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Title: | Cell-free DNA in plasma and ascites as a biomarker of bevacizumab response- a translational research sub-study of the REZOLVE (ANZGOG-1101) clinical trial. |
Epworth Authors: | Ananda, Sumitra |
Other Authors: | Werner, Bonnita Sjoquist, Katrin Espinoza, David Yip, Sonia Chang, Garry Cummins, Michelle Mileshkin, Linda Shannon, Catherine Friedlander, Michael Warton, Kristina Ford, Caroline |
Keywords: | Ascites Bevacizumab Biomarker Cell-free DNA Ovarian cancer Cancer Services Clinical Institute, Epworth HealthCare, Victoria, Australia |
Issue Date: | May-2024 |
Publisher: | Elsevier |
Citation: | Transl Oncol . 2024 May:43:101914 |
Abstract: | Objective: To investigate cell-free DNA (cfDNA) in plasma and ascites and its association with clinical outcomes (paracentesis-free interval, overall survival) and CA125 level in participants with advanced ovarian cancer, treated with palliative intraperitoneal bevacizumab to delay re-accumulation of ascites. Methods: cfDNA was extracted from 0.3 to 1 mL samples from 20/24 participants of the REZOLVE trial. Standard and methylation-specific PCRs were performed to measure 3 biomarkers: total cfDNA (Alu), tumour-derived cfDNA (ctDNA, methylated IFFO1 promoter) and endothelium-derived cfDNA (ec-cfDNA, unmethylated CDH5 promoter). Values were correlated to clinical outcomes. Results: cfDNA was detected in all samples, with higher yield in ascites (mean 669 ng/mL) than plasma (mean 75 ng/mL, p < 0.0001). Ascites had a higher ctDNA proportion than plasma (74 % vs. 20 %, p < 0.0001) and plasma had a higher ec-cfDNA proportion than ascites (24 % vs. 16 %, p < 0.002). High ctDNA proportion (>75 %) in ascites was associated with a significantly shorter paracentesis-free interval (median interval 47.5 versus 84 days, hazard ratio (HR) 2.21, 95 % confidence interval (CI) 0.85 to 5.73, p = 0.039) and ctDNA presence in plasma was unfavourable for survival (median survival 56 versus 242 days, HR 3.21, 95 % CI 1.15 to 9.00, p = 0.008). A significant positive correlation was observed between ctDNA proportion in plasma and CA125 level (p = 0.012). No significant difference in total cfDNA, ctDNA nor ec-cfDNA was observed between participants who were responders versus non-responders. Conclusion: Sufficient cfDNA was detected in both plasma and ascites to study three biomarkers. These samples can provide useful information and should be considered in the design of future ovarian cancer trials. |
URI: | http://hdl.handle.net/11434/2293 |
DOI: | doi: 10.1016/j.tranon.2024.101914 |
PubMed URL: | https://pubmed.ncbi.nlm.nih.gov/38417292/ |
ISSN: | 1936-5233 1944-7124 |
Journal Title: | Translational Oncology |
Type: | Journal Article |
Affiliated Organisations: | Gynaecological Cancer Research Group, School of Clinical Medicine, Faculty of Medicine and Health, University of New South Wales, Sydney, Australia. National Health and Medical Research Council Clinical Trials Centre, University of Sydney, Sydney, Australia. Peter MacCallum Cancer Centre, Melbourne, Australia. Western Health, Furlong Road, St Albans, Australia. Department of Medicine, Western Health, University of Melbourne, Melbourne, Australia. Mater Cancer Care Centre, South Brisbane, Australia. Prince of Wales Hospital, Sydney, Australia. School of Clinical Medicine, Faculty of Medicine and Health, University of New South Wales, Sydney, Australia. |
Type of Clinical Study or Trial: | Cohort Study |
Appears in Collections: | Cancer Services |
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