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The amount of activating EGFR mutations in circulating cell-free DNA is a marker to monitor osimertinib response
by
Valleggi, Simona
, Petrini, Iacopo
, Arrigoni, Elena
, Tiseo, Marcello
, Crucitta, Stefania
, Rofi, Eleonora
, Restante, Giuliana
, Marzia Del Re
, Morganti, Riccardo
, Minari, Roberta
, Chella, Antonio
, Danesi, Romano
, Bordi, Paola
in
Epidermal growth factor receptors
/ Gene frequency
/ Mutation
/ Non-small cell lung carcinoma
/ Patients
/ Targeted cancer therapy
2018
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The amount of activating EGFR mutations in circulating cell-free DNA is a marker to monitor osimertinib response
by
Valleggi, Simona
, Petrini, Iacopo
, Arrigoni, Elena
, Tiseo, Marcello
, Crucitta, Stefania
, Rofi, Eleonora
, Restante, Giuliana
, Marzia Del Re
, Morganti, Riccardo
, Minari, Roberta
, Chella, Antonio
, Danesi, Romano
, Bordi, Paola
in
Epidermal growth factor receptors
/ Gene frequency
/ Mutation
/ Non-small cell lung carcinoma
/ Patients
/ Targeted cancer therapy
2018
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While trying to remove the title from your shelf something went wrong :( Kindly try again later!
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The amount of activating EGFR mutations in circulating cell-free DNA is a marker to monitor osimertinib response
by
Valleggi, Simona
, Petrini, Iacopo
, Arrigoni, Elena
, Tiseo, Marcello
, Crucitta, Stefania
, Rofi, Eleonora
, Restante, Giuliana
, Marzia Del Re
, Morganti, Riccardo
, Minari, Roberta
, Chella, Antonio
, Danesi, Romano
, Bordi, Paola
in
Epidermal growth factor receptors
/ Gene frequency
/ Mutation
/ Non-small cell lung carcinoma
/ Patients
/ Targeted cancer therapy
2018
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The amount of activating EGFR mutations in circulating cell-free DNA is a marker to monitor osimertinib response
Journal Article
The amount of activating EGFR mutations in circulating cell-free DNA is a marker to monitor osimertinib response
2018
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Overview
BackgroundCirculating cell-free DNA (cfDNA) may help understand the molecular response to pharmacologic treatment and provide information on dynamics of clonal heterogeneity. Therefore, this study evaluated the correlation between treatment outcome and activating EGFR mutations (act-EGFR) and T790M in cfDNA in patients with advanced NSCLC given osimertinib.MethodsThirty-four NSCLC patients resistant to first/second-generation EGFR-TKIs, positive for both act-EGFR and T790M in cfDNA at the time of progression were enrolled in this study. Plasma samples were obtained at osimertinib baseline and after 3 months of therapy; cfDNA was analyzed by droplet digital PCR and results were expressed as mutant allele frequency (MAF).ResultsAt baseline, act-EGFR MAF was significantly higher than T790M (p < 0.0001). act-EGFR MAF and T790M/act-EGFR MAF ratio were significantly correlated with disease response (p = 0.02). Cut-off values of act-EGFR MAF and T790M/act-EGFR ratio of 2.6% and 0.22 were found, respectively. The PFS of patients with act-EGFR MAF of > 2.6% and < 2.6%, were 10 months vs. not reached, respectively (p = 0.03), whereas patients with T790M/act-EGFR ≤ 0.22 had poorer PFS than patients with a value of > 0.22 (6 months vs. not reached, respectively, p = 0.01).Conclusionact-EGFR MAF and T790M/act-EGFR MAF ratio are potential markers of outcome in patients treated with osimertinib.
Publisher
Nature Publishing Group
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