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dc.contributor.authorDuque, Galo-
dc.contributor.authorManterola, Carlos-
dc.contributor.authorOtzen, Tamara-
dc.contributor.authorArias, Cristina-
dc.contributor.authorGalindo, Bryan-
dc.contributor.authorMora, Miriam-
dc.contributor.authorGuerrero Quiroz, Enmanuel Isidoro-
dc.contributor.authorGarcía, Nayeli-
dc.date.accessioned2022-03-04T16:55:42Z-
dc.date.available2022-03-04T16:55:42Z-
dc.date.issued2018-
dc.identifier.issn1613-0073-
dc.identifier.urihttps://pubmed.ncbi.nlm.nih.gov/34687555/-
dc.descriptionAdvancements in genetic sequencing techniques along with the identification of specific mutations and structural changes in multiple cancer genes, make it possible to identify circulating tumor cells and cell free nucleic acids as blood-based biomarkers, serving as a liquid biopsy (LB) with great utility for the diagnosis, treatment and follow-up of patients with neoplasms. This systematic review focuses on the clinical utility of LB in patients with breast cancer (BC). Articles published between 1990 and 2021 were included. Databases searched: Trip Database, WoS, EMBASE, PubMed, SCOPUS, and Clinical Keys. Variables studied: Publication year, country, number of cases, primary study design, LB detection methods, genes found, overall survival, disease-free survival, stage, response to treatment, clinical utility, BC molecular type, systemic treatment and methodological quality of primary studies. Of 2619 articles, 74 were retained representing 12 658 patients, mainly cohort studies (66.2%), the majority were from China (15%) and Japan (12.2%). All primary studies described clinical stage and type of systemic treatment used. Most used biomarker detection method: DNA (52.7%) and type of analysis: quantification of total cfDNA (35.1%). PIK3CA mutation was most frequent (62.9%). Evidence suggests clinically useful applications of BC. Though heterogeneous, publications suggest that LB will constitute part of the standard diagnostic-therapeutic process of BC.-
dc.description.abstractAdvancements in genetic sequencing techniques along with the identification of specific mutations and structural changes in multiple cancer genes, make it possible to identify circulating tumor cells and cell free nucleic acids as blood-based biomarkers, serving as a liquid biopsy (LB) with great utility for the diagnosis, treatment and follow-up of patients with neoplasms. This systematic review focuses on the clinical utility of LB in patients with breast cancer (BC). Articles published between 1990 and 2021 were included. Databases searched: Trip Database, WoS, EMBASE, PubMed, SCOPUS, and Clinical Keys. Variables studied: Publication year, country, number of cases, primary study design, LB detection methods, genes found, overall survival, disease-free survival, stage, response to treatment, clinical utility, BC molecular type, systemic treatment and methodological quality of primary studies. Of 2619 articles, 74 were retained representing 12 658 patients, mainly cohort studies (66.2%), the majority were from China (15%) and Japan (12.2%). All primary studies described clinical stage and type of systemic treatment used. Most used biomarker detection method: DNA (52.7%) and type of analysis: quantification of total cfDNA (35.1%). PIK3CA mutation was most frequent (62.9%). Evidence suggests clinically useful applications of BC. Though heterogeneous, publications suggest that LB will constitute part of the standard diagnostic-therapeutic process of BC.-
dc.language.isoes_ES-
dc.sourceCEUR WORKSHOP PROCEEDINGS-
dc.subjectBiomarkers-
dc.subjectBreast cancer-
dc.subjectCell free circulating DNA-
dc.subjectCirculating tumor cells-
dc.subjectLiquid biopsy-
dc.titleClinical utility of liquid biopsy in breast cancer: a systematic review-
dc.title.alternativeClinical utility of liquid biopsy in breast cancer: a systematic review-
dc.typeARTÍCULO-
dc.ucuenca.idautor0000-0003-1306-9392-
dc.ucuenca.idautor0000-0001-9213-2905-
dc.ucuenca.idautor0000-0001-6014-1241-
dc.ucuenca.idautor0000-0002-8737-5109-
dc.ucuenca.idautor0000-0001-8911-7851-
dc.ucuenca.idautor0000-0002-6884-2007-
dc.ucuenca.idautor0104118310-
dc.ucuenca.idautor0000-0003-2725-0707-
dc.identifier.doi10.1111/cge.14077-
dc.ucuenca.versionVersión publicada-
dc.ucuenca.areaconocimientounescoamplio09 - Salud y Bienestar-
dc.ucuenca.afiliacionDuque, G., Universidad de la Frontera, Temuco, Chile; Duque, G., Universidad del Azuay, Cuenca, Ecuador-
dc.ucuenca.afiliacionManterola, C., Universidad de la Frontera, Temuco, Chile-
dc.ucuenca.afiliacionOtzen, T., Universidad de la Frontera, Temuco, Chile-
dc.ucuenca.afiliacionArias, C., Universidad del Azuay, Cuenca, Ecuador-
dc.ucuenca.afiliacionGalindo, B., Universidad del Azuay, Cuenca, Ecuador-
dc.ucuenca.afiliacionMora, M., Universidad de la Frontera, Temuco, Chile-
dc.ucuenca.afiliacionGuerrero, E., Instituto del Cáncer SOLCA, CUENCA, Ecuador; Guerrero, E., Universidad de la Frontera, Temuco, Chile-
dc.ucuenca.afiliacionGarcía, N., Universidad de la Frontera, Temuco, Chile-
dc.ucuenca.volumenVolumen 22-31-
dc.ucuenca.indicebibliograficoSIN INDEXAR-
dc.ucuenca.numerocitaciones0-
dc.ucuenca.areaconocimientofrascatiamplio3. Ciencias Médicas y de la Salud-
dc.ucuenca.areaconocimientofrascatiespecifico3.2 Medicina Clínica-
dc.ucuenca.areaconocimientofrascatidetallado3.2.23 Oncología-
dc.ucuenca.areaconocimientounescoespecifico091 - Salud-
dc.ucuenca.areaconocimientounescodetallado0912 - Medicina-
dc.ucuenca.urifuentehttps://http://ceur-ws.org/-
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