Scientific Reports (Jul 2024)

A comprehensive analysis of germline predisposition to early-onset ovarian cancer

  • Klara Horackova,
  • Petra Zemankova,
  • Petr Nehasil,
  • Michal Vocka,
  • Milena Hovhannisyan,
  • Katerina Matejkova,
  • Marketa Janatova,
  • Marta Cerna,
  • Petra Kleiblova,
  • Sandra Jelinkova,
  • Barbora Stastna,
  • Pavel Just,
  • Tatana Dolezalova,
  • Barbora Nemcova,
  • Marketa Urbanova,
  • Monika Koudova,
  • Jana Hazova,
  • Eva Machackova,
  • Lenka Foretova,
  • Viktor Stranecky,
  • Michal Zikan,
  • Zdenek Kleibl,
  • Jana Soukupova

DOI
https://doi.org/10.1038/s41598-024-66324-2
Journal volume & issue
Vol. 14, no. 1
pp. 1 – 12

Abstract

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Abstract The subset of ovarian cancer (OC) diagnosed ≤ 30yo represents a distinct subgroup exhibiting disparities from late-onset OC in many aspects, including indefinite germline cancer predisposition. We performed DNA/RNA-WES with HLA-typing, PRS assessment and survival analysis in 123 early-onset OC-patients compared to histology/stage-matched late-onset and unselected OC-patients, and population-matched controls. Only 6/123(4.9%) early-onset OC-patients carried a germline pathogenic variant (GPV) in high-penetrance OC-predisposition genes. Nevertheless, our comprehensive germline analysis of early-onset OC-patients revealed two divergent trajectories of potential germline susceptibility. Firstly, overrepresentation analysis highlighted a connection to breast cancer (BC) that was supported by the CHEK2 GPV enrichment in early-onset OC(p = 1.2 × 10–4), and the presumably BC-specific PRS313, which successfully stratified early-onset OC-patients from controls(p = 0.03). The second avenue pointed towards the impaired immune response, indicated by LY75-CD302 GPV(p = 8.3 × 10–4) and diminished HLA diversity compared with controls(p = 3 × 10–7). Furthermore, we found a significantly higher overall GPV burden in early-onset OC-patients compared to controls(p = 3.8 × 10–4). The genetic predisposition to early-onset OC appears to be a heterogeneous and complex process that goes beyond the traditional Mendelian monogenic understanding of hereditary cancer predisposition, with a significant role of the immune system. We speculate that rather a cumulative overall GPV burden than specific GPV may potentially increase OC risk, concomitantly with reduced HLA diversity.

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