using ESP technology, they evaluated P300 activity, SIRT2 expression, and H3K18 acetylation. The study revealed clear expression of acetyl P300, acetyl H3K18, and SIRT2 on CTCs, indicating potential markers for assessing acetylation activity. Patients with reduced SIRT2 expression showed shorter response times to ARSI therapy, suggesting a clinical impact of the CBP/P300 axis in prostate cancer treatment.

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