Neuroanatomical dimensions in recent-onset depression: clinical profiles, inflammatory markers, and proteomic ageing

  1. Paris Alexandros Lalousis
  2. Louise Moles
  3. Mathilde Antoniades
  4. Wenyi Xiao
  5. Amalie C. M. Couch
  6. Guray Erus
  7. Pranav Thokachichu
  8. Dhivya Srinivasan
  9. Yong Fan
  10. Rachel D. Woodham
  11. Danilo Arnone
  12. Stephen R. Arnott
  13. Taolin Chen
  14. Ki Sueng Choi
  15. Cherise Chin Fatt
  16. Benicio N. Frey
  17. Vibe G. Frokjaer
  18. Melanie Ganz
  19. Beata R. Godlewska
  20. Stefanie Hassel
  21. Keith Ho
  22. Andrew M. McIntosh
  23. Kun Qin
  24. Susan Rotzinger
  25. Matthew D. Sacchet
  26. Jonathan Savitz
  27. Haochang Shou
  28. Aleks Stolicyn
  29. Irina Strigo
  30. Stephen C. Strother
  31. Duygu Tosun
  32. Teresa A. Victor
  33. Dongtao Wei
  34. Toby Wise
  35. Roland Zahn
  36. Ian M. Anderson
  37. J.F. William Deakin
  38. W. Edward Craighead
  39. Boadie W. Dunlop
  40. Rebecca Elliott
  41. Qiyong Gong
  42. Ian H. Gotlib
  43. Catherine J. Harmer
  44. Sidney H. Kennedy
  45. Gitte M. Knudsen
  46. Helen S. Mayberg
  47. Martin P. Paulus
  48. Jiang Qiu
  49. Madhukar H. Trivedi
  50. Heather C. Whalley
  51. Chao-Gan Yan
  52. Allan H. Young
  53. Grace Jacobs
  54. Nora Penzel
  55. Raimo K.R. Salokangas
  56. Eva Meisenzahl
  57. Jarmo Hietala
  58. Alessandro Bertolino
  59. Rebekka Lencer
  60. Stephen Wood
  61. Christos Pantelis
  62. Georg Romer
  63. Dominic Dwyer
  64. Joseph Kambeitz
  65. Lana Kambeitz-Ilankovic
  66. Frauke Schultze-Lutter
  67. Stephan Ruhrmann
  68. Nicholas M. Barnes
  69. Rachel Upthegrove
  70. Nikolaos Koutsouleris
  71. Christos Davatzikos
  72. Cynthia H.Y. Fu
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Abstract

Background

Major depressive disorder (MDD) is clinically heterogeneous, hindering identification of reproducible biomarkers. Using a semi-supervised machine learning approach, HYDRA, we previously identified two neuroanatomical dimensions from structural MRI in medication-free MDD from COORDINATE-MDD consortium. These dimensions (D1, D2) showed differential responses to selective serotonin reuptake inhibitor (SSRI) antidepressants and placebo. External replication in UK Biobank linked D2, characterized by widespread subtle neuroanatomical reductions, to an immuno-metabolic profile. Here, we examined whether these dimensions are detectable early in the course of illness.

Methods

We applied the pre-trained model to structural MRI data from the multisite PRONIA cohort, comprising individuals with recent-onset depression (ROD; n = 377; mean age 25.8 years, SD 6.0; 51.3% female) and healthy controls (n = 267; mean age 25.5 years, SD 6.4; 61.0% female). Participants were assigned to clusters (C1, C2) corresponding to the previously identified dimensions (D1, D2). Clusters were compared on clinical symptom profiles, peripheral inflammatory markers, and in a subset (n = 107), proteomic ageing indices.

Results

Two neuroanatomical clusters were identified in PRONIA. C1 (n = 265) showed higher negative symptom severity and elevated interleukin-2 levels. C2 (n = 140) was associated with higher residual proteomic age. Overall depressive symptom severity did not differ significantly between clusters.

Conclusions

Neuroanatomical dimensions of MDD are reproducible and detectable at illness onset. Associations with negative symptom severity, inflammatory signalling, and proteomic ageing suggest these dimensions capture biologically meaningful heterogeneity early in depression. These findings support a biologically informed framework for stratified treatment approaches in MDD.

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  1. Version published to 10.64898/2026.06.01.26354320 on medRxiv