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dc.date.accessioned 2020-10-29T15:09:08Z
dc.date.available 2020-10-29T15:09:08Z
dc.date.issued 2020
dc.identifier.uri http://sedici.unlp.edu.ar/handle/10915/107940
dc.description.abstract Locally advanced rectal cancer (LARC) remains a medical challenge. Reliable biomarkers to predict which patients will significantly respond to neoadjuvant chemoradiotherapy (nCRT) have not been identified. We evaluated baseline genomic and transcriptomic features to detect differences that may help predict response to nCRT. Eligible LARC patients received nCRT (3D-LCRT 50.4 Gy plus capecitabine 825 mg/m2/bid), preceded by three cycles of CAPOX in high systemic-relapse risk tumors, and subsequent surgery. Frozen tumor biopsies at diagnosis were sequenced using a colorectal cancer panel. Transcriptomic data was used for pathway and cell deconvolution inferential algorithms, coupled with immunohistochemical validation. Clinical and molecular data were analyzed according to nCRT outcome. Pathways related to DNA repair and proliferation (p < 0.005), and co-occurrence of RAS and TP53 mutations (p = 0.001) were associated with poor response. Enrichment of expression signatures related to enhanced immune response, particularly B cells and interferon signaling (p < 0.005), was detected in good responders. Immunohistochemical analysis of CD20⁺ cells validated the association of good response with B cell infiltration (p = 0.047). Findings indicate that the presence of B cells is associated with successful tumor regression following nCRT in LARC. The prevalence of simultaneous RAS and TP53 mutations along with a proficient DNA repair system that may counteract chemoradio-induced DNA damage was associated with poor response. en
dc.language en es
dc.subject rectal cancer es
dc.subject immune response es
dc.subject gene expression es
dc.subject neoadjuvant chemoradiotherapy es
dc.subject biomarker es
dc.title Pre-Existing Tumoral B Cell Infiltration and Impaired Genome Maintenance Correlate with Response to Chemoradiotherapy in Locally Advanced Rectal Cancer en
dc.type Articulo es
sedici.identifier.uri http://europepmc.org/backend/ptpmcrender.fcgi?accid=PMC7464257&blobtype=pdf es
sedici.identifier.uri https://www.mdpi.com/2072-6694/12/8/2227 es
sedici.identifier.other pmid:32784964 es
sedici.identifier.other pmcid:PMC7464257 es
sedici.identifier.other https://doi.org/10.3390/cancers12082227 es
sedici.identifier.issn 2072-6694 es
sedici.creator.person Sendoya, Juan M. es
sedici.creator.person Iseas, Soledad es
sedici.creator.person Coraglio, Mariana es
sedici.creator.person Golubicki, Mariano es
sedici.creator.person Robbio, Juan es
sedici.creator.person Salanova, Ruben es
sedici.creator.person Kujaruk, Mirta es
sedici.creator.person Mikolaitis, Vanesa es
sedici.creator.person Rizzolo, Mariana es
sedici.creator.person Ruiz, Gonzalo es
sedici.creator.person Cabanne, Ana es
sedici.creator.person Gualdrini, Ubaldo es
sedici.creator.person Mendez, Guillermo es
sedici.creator.person Hirmas, Stella es
sedici.creator.person Rotondaro, Cecilia es
sedici.creator.person Viglino, Julieta es
sedici.creator.person Eleta, Martín es
sedici.creator.person Fernandez, Elmer es
sedici.creator.person Abba, Martín Carlos es
sedici.creator.person Podhajcer, Osvaldo es
sedici.creator.person Roca, Enrique es
sedici.creator.person Llera, Andrea S. es
sedici.subject.materias Medicina es
sedici.description.fulltext true es
mods.originInfo.place Facultad de Ciencias Médicas es
mods.originInfo.place Centro de Investigaciones Inmunológicas Básicas y Aplicadas es
sedici.subtype Articulo es
sedici.rights.license Creative Commons Attribution 4.0 International (CC BY 4.0)
sedici.rights.uri http://creativecommons.org/licenses/by/4.0/
sedici.description.peerReview peer-review es
sedici.relation.journalTitle Cancers es
sedici.relation.journalVolumeAndIssue vol. 12, no. 8 es


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Creative Commons Attribution 4.0 International (CC BY 4.0) Excepto donde se diga explícitamente, este item se publica bajo la siguiente licencia Creative Commons Attribution 4.0 International (CC BY 4.0)