par Vandeputte, Caroline;Geboes, Karen;Delaunoit, Thierry 
;Demolin, Gauthier;Peeters, Michel ;D'Hondt, Lionel;Janssens, Jos;Carrasco, Javier;Marechal, Raphaël ;Gomez-Galdon, Maria;Heimann, Pierre ;Kehagias, Pashalina ;Paesmans, Marianne ;Flamen, Patrick ;Hendlisz, Alain ;El Housni, Hakim ;Ameye, Lieveke;Laes, Jean-François ;Desmedt, Christine ;Sotiriou, Christos ;Deleporte, Amélie;Puleo, Francesco
Référence Oncotarget, 9, 25, page (17756-17769)
Publication Publié, 2018-04
;Demolin, Gauthier;Peeters, Michel ;D'Hondt, Lionel;Janssens, Jos;Carrasco, Javier;Marechal, Raphaël ;Gomez-Galdon, Maria;Heimann, Pierre ;Kehagias, Pashalina ;Paesmans, Marianne ;Flamen, Patrick ;Hendlisz, Alain ;El Housni, Hakim ;Ameye, Lieveke;Laes, Jean-François ;Desmedt, Christine ;Sotiriou, Christos ;Deleporte, Amélie;Puleo, Francesco Référence Oncotarget, 9, 25, page (17756-17769)
Publication Publié, 2018-04
Article révisé par les pairs
| Résumé : | Predictive biomarkers are eagerly awaited in advanced colorectal cancer (aCRC). Targeted sequencing performed on tumor and baseline plasma samples in 20 patients with aCRC treated with regorafenib identified 89 tumor-specific mutations of which ≥50% are also present in baseline plasma. Droplet digital PCR (ddPCR) assays were optimized to monitor circulating tumor DNA (ctDNA) levels in plasmatic samples collected throughout the treatment course and showed the importance of using the absolute value for ctDNA rather than the mutant/wild type ratio in monitoring the therapy outcome. High baseline cell free DNA (cfDNA) levels are associated with shorter overall survival (OS) (HR 7.38, P=0.001). An early increase (D14) in mutated copies/mL is associated with a significantly worse PFS (HR 6.12, P=0.008) and OS (HR 8.02, P=0.004). These data suggest a high prognostic value for early ctDNA level changes and support the use of blood-born genomic markers as a tool for treatment. |
