| Literature DB >> 33291569 |
Chiara Nicolazzo1, Ludovic Barault2,3, Salvatore Caponnetto4, Marco Macagno3, Gianluigi De Renzi1, Angela Gradilone1,5, Francesca Belardinilli5, Enrico Cortesi4, Federica Di Nicolantonio2,3, Paola Gazzaniga1.
Abstract
The clearance of RAS mutations in plasma circulating tumor DNA (ctDNA) from originally RAS-mutant metastatic colorectal cancer (mCRC) has been recently demonstrated. Clinical trials investigating whether RAS mutant mCRC who "convert" to wild-type in plasma might benefit from EGFR blockade are ongoing. Detection of tumor-specific DNA methylation alterations in ctDNA has been suggested as a specific tool to confirm the tumoral origin of cell-free DNA. We monitored RAS clearance in plasma from patients with RAS-mutant mCRC at baseline (pre-treatment) (T0); after 4 months of first-line therapy (T1); at the time of first (T2) and second (T3) progression. A five-gene methylation panel was used to confirm the presence of ctDNA in samples in which RAS mutation clearance was detected. At T1, ctDNA analysis revealed wild-type RAS status in 83% of samples, all not methylated, suggesting at this time point the lack of ctDNA shedding. At T2, ctDNA analysis revealed wild-type RAS status in 83% of samples, of which 62.5% were found methylated. At T3, 50% of wild-type RAS samples were found methylated. Non-methylated samples were found in patients with lung or brain metastases. This five-gene methylation test might be useful to confirm the presence of ctDNA in RAS wild-type plasma samples.Entities:
Keywords: EGFR inhibitors; RAS mutation clearance; circulating methylated DNA; circulating tumor DNA; liquid biopsy; metastatic colorectal cancer
Year: 2020 PMID: 33291569 PMCID: PMC7761880 DOI: 10.3390/cancers12123633
Source DB: PubMed Journal: Cancers (Basel) ISSN: 2072-6694 Impact factor: 6.639