| Literature DB >> 27194447 |
Anne C Knol1, Audrey Vallée1,2, Guillaume Herbreteau1,2, Jean-Michel Nguyen1,3, Emilie Varey1,4, Aurélie Gaultier3, Sandrine Théoleyre1,2, Mélanie Saint-Jean1,4, Lucie Peuvrel1,4, Anabelle Brocard1,4, Gaëlle Quéreux1,4, Amir Khammari1,4, Marc G Denis1,2, Brigitte Dréno5,6.
Abstract
Circulating tumor DNA is a promising non-invasive tool for cancer monitoring. The main objective of our work was to investigate the relationship between mutant BRAF DNA in plasma and clinical response. Thirty-eight stage IV patients with a V600 mutated BRAF melanoma were included prior to any treatment. DNA was extracted from plasma and mutant DNA was detected using the amplification-refractory mutation system method. Before the beginning of any treatment, the corresponding BRAF mutation was detected in 29 of the 38 tested plasma samples (76.3% positive per cent agreement). We observed a strong correlation between the presence of circulating mutated DNA and overall survival (OS; P=.02), and with the number of metastatic sites (P=.01). The presence of circulating mutated DNA was also strongly correlated with serum LDH activity (P<.01) and S100 protein concentration (P<.01). Finally, seven patients presented discordant BRAF status in different tumor sites. In all these patients, the test performed on ctDNA was positive, suggesting that ctDNA analysis might be less sensitive to tumor heterogeneity. Altogether, these results suggest that plasmatic mutant BRAF DNA is a prognostic factor of OS, correlated with tumor burden. In addition, it represents an interesting alternative source of DNA to detect BRAF mutations before treatment.Entities:
Keywords: BRAF mutation; metastatic melanoma; overall survival; plasma DNA
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Year: 2016 PMID: 27194447 DOI: 10.1111/exd.13065
Source DB: PubMed Journal: Exp Dermatol ISSN: 0906-6705 Impact factor: 3.960