Meta-analysis of genome-wide association studies for cancer therapy-related cardiovascular dysfunction and functional mapping highlight an intergenic region close to TP63

Laura Martínez-Campelo(Instituto de Investigación Sanitaria de Santiago), Alejandro Blanco‐Verea(Instituto de Investigación Sanitaria de Santiago), Teresa López‐Fernández(Hospital Universitario La Paz), Amparo Martínez‐Monzonís(Complejo Hospitalario Universitario de Santiago), A. Buño(Hospital Universitario La Paz), Pilar Mazón(Complejo Hospitalario Universitario de Santiago), Pilar Zamora(Hospital Universitario La Paz), Nadine Norton(Mayo Clinic in Florida), Joseph S. Reddy(Mayo Clinic in Florida), Alejandro Velasco-Ruíz(Spanish National Cancer Research Centre), Anna González‐Neira(Spanish National Cancer Research Centre), Christof Vulsteke(University of Antwerp), T. Alonso-Gordoa(Hospital Universitario Ramón y Cajal), Raquel Cruz(Universidade de Santiago de Compostela), Silvia Diz‐de Almeida(Universidade de Santiago de Compostela), Ángel Carracedo(Universidade de Santiago de Compostela), JR González-Juanatey(Complejo Hospitalario Universitario de Santiago), José López‐Sendón(Hospital Universitario La Paz), Marı́a Brión(Complejo Hospitalario Universitario de Santiago), The CardioTox registry investigators(Hospital Universitario La Paz), J. López Sendón(Hospital Universitario La Paz), Antonio Buño Soto(Hospital Universitario La Paz), Miguel Canales(Hospital Universitario La Paz), Enrique Espinosa(Hospital Universitario La Paz), Jaime Feliú Batlle(Hospital Universitario La Paz), Teresa López‐Fernández(Hospital Universitario La Paz), Esteban López de Sá(Hospital Universitario La Paz), Mar Moreno Yangüela(Hospital Universitario La Paz), Elena Ramı́rez(Hospital Universitario La Paz), Olaia Rodríguez Fraga(Hospital Universitario La Paz), Investigators(Hospital Universitario La Paz), Ainara Albaladejo(Hospital Universitario La Paz), Guiomar Mediavilla(Hospital Universitario La Paz), Carlos Álvarez-Ortega(Hospital Universitario La Paz), Mar Moreno Yangüela(Hospital Universitario La Paz), Silvia Valbuena-López(Hospital Universitario La Paz), Regina Dalmau(Hospital Universitario La Paz), Almudena Castro(Hospital Universitario La Paz), Esteban López de Sá(Hospital Universitario La Paz), Juan Caro Codón(Hospital Universitario La Paz), Pilar Auñón(Hospital Universitario La Paz), Jaime Feliú Batlle(Hospital Universitario La Paz), Enrique Espinosa(Hospital Universitario La Paz), Beatriz Castelo(Hospital Universitario La Paz), Andrés Redondo(Hospital Universitario La Paz), Álvaro Pinto(Hospital Universitario La Paz), Miguel Canales(Hospital Universitario La Paz), Pilar Gómez Prieto(Hospital Universitario La Paz), Patricia Chanca(Hospital Universitario La Paz), Paloma Oliver(Hospital Universitario La Paz), Olaia Rodríguez Fraga(Hospital Universitario La Paz), Isabel Rodrı́guez(Hospital Universitario La Paz), Lara Miralles(Hospital Universitario La Paz), Belén Belinchón(Hospital Universitario La Paz), Á. Manso(Hospital Universitario La Paz), Rosa Moreiras(Hospital Universitario La Paz), Gema Casado(Hospital Universitario La Paz), Alicia Herrero(Hospital Universitario La Paz), José González‐Costello(Bellvitge University Hospital), Sonia Pernas Simón(Bellvitge University Hospital), José Ramón González‐Juanatey(Complejo Hospitalario Universitario de Santiago), Pilar Mazón‐Ramos(Complejo Hospitalario Universitario de Santiago), A. Martínez Monzonís(Complejo Hospitalario Universitario de Santiago), Rafael López López(Complejo Hospitalario Universitario de Santiago), Patricia Palacios Ozores(Complejo Hospitalario Universitario de Santiago), Milagros Pedreira Pérez(Complejo Hospitalario Universitario de Santiago), Belén Álvarez Álvarez(Complejo Hospitalario Universitario de Santiago), B. Campos Balea(Hospital Universitario Lucus Augusti), Carlos González-Juanatey(Hospital Universitario Lucus Augusti), Ana Testa Fernández(Hospital Universitario Lucus Augusti), Silvia Varela Ferreiro(Hospital Universitario Lucus Augusti), José María Serrano Antolín(Hospital Universitario de Fuenlabrada), Juan Antonio Guerra(Hospital Universitario de Fuenlabrada), Luis Javier Morales García(Hospital Universitario de Fuenlabrada), Carlos Gutiérrez‐Landaluce(Hospital Universitario de Fuenlabrada), Elena Merino(Hospital Universitario de Fuenlabrada), Nieves Estival Ortega(Hospital General Universitario Gregorio Marañón), Joaquín Alonso(Hospital General Universitario Gregorio Marañón), Francisco Fernández‐Avilés(Hospital General Universitario Gregorio Marañón), Ana González‐Mansilla(Hospital General Universitario Gregorio Marañón), Pilar García‐Alfonso(Hospital General Universitario Gregorio Marañón), Rosalía Cadenas Chamorro(Hospital Universitario Infanta Sofía), María Merino Salvador(Hospital Universitario Infanta Sofía), Ignacio Plaza(Hospital Universitario Infanta Sofía), Vicente Bertomeu‐González(Hospital Universitario Infanta Sofía), Juan Quiles(Hospital Universitario Infanta Sofía)
Scientific Reports
August 8, 2024
10.1038/s41598-024-69064-5
Cited by 7Open Access
Full Text

Abstract

Cancer therapy-related cardiac dysfunction (CTRCD), which commonly includes left ventricular dysfunction and heart failure, is the main adverse effect of anticancer therapy. In recent years several candidate genes studies and genome-wide association studies have identified common genetic variants associated with CTRCD, but evidence remains limited and few genetic variants are robust. A genome-wide meta-analysis of CTRCD was performed with 852 oncology patients receiving cancer therapy. DNA samples were genotyped and imputed to perform a GWAS meta-analysis for case–control (N = 852 (380 cases and 472 controls) and extreme phenotypes (N = 618 (78 cases and 472 controls) looking for genetic variants that predispose to CTRCD. The results were validated in a replicate cohort of 1,191 oncology patients (245 cases and 946 controls). Functional mapping of the replicated loci was then performed. The meta-analysis showed 9 and 17 loci suggestively associated (P-value < 1 × 10–5) with CTRCD in case–control and extreme phenotypes analyses, respectively. The 3q28 locus (rs rs7652759, P = 5.64 × 10–6) in the case–control analysis was the strongest signal, with up to 64 SNPs above the suggestive significance threshold. The rs7652759, an intergenic variant between TPRG1 and TP63 genes, was the only variant validated in the replication cohort (P-value = 0.01). Functional mapping of this significant locus revealed up to 5 new genes potentially involved in the CTRCD. We identified the intergenic region near TP63 as a novel CTRCD susceptibility locus. In the future, the genotyping of these markers could be considered in new CTRCD risk scores to improve preventive strategies in cardio-oncology.

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