Author
Listed:
- Stasa Stankovic
(University of Cambridge)
- Saleh Shekari
(University of Exeter
University of Queensland)
- Qin Qin Huang
(Wellcome Genome Campus)
- Eugene J. Gardner
(University of Cambridge)
- Erna V. Ivarsdottir
(deCODE Genetics/Amgen)
- Nick D. L. Owens
(University of Exeter)
- Nasim Mavaddat
(University of Cambridge)
- Ajuna Azad
(University of Copenhagen)
- Gareth Hawkes
(University of Exeter)
- Katherine A. Kentistou
(University of Cambridge)
- Robin N. Beaumont
(University of Exeter)
- Felix R. Day
(University of Cambridge)
- Yajie Zhao
(University of Cambridge)
- Hakon Jonsson
(deCODE Genetics/Amgen)
- Thorunn Rafnar
(deCODE Genetics/Amgen)
- Vinicius Tragante
(deCODE Genetics/Amgen)
- Gardar Sveinbjornsson
(deCODE Genetics/Amgen)
- Asmundur Oddsson
(deCODE Genetics/Amgen)
- Unnur Styrkarsdottir
(deCODE Genetics/Amgen)
- Julius Gudmundsson
(deCODE Genetics/Amgen)
- Simon N. Stacey
(deCODE Genetics/Amgen)
- Daniel F. Gudbjartsson
(deCODE Genetics/Amgen)
- Kitale Kennedy
(University of Exeter)
- Andrew R. Wood
(University of Exeter)
- Michael N. Weedon
(University of Exeter)
- Ken K. Ong
(University of Cambridge
University of Cambridge)
- Caroline F. Wright
(University of Exeter)
- Eva R. Hoffmann
(University of Copenhagen)
- Patrick Sulem
(deCODE Genetics/Amgen)
- Matthew E. Hurles
(Wellcome Genome Campus)
- Katherine S. Ruth
(University of Exeter)
- Hilary C. Martin
(Wellcome Genome Campus)
- Kari Stefansson
(deCODE Genetics/Amgen)
- John R. B. Perry
(University of Cambridge
University of Cambridge)
- Anna Murray
(University of Exeter)
Abstract
Human genetic studies of common variants have provided substantial insight into the biological mechanisms that govern ovarian ageing1. Here we report analyses of rare protein-coding variants in 106,973 women from the UK Biobank study, implicating genes with effects around five times larger than previously found for common variants (ETAA1, ZNF518A, PNPLA8, PALB2 and SAMHD1). The SAMHD1 association reinforces the link between ovarian ageing and cancer susceptibility1, with damaging germline variants being associated with extended reproductive lifespan and increased all-cause cancer risk in both men and women. Protein-truncating variants in ZNF518A are associated with shorter reproductive lifespan—that is, earlier age at menopause (by 5.61 years) and later age at menarche (by 0.56 years). Finally, using 8,089 sequenced trios from the 100,000 Genomes Project (100kGP), we observe that common genetic variants associated with earlier ovarian ageing associate with an increased rate of maternally derived de novo mutations. Although we were unable to replicate the finding in independent samples from the deCODE study, it is consistent with the expected role of DNA damage response genes in maintaining the genetic integrity of germ cells. This study provides evidence of genetic links between age of menopause and cancer risk.
Suggested Citation
Stasa Stankovic & Saleh Shekari & Qin Qin Huang & Eugene J. Gardner & Erna V. Ivarsdottir & Nick D. L. Owens & Nasim Mavaddat & Ajuna Azad & Gareth Hawkes & Katherine A. Kentistou & Robin N. Beaumont , 2024.
"Genetic links between ovarian ageing, cancer risk and de novo mutation rates,"
Nature, Nature, vol. 633(8030), pages 608-614, September.
Handle:
RePEc:nat:nature:v:633:y:2024:i:8030:d:10.1038_s41586-024-07931-x
DOI: 10.1038/s41586-024-07931-x
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