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Impact of germline RAD51D mutations on breast cancer: Susceptibility to DNA-damaging agents

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dc.contributor.authorJo, Seongyeon-
dc.contributor.authorShim, Wan Cheol-
dc.contributor.authorPark, Shinyoung-
dc.contributor.authorKweon, Taeyong-
dc.contributor.authorRyu, Won-Ji-
dc.contributor.authorHwang, Yumi-
dc.contributor.authorKim, Min Woo-
dc.contributor.authorAhn, Jee Hyun-
dc.contributor.authorLee, Yoon Jung-
dc.contributor.authorLee, Sun Hwa-
dc.contributor.authorWon, Dongju-
dc.contributor.authorNam, Eun Ji-
dc.contributor.authorHan, Jung Woo-
dc.contributor.authorKim, Tae Il-
dc.contributor.authorPark, Ji Soo-
dc.contributor.authorPark, Hyung Seok-
dc.date.accessioned2026-07-13T02:06:59Z-
dc.date.available2026-07-13T02:06:59Z-
dc.date.created2026-07-07-
dc.date.issued2026-06-
dc.identifier.issn2950-3299-
dc.identifier.urihttps://ir.ymlib.yonsei.ac.kr/handle/22282913/212970-
dc.description.abstractGermline mutations in homologous recombination-related genes significantly increase the lifetime risk of breast, ovarian, and other cancers; thus, the concept of BRCAness has been extensively studied. In this study, we aimed to investigate the association between germline RAD51D mutations and breast cancer in clinical and experimental settings. Germline pathogenic or likely pathogenic variants in RAD51D were identified through multigene panel testing in the PLEASANT studies. Fourteen cases of breast cancer with germline pathogenic or likely pathogenic variants in RAD51D were identified. Compared to 1,446 wild-type cases of breast cancer, they appeared to be more aggressive. The proportion of patients with triple-negative breast cancer (TNBC) was higher and larger tumors (>2 cm) were more common. RAD51D-deficient tumors showed better pathological complete responses, defined as ypT0 ypN0, to neoadjuvant chemotherapy. Based on clinical findings, we analyzed the impact of RAD51D-deficiency on drug sensitivity in vitro to identify targetable vulnerabilities in RAD51D-deficient tumors. These TNBC cells were significantly more sensitive to cisplatin than wild-type TNBC cells, consistent with our clinical data. In conclusion, RAD51D-deficient tumors were shown to have a phenotype similar to that of BRCA1-deficient tumors, and further investigation of responses to DNA-damaging agents, particularly platinum-based chemotherapy, is warranted.-
dc.language영어-
dc.publisherCELL PRESS-
dc.relation.isPartOfMOLECULAR THERAPY ONCOLOGY-
dc.titleImpact of germline RAD51D mutations on breast cancer: Susceptibility to DNA-damaging agents-
dc.typeArticle-
dc.contributor.googleauthorJo, Seongyeon-
dc.contributor.googleauthorShim, Wan Cheol-
dc.contributor.googleauthorPark, Shinyoung-
dc.contributor.googleauthorKweon, Taeyong-
dc.contributor.googleauthorRyu, Won-Ji-
dc.contributor.googleauthorHwang, Yumi-
dc.contributor.googleauthorKim, Min Woo-
dc.contributor.googleauthorAhn, Jee Hyun-
dc.contributor.googleauthorLee, Yoon Jung-
dc.contributor.googleauthorLee, Sun Hwa-
dc.contributor.googleauthorWon, Dongju-
dc.contributor.googleauthorNam, Eun Ji-
dc.contributor.googleauthorHan, Jung Woo-
dc.contributor.googleauthorKim, Tae Il-
dc.contributor.googleauthorPark, Ji Soo-
dc.contributor.googleauthorPark, Hyung Seok-
dc.identifier.doi10.1016/j.omton.2026.201242-
dc.identifier.pmid42306566-
dc.contributor.affiliatedAuthorJo, Seongyeon-
dc.contributor.affiliatedAuthorShim, Wan Cheol-
dc.contributor.affiliatedAuthorPark, Shinyoung-
dc.contributor.affiliatedAuthorKweon, Taeyong-
dc.contributor.affiliatedAuthorRyu, Won-Ji-
dc.contributor.affiliatedAuthorHwang, Yumi-
dc.contributor.affiliatedAuthorKim, Min Woo-
dc.contributor.affiliatedAuthorAhn, Jee Hyun-
dc.contributor.affiliatedAuthorWon, Dongju-
dc.contributor.affiliatedAuthorNam, Eun Ji-
dc.contributor.affiliatedAuthorHan, Jung Woo-
dc.contributor.affiliatedAuthorKim, Tae Il-
dc.contributor.affiliatedAuthorPark, Ji Soo-
dc.contributor.affiliatedAuthorPark, Hyung Seok-
dc.identifier.scopusid2-s2.0-105040805270-
dc.identifier.wosid001793311700001-
dc.citation.volume34-
dc.citation.number2-
dc.identifier.bibliographicCitationMOLECULAR THERAPY ONCOLOGY, Vol.34(2), 2026-06-
dc.identifier.rimsid94525-
dc.type.rimsART-
dc.description.journalClass1-
dc.description.journalClass1-
dc.subject.keywordPlusPATHOLOGICAL COMPLETE RESPONSE-
dc.subject.keywordPlusHOMOLOGOUS RECOMBINATION-
dc.subject.keywordPlusCELLULAR-RESPONSE-
dc.subject.keywordPlusREPAIR DEFECTS-
dc.subject.keywordPlusBRCA MUTATION-
dc.subject.keywordPlusOVARIAN-
dc.subject.keywordPlusGENES-
dc.subject.keywordPlusASSOCIATION-
dc.subject.keywordPlusPOLYMERASE-
dc.subject.keywordPlusPARALOGS-
dc.type.docTypeArticle-
dc.description.isOpenAccessY-
dc.description.journalRegisteredClassscie-
dc.description.journalRegisteredClassscopus-
dc.relation.journalWebOfScienceCategoryOncology-
dc.relation.journalWebOfScienceCategoryMedicine, Research & Experimental-
dc.relation.journalResearchAreaOncology-
dc.relation.journalResearchAreaResearch & Experimental Medicine-
dc.identifier.articleno201242-
Appears in Collections:
1. College of Medicine (의과대학) > Dept. of Internal Medicine (내과학교실) > 1. Journal Papers
1. College of Medicine (의과대학) > Dept. of Surgery (외과학교실) > 1. Journal Papers
1. College of Medicine (의과대학) > Dept. of Laboratory Medicine (진단검사의학교실) > 1. Journal Papers
1. College of Medicine (의과대학) > Dept. of Obstetrics and Gynecology (산부인과학교실) > 1. Journal Papers
1. College of Medicine (의과대학) > Dept. of Pediatrics (소아과학교실) > 1. Journal Papers

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