Author
Listed:
- Jeewoo Kim
(Vanderbilt University Medical Center
Vanderbilt University School of Medicine
Vanderbilt University Medical Center
Vanderbilt University)
- Ariel Williams
(National Institute of Health)
- Hannah Noh
(Tufts University Medical School Graduate Programs
Vanderbilt University)
- Elizabeth A. Jasper
(Vanderbilt University Medical Center
Vanderbilt University Medical Center)
- Sarah H. Jones
(Vanderbilt University Medical Center)
- James A. Jaworski
(Vanderbilt University
Vanderbilt University Medical Center)
- Megan M. Shuey
(Vanderbilt University Medical Center)
- Edward A. Ruiz-Narváez
(Department of Nutritional Sciences University of Michigan School of Public Health)
- Lauren A. Wise
(Boston University School of Public Health)
- Julie R. Palmer
(Slone Epidemiology Center at Boston University)
- John Connolly
(Children’s Hospital of Philadelphia)
- Jacob M. Keaton
(National Institute of Health
Vanderbilt University Medical Center)
- Joshua C. Denny
(National Institute of Health
National Institutes of Health)
- Atlas Khan
(Columbia University)
- Mohammad A. Abbass
(Northwestern University Feinberg School of Medicine)
- Laura J. Rasmussen-Torvik
(Northwestern University Feinberg School of Medicine)
- Leah C. Kottyan
(University of Cincinnati)
- Purnima Madhivanan
(University of Arizona Comprehensive Cancer Center
University of Arizona
Public Health Research Institute of India
University of Arizona)
- Karl Krupp
(University of Arizona Comprehensive Cancer Center
Public Health Research Institute of India
Mel & Enid Zuckerman College of Public Health)
- Wei-Qi Wei
(Vanderbilt University Medical Center)
- Todd L. Edwards
(Vanderbilt University Medical Center)
- Digna R. Velez Edwards
(Vanderbilt University Medical Center
Vanderbilt University Medical Center
Vanderbilt University Medical Center
Vanderbilt University Medical Center)
- Jacklyn N. Hellwege
(Vanderbilt University Medical Center
Vanderbilt University
Vanderbilt University Medical Center)
Abstract
Uterine leiomyomata or fibroids are highly heritable, common, and benign tumors of the uterus with poorly understood etiology. Previous GWAS have reported 72 associated genes but included limited numbers of non-European individuals. Here, we identify 11 novel genes associated with fibroids across multi-ancestry and ancestry-stratified GWAS analyses. We replicate a known fibroid GWAS gene in African ancestry individuals and estimate the SNP-based heritability of fibroids in African ancestry populations as 15.9%. Using genetically predicted gene expression and colocalization analyses, we identify 46 novel genes associated with fibroids. These genes are significantly enriched in cancer, cell death and survival, reproductive system disease, and cellular growth and proliferation networks. We also find that increased predicted expression of HEATR3 in uterine tissue is associated with fibroids across ancestry strata. Overall, we report genetic variants associated with fibroids coupled with functional and gene pathway enrichment analyses.
Suggested Citation
Jeewoo Kim & Ariel Williams & Hannah Noh & Elizabeth A. Jasper & Sarah H. Jones & James A. Jaworski & Megan M. Shuey & Edward A. Ruiz-Narváez & Lauren A. Wise & Julie R. Palmer & John Connolly & Jacob, 2025.
"Genome-wide meta-analysis identifies novel risk loci for uterine fibroids within and across multiple ancestry groups,"
Nature Communications, Nature, vol. 16(1), pages 1-13, December.
Handle:
RePEc:nat:natcom:v:16:y:2025:i:1:d:10.1038_s41467-025-57483-5
DOI: 10.1038/s41467-025-57483-5
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