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Germline pathogenic variants in the MRE11, RAD50, and NBN (MRN) genes in cancer predisposition: A systematic review and meta-analysis

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Author
Šťastná, BarboraORCiD Profile - 0000-0003-3463-8320WoS Profile - HSF-4697-2023Scopus Profile - 58055722200
Doležalová, TaťánaORCiD Profile - 0009-0002-7205-7287WoS Profile - KLH-6842-2024Scopus Profile - 58931215700
Matějková, Kateřina
Němcová, BarboraWoS Profile - KLQ-1684-2024Scopus Profile - 59068717200
Zemánková, PetraORCiD Profile - 0000-0001-7315-1975WoS Profile - BBB-8243-2020Scopus Profile - 57090750000
Janatová, MarkétaORCiD Profile - 0000-0003-2816-6769WoS Profile - EZJ-1139-2022Scopus Profile - 57217189332
Kleiblová, PetraORCiD Profile - 0000-0002-4806-9854WoS Profile - K-9899-2017Scopus Profile - 22938249100
Soukupová, JanaORCiD Profile - 0000-0003-2413-1542WoS Profile - ABI-2077-2020Scopus Profile - 57222641653
Kleibl, ZdeněkORCiD Profile - 0000-0003-2050-9667WoS Profile - A-2009-2008Scopus Profile - 6602616305

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Publication date
2024
Published in
International Journal of Cancer
Volume / Issue
155 (9)
ISBN / ISSN
ISSN: 0020-7136
ISBN / ISSN
eISSN: 1097-0215
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This publication has a published version with DOI 10.1002/ijc.35066

Abstract
The MRE11, RAD50, and NBN genes encode the MRN complex sensing DNA breaks and directing their repair. While carriers of biallelic germline pathogenic variants (gPV) develop rare chromosomal instability syndromes, the cancer risk in heterozygotes remains controversial. We performed a systematic review and meta-analysis of 53 studies in patients with different cancer diagnoses to better understand the cancer risk. We found an increased risk (odds ratio, 95% confidence interval) for gPV carriers in NBN for melanoma (7.14; 3.30-15.43), pancreatic cancer (4.03; 2.14-7.58), hematological tumors (3.42; 1.14-10.22), and prostate cancer (2.44, 1.84-3.24), but a low risk for breast cancer (1.29; 1.00-1.66) and an insignificant risk for ovarian cancer (1.53; 0.76-3.09). We found no increased breast cancer risk in carriers of gPV in RAD50 (0.93; 0.74-1.16; except of c.687del carriers) and MRE11 (0.87; 0.66-1.13). The secondary burden analysis compared the frequencies of gPV in MRN genes in patients from 150 studies with those in the gnomAD database. In NBN gPV carriers, this analysis additionally showed a high risk for brain tumors (5.06; 2.39-9.52), a low risk for colorectal (1.64; 1.26-2.10) and hepatobiliary (2.16; 1.02-4.06) cancers, and no risk for endometrial, and gastric cancer. The secondary burden analysis showed also a moderate risk for ovarian cancer (3.00; 1.27-6.08) in MRE11 gPV carriers, and no risk for ovarian and hepatobiliary cancers in RAD50 gPV carriers. These findings provide a robust clinical evidence of cancer risks to guide personalized clinical management in heterozygous carriers of gPV in the MRE11, RAD50, and NBN genes.
Keywords
germline variants, meta-analysis, MRE11, NBN, RAD50
Permanent link
https://hdl.handle.net/20.500.14178/2602
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WOS:001254317300001
SCOPUS:2-s2.0-85196858241
PUBMED:38924040
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Full text of this result is licensed under: Creative Commons Uveďte původ 4.0 International

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