Immune, Developmental, and Synaptic Pathways Define Bipolar Disorder Clinical Heterogeneity

  1. Tracey van der Veen
  2. Markos Tesfaye
  3. Jessica Mei Kay Yang
  4. Toni Boltz
  5. Friederike S. David
  6. Shane Crinion
  7. Maria Koromina
  8. Till F. M. Andlauer
  9. Tim B. Bigdeli
  10. Brandon J. Coombes
  11. Tiffany A. Greenwood
  12. Georgia Panagiotaropoulou
  13. Nadine Parker
  14. Heejong Sung
  15. Nicholas Bass
  16. Jonathan R. I. Coleman
  17. José Guzman-Parra
  18. Janos L. Kalman
  19. Caroline C. McGrouther
  20. Brittany L. Mitchell
  21. Aaditya V. Rangan
  22. Katie Scott
  23. Alexey Shadrin
  24. Daniel J. Smith
  25. Annabel Vreeker
  26. Kristina Adorjan
  27. Diego Albani
  28. Silvia Alemany
  29. Ney Alliey-Rodriguez
  30. Anastasia Antoniou
  31. Michael Bauer
  32. Eva C. Beins
  33. Marco P. Boks
  34. Rosa Bosch
  35. Ben M. Brumpton
  36. Nathalie Brunkhorst-Kanaan
  37. Monika Budde
  38. William Byerley
  39. Judit Cabana-Domínguez
  40. Murray J. Cairns
  41. Bernardo Carpiniello
  42. Miquel Casas
  43. Pablo Cervantes
  44. Chris Chatzinakos
  45. Toni-Kim Clarke
  46. Isabelle Claus
  47. Cristiana Cruceanu
  48. Alfredo Cuellar-Barboza
  49. Piotr M. Czerski
  50. Konstantinos Dafnas
  51. Anders M. Dale
  52. Nina Dalkner
  53. J. Raymond DePaulo
  54. Franziska Degenhardt
  55. Srdjan Djurovic
  56. Valentina Escott-Price
  57. Ayman H. Fanous
  58. Frederike T. Fellendorf
  59. I. Nicol Ferrier
  60. Liz Forty
  61. Josef Frank
  62. Oleksandr Frei
  63. Nelson B. Freimer
  64. Julie Garnham
  65. Ian R. Gizer
  66. Scott D. Gordon
  67. Katherine Gordon-Smith
  68. Tim Hahn
  69. L. Marian
  70. Arvid Harder
  71. Martin Hautzinger
  72. Urs Heilbronner
  73. Dennis Hellgren
  74. Stefan Herms
  75. Ian B. Hickie
  76. Per Hoffmann
  77. Peter A. Holmans
  78. Stéphane Jamain
  79. Lina Jonsson
  80. James L. Kennedy
  81. Sarah Kittel-Schneider
  82. James A. Knowles
  83. Elise Koch
  84. Manolis Kogevinas
  85. Thorsten M. Kranz
  86. Steven A. Kushner
  87. Catharina Lavebratt
  88. Jacob Lawrence
  89. Markus Leber
  90. Penelope A. Lind
  91. Susanne Lucae
  92. Martin Lundberg
  93. Donald J. MacIntyre
  94. Wolfgang Maier
  95. Adam X. Maihofer
  96. Dolores Malaspina
  97. Mirko Manchia
  98. Eirini Maratou
  99. Lina Martinsson
  100. Melvin G. McInnis
  101. James D. McKay
  102. Helena Medeiros
  103. Andreas Meyer-Lindenberg
  104. Vincent Millischer
  105. Derek W. Morris
  106. Paraskevi Moutsatsou
  107. Thomas W. Mühleisen
  108. Claire O. ’Donovan
  109. Catherine M. Olsen
  110. Sergi Papiol
  111. Antonio F. Pardiñas
  112. Amy Perry
  113. Andrea Pfennig
  114. Claudia Pisanu
  115. James B. Potash
  116. Digby Quested
  117. Mark H. Rapaport
  118. Eline J. Regeer
  119. John P. Rice
  120. Margarita Rivera
  121. Eva C. Schulte
  122. Fanny Senner
  123. Paul D. Shilling
  124. Lisa Sindermann
  125. Lea Sirignano
  126. Dan Siskind
  127. Claire Slaney
  128. Olav B. Smeland
  129. Janet L. Sobell
  130. Maria Soler Artigas
  131. Dan J. Stein
  132. Frederike Stein
  133. Beata Swiatkowska
  134. Jackson G. Thorp
  135. Claudio Toma
  136. Leonardo Tondo
  137. Paul A. Tooney
  138. Marquis P. Vawter
  139. Helmut Vedder
  140. James T. R. Walters
  141. Stephanie H. Witt
  142. Allan H. Young
  143. Peter P. Zandi
  144. Lea Zillich
  145. Estonian Biobank research team
  146. Genomic Psychiatry Cohort (GPC) Investigators
  147. HUNT All-In Psychiatry
  148. Rolf Adolfsson
  149. Lars Alfredsson
  150. Lena Backlund
  151. Bernhard T. Baune
  152. Frank Bellivier
  153. Susanne Bengesser
  154. Wade H. Berrettini
  155. Joanna M. Biernacka
  156. Douglas Blackwood
  157. Michael Boehnke
  158. Gerome Breen
  159. Vaughan J. Carr
  160. Stanley Catts
  161. Sven Cichon
  162. Aiden Corvin
  163. Nicholas Craddock
  164. Udo Dannlowski
  165. Dimitris Dikeos
  166. Tõnu Esko
  167. Bruno Etain
  168. Panagiotis Ferentinos
  169. Mark Frye
  170. Janice M. Fullerton
  171. Micha Gawlik
  172. Elliot S. Gershon
  173. Fernando S. Goes
  174. Melissa J. Green
  175. Joanna Hauser
  176. Frans A. Henskens
  177. Jens Hjerling-Leffler
  178. Ian Jones
  179. Lisa A. Jones
  180. René S. Kahn
  181. John R. Kelsoe
  182. Tilo Kircher
  183. George Kirov
  184. Nene Kobayashi
  185. Mikael Landén
  186. Marion Leboyer
  187. Melanie Lenger
  188. Qingqin S. Li
  189. Jolanta Lissowska
  190. Carmel Loughland
  191. Jurjen J. Luykx
  192. Nicholas G. Martin
  193. Carol A. Mathews
  194. Fermin Mayoral
  195. Susan L. McElroy
  196. Andrew M. McIntosh
  197. Sarah E. Medland
  198. Ingrid Melle
  199. Philip B. Mitchell
  200. Gunnar Morken
  201. Richard M. Myers
  202. Chiara Möser
  203. Bertram Müller-Myhsok
  204. Benjamin M. Neale
  205. Caroline M. Nievergelt
  206. John I. Nurnberger
  207. Markus M. Nöthen
  208. Michael C. O’Donovan
  209. Ketil J. Oedegaard
  210. Tomas Olsson
  211. Michael J. Owen
  212. Sara A. Paciga
  213. Christos Pantelis
  214. Carlos N. Pato
  215. Michele T. Pato
  216. George P. Patrinos
  217. Joanna M. Pawlak
  218. Roy Perlis
  219. Josep Antoni Ramos-Quiroga
  220. Andreas Reif
  221. Eva Z. Reininghaus
  222. Marta Ribasés
  223. Marcella Rietschel
  224. Stephan Ripke
  225. Guy A. Rouleau
  226. Ulrich Schall
  227. Martin Schalling
  228. Peter R. Schofield
  229. Thomas G. Schulze
  230. Laura J. Scott
  231. Rodney J. Scott
  232. Alessandro Serretti
  233. Jordan W. Smoller
  234. Alessio Squassina
  235. Eli A. Stahl
  236. Eystein Stordal
  237. Fabian Streit
  238. Patrick F. Sullivan
  239. Gustavo Turecki
  240. Arne E. Vaaler
  241. Eduard Vieta
  242. John B. Vincent
  243. Irwin D. Waldman
  244. Cynthia S. Weickert
  245. Thomas W. Weickert
  246. David C. Whiteman
  247. Martin Alda
  248. Roel A. Ophoff
  249. Kevin S. O’Connell
  250. Niamh Mullins
  251. Andreas J. Forstner
  252. Maria Grigoroiu-Serbanescu
  253. Howard J. Edenberg
  254. Francis J. McMahon
  255. Ole A. Andreassen
  256. Arianna Di Florio
  257. Andrew McQuillin
  258. the Bipolar Disorder Working Group of the Psychiatric Genomics Consortium
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Abstract

Importance

The clinical heterogeneity of bipolar disorder (BD) is a major obstacle to improving diagnosis, predicting patient outcomes, and developing personalized treatments. A genetic approach is needed to deconstruct the disorder and uncover its fundamental biology. Previous genetic studies focusing on broad diagnostic categories have been limited in their ability to parse this complexity.

Objective

To test the hypothesis that clinically distinct subphenotypes of BD are associated with different underlying common variant genetic architectures.

Design, Setting, and Participants

This multicenter study included a primary genome-wide association study (GWAS) of up to 23,819 bipolar disorder (BD) cases and 163,839 controls. These results were integrated via multi-trait analysis of GWAS (MTAG) with external summary statistics for BD (59,287 cases; 781,022 controls) and schizophrenia (SCZ; 53,386 cases; 77,258 controls). Sample overlap was statistically accounted for.

Main Outcomes and Measures

The primary outcomes were the genetic dimensions underlying BD heterogeneity, differentiated by single nucleotide polymorphism (SNP)-heritability (h 2 SNP ), genetic correlations, genomic loci ( P ≤5×10 -8 ), and functional, cell-type, and gene-expression pathway analyses.

Results

We identified four genetically-informed dimensions of BD: Severe Illness, Core Mania, Externalizing/Impulsive Comorbidity, and Internalizing/Affective Comorbidity. The analyses yielded up to 181 subphenotype-associated loci, 53 of which are novel. The Severe Illness Dimension was characterized by a unique neuro-immune signature (a protective association with HLA-DMB , P =2.50×10 -273 ) evident only when leveraging SCZ genetic data. The Internalizing/Affective dimension was associated with neurodevelopmental genes (e.g., DCC ). Notably, the rapid-cycling subphenotype showed a unique signature of strong negative selection, a finding not observed in other subphenotypes.

Conclusions and Relevance

The clinical heterogeneity of bipolar disorder appears to be defined by a complex and multi-layered genetic architecture. The presented findings provide an empirical framework that may advance psychiatric nosology beyond its current diagnostic boundaries. These results may also inform future research to identify targets for personalized interventions. The delineation of these genetically-informed dimensions offers specific, biologically-grounded hypotheses for subsequent therapeutic discovery. Establishing such a framework is an essential step toward refining diagnostic criteria and developing more effective, personalized treatments. This work lays the foundation for a transition from a uniform treatment model to the paradigm of precision psychiatry.

Key Points

Question

What are the distinct genetic architectures underlying the clinical heterogeneity of bipolar disorder?

Findings

In this genetic study of 23,819 bipolar disorder (BD) cases and 163,839 controls, clinical heterogeneity mapped onto four genetically-informed dimensions. A severe illness dimension was defined by a neuro-immune signature ( HLA-DMB ) shared with schizophrenia. An affective comorbidity dimension was distinguished by neurodevelopmental pathways involving axonal guidance ( DCC ). Notably, the rapid-cycling phenotype showed evidence of purifying selection, suggesting influence by rare, highly penetrant alleles.

Meaning

These findings provide a data-driven biological framework for bipolar disorder, guiding future research toward patient stratification and targeted therapeutics.

Article activity feed

  1. Version published to 10.1101/2025.06.23.25330155v5 on medRxiv
  2. Version published to 10.1101/2025.06.23.25330155v3 on medRxiv
  3. Version published to 10.1101/2025.06.23.25330155v4 on medRxiv
  4. Version published to 10.1101/2025.06.23.25330155v1 on medRxiv
  5. Version published to 10.1101/2025.06.23.25330155v2 on medRxiv