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Genetic drivers and cellular selection of female mosaic X chromosome loss

Genetic drivers and cellular selection of female mosaic X chromosome loss
Genetic drivers and cellular selection of female mosaic X chromosome loss

Mosaic loss of the X chromosome (mLOX) is the most common clonal somatic alteration in leukocytes of female individuals1,2, but little is known about its genetic determinants or phenotypic consequences. Here, to address this, we used data from 883,574 female participants across 8 biobanks; 12% of participants exhibited detectable mLOX in approximately 2% of leukocytes. Female participants with mLOX had an increased risk of myeloid and lymphoid leukaemias. Genetic analyses identified 56 common variants associated with mLOX, implicating genes with roles in chromosomal missegregation, cancer predisposition and autoimmune diseases. Exome-sequence analyses identified rare missense variants in FBXO10 that confer a twofold increased risk of mLOX. Only a small fraction of associations was shared with mosaic Y chromosome loss, suggesting that distinct biological processes drive formation and clonal expansion of sex chromosome missegregation. Allelic shift analyses identified X chromosome alleles that are preferentially retained in mLOX, demonstrating variation at many loci under cellular selection. A polygenic score including 44 allelic shift loci correctly inferred the retained X chromosomes in 80.7% of mLOX cases in the top decile. Our results support a model in which germline variants predispose female individuals to acquiring mLOX, with the allelic content of the X chromosome possibly shaping the magnitude of clonal expansion.

0028-0836
134-141
Liu, Aoxing
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Genovese, Giulio
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Zhao, Yajie
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Eccles, Diana
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Liu, Xiaoxi
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Sankaran, Vijay G.
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Natarajan, Pradeep
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McCarroll, Steven A.
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Terao, Chikashi
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Perry, John R.B.
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Machiela, Mitchell J.
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Breast Cancer Association Consortium
Million Veteran Program
FinnGen
Estonian Biobank Research Team
et al.
Liu, Aoxing
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Genovese, Giulio
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Zhao, Yajie
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Eccles, Diana
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Pirinen, Matti
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Kentistou, Katherine A.
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Yang, Zhiyu
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Yu, Kai
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Momozawa, Yukihide
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Pyarajan, Saiju
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Huang, Wen Yi
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Freedman, Neal D.
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Song, Lei
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Gardner, Eugene J.
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Metspalu, Andres
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Esko, Tõnu
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Nelis, Mari
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Milani, Lili
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Sankaran, Vijay G.
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Palotie, Aarno
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Ollila, Hanna M.
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Tukiainen, Taru
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Chanock, Stephen J.
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Mägi, Reedik
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Natarajan, Pradeep
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Daly, Mark J.
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Bick, Alexander
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McCarroll, Steven A.
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Terao, Chikashi
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Loh, Po Ru
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Perry, John R.B.
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Machiela, Mitchell J.
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Liu, Aoxing, Genovese, Giulio and Zhao, Yajie , Breast Cancer Association Consortium, Million Veteran Program, FinnGen, Estonian Biobank Research Team and et al. (2024) Genetic drivers and cellular selection of female mosaic X chromosome loss. Nature, 631 (8019), 134-141, [631]. (doi:10.1038/s41586-024-07533-7).

Record type: Article

Abstract

Mosaic loss of the X chromosome (mLOX) is the most common clonal somatic alteration in leukocytes of female individuals1,2, but little is known about its genetic determinants or phenotypic consequences. Here, to address this, we used data from 883,574 female participants across 8 biobanks; 12% of participants exhibited detectable mLOX in approximately 2% of leukocytes. Female participants with mLOX had an increased risk of myeloid and lymphoid leukaemias. Genetic analyses identified 56 common variants associated with mLOX, implicating genes with roles in chromosomal missegregation, cancer predisposition and autoimmune diseases. Exome-sequence analyses identified rare missense variants in FBXO10 that confer a twofold increased risk of mLOX. Only a small fraction of associations was shared with mosaic Y chromosome loss, suggesting that distinct biological processes drive formation and clonal expansion of sex chromosome missegregation. Allelic shift analyses identified X chromosome alleles that are preferentially retained in mLOX, demonstrating variation at many loci under cellular selection. A polygenic score including 44 allelic shift loci correctly inferred the retained X chromosomes in 80.7% of mLOX cases in the top decile. Our results support a model in which germline variants predispose female individuals to acquiring mLOX, with the allelic content of the X chromosome possibly shaping the magnitude of clonal expansion.

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More information

Accepted/In Press date: 7 May 2024
e-pub ahead of print date: 12 June 2024
Published date: 4 July 2024

Identifiers

Local EPrints ID: 499873
URI: http://eprints.soton.ac.uk/id/eprint/499873
ISSN: 0028-0836
PURE UUID: 87e927c0-211f-4e15-9bdd-330a7dbd0c8c
ORCID for Diana Eccles: ORCID iD orcid.org/0000-0002-9935-3169

Catalogue record

Date deposited: 08 Apr 2025 16:31
Last modified: 09 Apr 2025 01:33

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Contributors

Author: Aoxing Liu
Author: Giulio Genovese
Author: Yajie Zhao
Author: Diana Eccles ORCID iD
Author: Matti Pirinen
Author: Seyedeh M. Zekavat
Author: Katherine A. Kentistou
Author: Zhiyu Yang
Author: Kai Yu
Author: Caitlyn Vlasschaert
Author: Xiaoxi Liu
Author: Derek W. Brown
Author: Georgi Hudjashov
Author: Bryan R. Gorman
Author: Joe Dennis
Author: Weiyin Zhou
Author: Yukihide Momozawa
Author: Saiju Pyarajan
Author: Valdislav Tuzov
Author: Fanny Dhelia Pajuste
Author: Mervi Aavikko
Author: Timo P. Sipilä
Author: Awaisa Ghazal
Author: Wen Yi Huang
Author: Neal D. Freedman
Author: Lei Song
Author: Eugene J. Gardner
Author: Andres Metspalu
Author: Tõnu Esko
Author: Mari Nelis
Author: Lili Milani
Author: Vijay G. Sankaran
Author: Aarno Palotie
Author: Hanna M. Ollila
Author: Taru Tukiainen
Author: Stephen J. Chanock
Author: Reedik Mägi
Author: Pradeep Natarajan
Author: Mark J. Daly
Author: Alexander Bick
Author: Steven A. McCarroll
Author: Chikashi Terao
Author: Po Ru Loh
Author: Andrea Ganna
Author: John R.B. Perry
Author: Mitchell J. Machiela
Corporate Author: Breast Cancer Association Consortium
Corporate Author: Million Veteran Program
Corporate Author: FinnGen
Corporate Author: Estonian Biobank Research Team
Corporate Author: et al.

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