The burden of endometriosis on quality of life in Danish women: an analysis of the Danish Blood Donor Study

  1. Lisette J. A. Kogelman
  2. Dorte Rytter
  3. Lone Hummelshoj
  4. Karina Ejgaard Hansen
  5. Ulrik Bak Kirk
  6. Juliane Lyng Beauchamp
  7. Jakob Thaning Bay
  8. Mie Topholm Bruun
  9. Nanna Brøns
  10. Christian Erikstrup
  11. Bitten Aagaard
  12. Bertram Dalskov Kjerulff
  13. Christina Mikkelsen
  14. Susan Mikkelsen
  15. Sisse Rye Ostrowski
  16. Ole Birger Pedersen
  17. Erik Sørensen
  18. Henrik Ullum
  19. DBDS Genomic Consortium
  20. Jakob Bay
  21. Andrea Barghetti
  22. Mette Skou Bendtsen
  23. Jens Kjærgaard Boldsen
  24. Søren Brunak
  25. Alfonso Buil Demur
  26. Johan Skov Bundgaard
  27. Lea Arregui Nordahl Christoffersen
  28. Maria Didriksen
  29. Khoa Manh Dinh
  30. Joseph Dowsett
  31. Josephine Gladov
  32. Daniel Gudbjartsson
  33. Thomas Folkmann Hansen
  34. Dorte Helenius Mikkelsen
  35. Lotte Hindhede
  36. Henrik Hjalgrim
  37. Jakob Hjorth von Stemann
  38. Bitten Aagaard Jensen
  39. Kathrine Kaspersen
  40. Bertram Dalskov Kjerulff
  41. Lisette J. A. Kogelman
  42. Mette Kongstad
  43. Line Hjorth Sjernholm Nielsen
  44. Janna Nissen
  45. Frederikke Byron Pedersen
  46. Liam James Elgaard Quinn
  47. Þórunn Rafnar
  48. Klaus Rostgaard
  49. Andrew Joseph Schork
  50. Michael Schwinn
  51. Hreinn Stefánsson
  52. Jacob Træholt
  53. Unnur Þorsteinsdóttir
  54. Thomas Werge
  55. Anne Karmisholt Grosen
  56. Christian Lodberg Hvas
  57. Valgerdur Steinthorsdottir
  58. Kari Stefansson
  59. Karina Banasik
  60. Palle Duun Rohde
  61. Henriette Svarre Nielsen
  62. Mette Nyegaard
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Abstract

Background

Endometriosis is a complex condition with a wide range of comorbidities. It is widely underdiagnosed, with a diagnostic delay of 4 to 10 years, potentially leading to worsened disease progression and a higher burden of comorbidities affecting quality of life. Understanding the link between endometriosis and its comorbidities is essential for improving early detection of the disease.

Methods

We analysed data from 953 women with a clinical diagnosis of endometriosis and 23,652 age-matched female controls enrolled in the Danish Blood Donor Study, using a case-control design. Participants completed one to four questionnaires covering a wide range of potential comorbidities; genetic data were available for a subset of participants. First, we compared the potential comorbidities between women with endometriosis and controls. Next, we investigated whether a polygenic score (PGS) for endometriosis was associated with those comorbidities. Lastly, we investigated whether women with a high genetic burden of endometriosis (highest PGS decile) experienced similar comorbidities to those diagnosed with endometriosis.

Results

Women with endometriosis experienced challenges in conception, gastrointestinal symptoms, and disturbed sleep patterns, compared to age-matched controls. The endometriosis PGS showed to be a predictor for endometriosis (OR per unit PGS = 1.43, 95% CI = 1.32–1.55). Gastrointestinal symptoms were also nominally associated with the endometriosis PGS, suggesting shared genetic pathways. Women without a diagnosis of endometriosis but with a high genetic burden of endometriosis did not suffer from the same wide range of comorbidities as women diagnosed with endometriosis.

Conclusions

Our findings highlight the complex genetic and clinical relationships between endometriosis and its comorbidities, emphasizing the need for future research investigating potential endometriosis subtypes.

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  1. Version published to 10.1186/s12916-025-04398-z
  2. Version published to 10.21203/rs.3.rs-6620337/v1 on Research Square