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dc.contributor.authorJ., Vidal
dc.contributor.authorB., Bellosillo
dc.contributor.authorC., Santos Vivas
dc.contributor.authorP., Garcia-Alfonso
dc.contributor.authorA., Carrato
dc.contributor.authorM.T., Cano
dc.contributor.authorR., Garcia-Carbonero
dc.contributor.authorE., Elez
dc.contributor.authorF., Losa
dc.contributor.authorB., Massuti
dc.contributor.authorValladares Ayerbes, Manuel 
dc.contributor.authorJ.M., Vieitez
dc.contributor.authorJ.L., Manzano
dc.contributor.authorD., Azuara
dc.contributor.authorJ., Gallego
dc.contributor.authorS., Pairet
dc.contributor.authorG., Capella
dc.contributor.authorR., Salazar
dc.contributor.authorJ., Tabernero
dc.contributor.authorE., Aranda
dc.contributor.authorC., Montagut
dc.date.accessioned2022-02-01T13:00:38Z
dc.date.available2022-02-01T13:00:38Z
dc.date.issued2019
dc.identifier.issn0923-7534
dc.identifier.otherhttps://www.ncbi.nlm.nih.gov/pubmed/30689692es
dc.identifier.urihttp://hdl.handle.net/20.500.11940/16061
dc.description.abstractBACKGROUND: Extended RAS analysis is mandatory in metastatic colorectal cancer (mCRC) patients. The optimal threshold of RAS mutated subclones to identify patients most likely to benefit from antiepidermal growth factor receptor (EGFR) therapy is controversial. Our aim was to assess the clinical impact of detecting mutations in RAS, BRAF, PIK3CA and EGFRS492R in basal tissue tumour samples by using a highly sensitive next-generation sequencing (NGS) technology in mCRC patients treated with chemotherapy plus anti-EGFR or anti-vascular endothelial growth factor. PATIENTS AND METHODS: Five hundred and eighty-one tumour samples from untreated mCRC patients from 7 clinical studies were collected. Mutational analysis was carried out by standard-of-care (therascreen pyro) with a sensitivity detection of 5% mutant allele fraction (MAF), and compared with NGS technology using 454GS Junior platform (Roche Applied Science, Germany) with a sensitivity of 1%. Molecular results were correlated with clinical outcomes. RESULTS: After quality assessment, 380 samples were evaluable for molecular analysis. Standard-of-care mutational analysis detected RAS, BRAFV600E or PIK3CA mutations in 56.05% of samples compared with 69.21% by NGS (P = 0.00018). NGS identified coexistence of multiple low-frequency mutant alleles in 96 of the 263 mutated cases (36.5%; range 2-7). Response rate (RR), progression-free survival (PFS) and overall survival (OS) were increasingly improved in patients with RAS wild-type, RAS/BRAF wild-type or quadruple (KRAS/NRAS/BRAF/PIK3CA) wild-type tumours treated with anti-EGFR, assessed by standard-of-care. No additional benefit in RR, PFS or OS was observed by increasing the detection threshold to 1% by NGS. An inverse correlation between the MAF of the most prevalent mutation detected by NGS and anti-EGFR response was observed (P = 0.039). EGFRS492Rmutation was not detected in untreated samples. CONCLUSIONS: No improvement in the selection of patients for anti-EGFR therapy was obtained by adjusting the mutation detection threshold in tissue samples from 5% to 1% MAF. Response to anti-EGFR was significantly better in patients with quadruple wild-type tumours.en
dc.language.isoenges
dc.rightsAttribution-NonCommercial-NoDerivatives 4.0 International*
dc.rights.urihttps://creativecommons.org/licenses/by-nc-nd/4.0/*
dc.subject.meshMembrane Proteins*
dc.subject.meshAdult*
dc.subject.meshProto-Oncogene Proteins B-raf*
dc.subject.meshMiddle Aged*
dc.subject.meshNeoplasm Metastasis*
dc.subject.meshGTP Phosphohydrolases*
dc.subject.meshProtein Kinase Inhibitors*
dc.subject.meshProto-Oncogene Proteins p21(ras)*
dc.subject.meshAntineoplastic Combined Chemotherapy Protocols*
dc.subject.meshMutation*
dc.subject.meshClass I Phosphatidylinositol 3-Kinases*
dc.subject.meshDNA Mutational Analysis*
dc.subject.meshHumans*
dc.subject.meshTreatment Outcome*
dc.subject.meshDisease-Free Survival*
dc.subject.meshHigh-Throughput Nucleotide Sequencing*
dc.subject.meshColorectal Neoplasms*
dc.titleUltra-selection of metastatic colorectal cancer patients using next-generation sequencing to improve clinical efficacy of anti-EGFR therapyen
dc.typeArtigoes
dc.identifier.doi10.1093/annonc/mdz005
dc.identifier.pmid30689692
dc.identifier.sophos34051
dc.issue.number3es
dc.journal.titleANNALS OF ONCOLOGYes
dc.organizationServizo Galego de Saúde::Estrutura de Xestión Integrada (EOXI)::EOXI de A Coruña - Complexo Hospitalario Universitario de A Coruña::Oncoloxía médicaes
dc.page.initial439es
dc.page.final446es
dc.relation.publisherversionhttps://www.annalsofoncology.org/article/S0923-7534(19)31085-3/pdfes
dc.rights.accessRightsopenAccesses
dc.subject.decsmutación*
dc.subject.decsresultado del tratamiento*
dc.subject.decsGTP fosfohidrolasas*
dc.subject.decsanálisis de mutaciones del ADN*
dc.subject.decssecuenciación de nucleótidos de alto rendimiento*
dc.subject.decsmediana edad*
dc.subject.decsmetástasis neoplásica*
dc.subject.decsadulto*
dc.subject.decsproteínas protooncogénicas p21(ras)*
dc.subject.decsprotocolos de quimioterapia antineoplásica combinada*
dc.subject.decssupervivencia sin enfermedad*
dc.subject.decsproteínas de membranas*
dc.subject.decshumanos*
dc.subject.decsproteínas protooncogénicas B-raf*
dc.subject.decsinhibidores de proteína cinasas*
dc.subject.decsfosfatidilinositol 3-cinasas de clase I*
dc.subject.decsneoplasias colorrectales*
dc.subject.keywordCHUACes
dc.typefidesArtículo Originales
dc.typesophosArtículo Originales
dc.volume.number30es


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Attribution-NonCommercial-NoDerivatives 4.0 International
Excepto si se señala otra cosa, la licencia del ítem se describe como Attribution-NonCommercial-NoDerivatives 4.0 International