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APA
Romero, Atocha & Jantus Lewintre, Eloisa & García Pelaez, Beatriz & Royuela, Ana & Insa, Amelia & Cruz, Patricia & Collazo, Ana & Perez Altozano, Javier & Juan Vidal, Oscar & Diz, Pilar & Cobo, Manuel & Hernandez, Berta & Vazquez Estevez, Sergio & Benítez, Gretel & Guirado, Maria & Majem, Margarita & Bernabe, Reyes & Ortega, Ana Laura & Blasco, Ana & Bosch Barrera, Joaquim & Jurado, Jose M. & García Gonzalez, Jorge & Viteri, Santiago & Garcia Giron, Carlos & Massutí, Bartomeu & López Martín, Ana & Rodriguez Festa, Alejandro & Calabuig Fariñas, Silvia & Molina Vila, Miguel Angel & Provencio, Mariano (ISO 690
Romero, Atocha & Jantus Lewintre, Eloisa & García Pelaez, Beatriz & Royuela, Ana & Insa, Amelia & Cruz, Patricia & Collazo, Ana & Perez Altozano, Javier & Juan Vidal, Oscar & Diz, Pilar & Cobo, Manuel & Hernandez, Berta & Vazquez Estevez, Sergio & Benítez, Gretel & Guirado, Maria & Majem, Margarita & Bernabe, Reyes & Ortega, Ana Laura & Blasco, Ana & Bosch Barrera, Joaquim & Jurado, Jose M. & García Gonzalez, Jorge & Viteri, Santiago & Garcia Giron, Carlos & Massutí, Bartomeu & López Martín, Ana & Rodriguez Festa, Alejandro & Calabuig Fariñas, Silvia & Molina Vila, Miguel Angel & Provencio, Mariano.Comprehensive cross-platform comparison of methods for non-invasive EGFR mutation testing: results of the RING observational trial
Romero, Atocha; Jantus Lewintre, Eloisa; García Pelaez, Beatriz; Royuela, Ana; Insa, Amelia; Cruz, Patricia; Collazo, Ana; Perez Altozano, Javier; Juan Vidal, Oscar; Diz, Pilar; Cobo, Manuel; Hernandez, Berta; Vazquez Estevez, Sergio; Benítez, Gretel; Guirado, Maria; Majem, Margarita; Bernabe, Reyes; Ortega, Ana Laura; Blasco, Ana; Bosch Barrera, Joaquim; Jurado, Jose M.; García Gonzalez, Jorge; Viteri, Santiago; Garcia Giron, Carlos; Massutí, Bartomeu; López Martín, Ana; Rodriguez Festa, Alejandro; Calabuig Fariñas, Silvia; Molina Vila, Miguel Angel; Provencio, Mariano
Fecha:
2021
Resumen:
Several platforms for noninvasive EGFR testing are currently used in the
clinical setting with sensitivities ranging from 30% to 100%. Prospective
studies evaluating agreement and sources for discordant results remain
lacking. Herein, seven methodologies including two next-generation sequencing (NGS)-based methods, three high-sensitivity PCR-based plat forms, and two FDA-approved methods were compared using 72 plasma
samples, from EGFR-mutant non-small-cell lung cancer (NSCLC) patients
progressing on a first-line tyrosine kinase inhibitor (TKI). NGS platforms
as well as high-sensitivity PCR-based methodologies showed excellent
agreement for EGFR-sensitizing mutations (K = 0.80¿0.89) and substantial
agreement for T790M testing (K = 0.77 and 0.68, respectively). Mutant
allele frequencies (MAFs) obtained by different quantitative methods
showed an excellent reproducibility (intraclass correlation coefficients 0.86¿
0.98). Among other technical factors, discordant calls mostly occurred at
mutant allele frequencies (MAFs) ¿ 0.5%. Agreement significantly
improved when discarding samples with MAF ¿ 0.5%. EGFR mutations
were detected at significantly lower MAFs in patients with brain metas tases, suggesting that these patients risk for a false-positive result. Our
results support the use of liquid biopsies for noninvasive EGFR testing and
highlight the need to systematically report MAFs.
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