Disease areas:
  • cancer and other tissue growths
Last updated:
Author(s):
Pooja Middha, Linda Kachuri, Jovia L. Nierenberg, Rebecca E. Graff, Taylor B. Cavazos, Thomas J. Hoffmann, Jie Zhang, Stacey Alexeeff, Laurel Habel, Douglas A. Corley, Stephen Van Den Eeden, Lawrence H. Kushi, Elad Ziv, Lori C. Sakoda, John S. Witte
Publish date:
4 February 2025
Journal:
Human Genetics and Genomics Advances
PubMed ID:
39910817

Abstract

With advances in cancer screening and treatment, there is a growing population of cancer survivors who may develop subsequent primary cancers. While hereditary cancer syndromes account for only a portion of multiple cancer cases, we sought to explore the role of common genetic variation in susceptibility to multiple primary tumors. We conducted a cross-ancestry genome-wide association study (GWAS) and transcriptome-wide association study (TWAS) of 10,983 individuals with multiple primary cancers, 84,475 individuals with single cancer, and 420,944 cancer-free controls from two large-scale studies. Our GWAS identified six lead variants across five genomic regions that were significantly associated (p < 5 × 10-8) with the risk of developing multiple primary tumors (overall and invasive) relative to cancer-free controls (at 3q26, 8q24, 10q24, 11q13.3, and 17p13). We also found one variant significantly associated with multiple cancers when compared with single cancer cases (at 22q13.1). Multi-tissue TWAS detected associations with genes involved in telomere maintenance in two of these regions (ACTRT3 in 3q26 and SLK and STN1 in 10q24) and the development of multiple cancers. Additionally, the TWAS also identified several novel genes associated with multiple cancers, including two immune-related genes, IRF4 and TNFRSF6B. Telomere maintenance and immune dysregulation emerge as central, common pathways influencing susceptibility to multiple cancers. These findings underscore the importance of exploring shared mechanisms in carcinogenesis, offering insights for targeted prevention and intervention strategies.

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The goal of our proposed research is to characterize pleiotropic loci in order to gain new insight into common carcinogenic mechanisms, shared etiology of multiple…

Institution:
University of California, San Francisco, United States of America

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