CTNND1 is involved in germline predisposition to early-onset gastric cancer by affecting cell-to-cell interactions
Herrera-Pariente, Cristina ; Bonjoch, Laia ; Muñoz, Jenifer ; Fernàndez, Guerau ; Soares de Lima, Yasmin ; Mahmood, Romesa ; Cuatrecasas, Miriam ; Ocaña, Teresa ; Lopez-Prades, Sandra ; Llargués-Sistac, Gemma ; Domínguez-Rovira, Xavier ; Llach, Joan ; Luzko, Irina ; Díaz-Gay, Marcos ; Lazaro, Conxi ; Brunet, Joan ; Castillo-Manzano, Carmen ; García-González, María Asunción ; Lanas, Ángel (Universidad de Zaragoza) ; Carrillo, Marta ; Hernández San Gil, Raquel ; Quintero, Enrique ; Sala, Nuria ; Llort, Gemma ; Aguilera, Lara ; Carot, Laura ; Diez-Redondo, Pilar ; Jover, Rodrigo ; Ramon y Cajal, Teresa ; Cubiella, Joaquín ; Castells, Antoni ; Balaguer, Francesc ; Bujanda, Luis ; Castellví-Bel, Sergi ; Moreira, Leticia
Resumen: Background: CDH1 and CTNNA1 remain as the main genes for hereditary gastric cancer. However, they only explain a small fraction of gastric cancer cases with suspected inherited basis. In this study, we aimed to identify new hereditary genes for early-onset gastric cancer patients (EOGC;<50 years old).
Methods: After germline exome sequencing in 20 EOGC patients and replication of relevant fndings by gene-panel sequencing in an independent cohort of 152 patients, CTNND1 stood out as an interesting candidate gene, since its protein product (p120ctn) directly interacts with E-cadherin. We proceeded with functional characterization by generating two knockout CTNND1 cellular models by gene editing and introducing the detected genetic variants using a lentiviral delivery system. We assessed β-catenin and E-cadherin levels, cell detachment, as well as E-cadherin localization and cell-to-cell interaction by spheroid modeling.
Results: Three CTNND1 germline variants [c.28_29delinsCT, p.(Ala10Leu); c.1105C>T, p.(Pro369Ser); c.1537A > G, p.(Asn513Asp)] were identifed in our EOGC cohorts. Cells encoding CTNND1 variants displayed altered E-cadherin levels and intercellular interactions. In addition, the p.(Pro369Ser) variant, located in a key region in the E-cadherin/p120ctn binding domain, showed E-cadherin mislocalization.
Conclusions: Defects in CTNND1 could be involved in germline predisposition to gastric cancer by altering E-cadherin and, consequently, cell-to-cell interactions. In the present study, CTNND1 germline variants explained 2% (3/172) of the cases, although further studies in larger external cohorts are needed.
Idioma: Inglés
DOI: 10.1007/s10120-024-01504-7
Año: 2024
Publicado en: Gastric Cancer 27, 4 (2024), 747-759
ISSN: 1436-3291
Financiación: info:eu-repo/grantAgreement/EC/HORIZON EUROPE/101079217/EU/TWINNING FOR A EUROPEAN CONSORTIUM OF RECTAL CANCER RESEARCH INSTITUTIONS THROUGH STEPPING UP SCIENTIFIC, TECHNOLOGICAL AND INNOVATION EXCELLENCE OF IORS/STEPUPIORS
Financiación: info:eu-repo/grantAgreement/ES/ISCIII/PI16-00599
Financiación: info:eu-repo/grantAgreement/ES/ISCIII/PI20-00113
Financiación: info:eu-repo/grantAgreement/ES/ISCIII/PI21-00333
Financiación: info:eu-repo/grantAgreement/ES/ISCIII/PI22-00537
Tipo y forma: Article (Published version)
Área (Departamento): Area Medicina (Dpto. Medicina, Psiqu. y Derm.)
You must give appropriate credit, provide a link to the license, and indicate if changes were made. You may do so in any reasonable manner, but not in any way that suggests the licensor endorses you or your use.
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Methods: After germline exome sequencing in 20 EOGC patients and replication of relevant fndings by gene-panel sequencing in an independent cohort of 152 patients, CTNND1 stood out as an interesting candidate gene, since its protein product (p120ctn) directly interacts with E-cadherin. We proceeded with functional characterization by generating two knockout CTNND1 cellular models by gene editing and introducing the detected genetic variants using a lentiviral delivery system. We assessed β-catenin and E-cadherin levels, cell detachment, as well as E-cadherin localization and cell-to-cell interaction by spheroid modeling.
Results: Three CTNND1 germline variants [c.28_29delinsCT, p.(Ala10Leu); c.1105C>T, p.(Pro369Ser); c.1537A > G, p.(Asn513Asp)] were identifed in our EOGC cohorts. Cells encoding CTNND1 variants displayed altered E-cadherin levels and intercellular interactions. In addition, the p.(Pro369Ser) variant, located in a key region in the E-cadherin/p120ctn binding domain, showed E-cadherin mislocalization.
Conclusions: Defects in CTNND1 could be involved in germline predisposition to gastric cancer by altering E-cadherin and, consequently, cell-to-cell interactions. In the present study, CTNND1 germline variants explained 2% (3/172) of the cases, although further studies in larger external cohorts are needed.
Idioma: Inglés
DOI: 10.1007/s10120-024-01504-7
Año: 2024
Publicado en: Gastric Cancer 27, 4 (2024), 747-759
ISSN: 1436-3291
Financiación: info:eu-repo/grantAgreement/EC/HORIZON EUROPE/101079217/EU/TWINNING FOR A EUROPEAN CONSORTIUM OF RECTAL CANCER RESEARCH INSTITUTIONS THROUGH STEPPING UP SCIENTIFIC, TECHNOLOGICAL AND INNOVATION EXCELLENCE OF IORS/STEPUPIORS
Financiación: info:eu-repo/grantAgreement/ES/ISCIII/PI16-00599
Financiación: info:eu-repo/grantAgreement/ES/ISCIII/PI20-00113
Financiación: info:eu-repo/grantAgreement/ES/ISCIII/PI21-00333
Financiación: info:eu-repo/grantAgreement/ES/ISCIII/PI22-00537
Tipo y forma: Article (Published version)
Área (Departamento): Area Medicina (Dpto. Medicina, Psiqu. y Derm.)
You must give appropriate credit, provide a link to the license, and indicate if changes were made. You may do so in any reasonable manner, but not in any way that suggests the licensor endorses you or your use. Exportado de SIDERAL (2024-06-27-13:20:53)
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Record created 2024-06-27, last modified 2024-06-27