Profiles of Genetic Risks for Psychotic Disorders

Kendler, Kenneth S.; Ohlsson, Henrik; Sundquist, Jan; Sundquist, Kristina

Profiles of Genetic Risks for Psychotic Disorders

Mark

Kendler, Kenneth S. ; Ohlsson, Henrik ^LU ; Sundquist, Jan ^LU and Sundquist, Kristina ^LU (2025) In JAMA Psychiatry 82(9). p.926-933

Abstract: Importance: The etiologic interrelationship of 4 rare/controversial psychotic disorders (delusional disorder [DD], acute psychoses [AP], psychosis not otherwise specified [PNOS], and schizoaffective disorder [SAD]) is poorly understood. Objective: To assess levels of the family genetic risk score (FGRS) for schizophrenia (SZ), bipolar disorder (BD), and major depression (MD) in individuals with DD, AP, PNOS, and SAD, thereby clarifying their genetic relationships. Design, Setting, and Participants: This cohort study included all individuals born in Sweden between 1950 and 2000 to Swedish-born parents followed up until 2018 with diagnoses of MD, BD, SZ, SAD, AP, PNOS, and DD, based on diagnosis codes from national registries. Exposures:... (More); Importance: The etiologic interrelationship of 4 rare/controversial psychotic disorders (delusional disorder [DD], acute psychoses [AP], psychosis not otherwise specified [PNOS], and schizoaffective disorder [SAD]) is poorly understood. Objective: To assess levels of the family genetic risk score (FGRS) for schizophrenia (SZ), bipolar disorder (BD), and major depression (MD) in individuals with DD, AP, PNOS, and SAD, thereby clarifying their genetic relationships. Design, Setting, and Participants: This cohort study included all individuals born in Sweden between 1950 and 2000 to Swedish-born parents followed up until 2018 with diagnoses of MD, BD, SZ, SAD, AP, PNOS, and DD, based on diagnosis codes from national registries. Exposures: FGRS for SZ, BD, and MD calculated from first- through fifth-degree relatives, controlling for cohabitation. Main Outcomes and Measures: Diagnoses of DD, AP, PNOS, and SAD. Results: In the cohort, 667 012 individuals had MD (420 142 females [63%] and 246 870 males [37.0%]), 58 385 had BD (36 344 females [62%] and 22 041 males [38%]), 17 465 had SZ (6330 females [36%] and 11 135 males [64%]), 7597 had SAD (4125 females [54%] and 3472 males [46%]), 16 315 had AP (7907 females [49%] and 8408 males [51%]), 27 127 had PNOS (12 277 females [45%] and 14 850 males [55%]), and 11 560 had DD (5060 females [44%] and 6500 males [56%]). On "genetic maps" of SZ FGRS, BD FGRS, and MD FGRS, DD stood alone with approximately half the genetic risk for SZ compared with SZ cases and similar levels of BD and MD risk. SAD was also distinct as the only disorder with quite high genetic risks for both SZ and BD and was clearly separable from psychotic BD. AP and PNOS had similar genetic profiles with levels of SZ FGRS similar to DD but higher levels of genetic risk for BD and MD. Subdividing psychoses by outcome produced minimal effects on the DD genetic profile, moderate effects on AP and PNOS, and large effects on SAD, with good social outcomes associated with decreased SZ FGRS and increased BD FGRS. Conclusions and Relevance: In a Swedish population, none of the 4 disorders appeared, from a genetic perspective, to be subtypes of SZ, BD, or MD. Further genetics research on the syndromes of DD, AP, PNOS, and SAD have much to teach about the relationship between dimensions of genetic risks and the clinical presentation and course of psychotic illness.
(Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/072dec75-bf5e-49f6-98c8-2acabec100a3

author

Kendler, Kenneth S. ; Ohlsson, Henrik ^LU ; Sundquist, Jan ^LU and Sundquist, Kristina ^LU

organization

publishing date

2025-09

type

Contribution to journal

publication status

published

subject

Psychiatry

in

JAMA Psychiatry

volume

82

issue

9

pages

8 pages

publisher

American Medical Association

external identifiers

pmid:40632548
scopus:105015164581

ISSN

2168-622X

DOI

10.1001/jamapsychiatry.2025.1289

language

English

LU publication?

yes

id

072dec75-bf5e-49f6-98c8-2acabec100a3

date added to LUP

2025-10-16 11:05:44

date last changed

2025-12-11 15:58:52

@article{072dec75-bf5e-49f6-98c8-2acabec100a3,
  abstract     = {{<p>Importance: The etiologic interrelationship of 4 rare/controversial psychotic disorders (delusional disorder [DD], acute psychoses [AP], psychosis not otherwise specified [PNOS], and schizoaffective disorder [SAD]) is poorly understood. Objective: To assess levels of the family genetic risk score (FGRS) for schizophrenia (SZ), bipolar disorder (BD), and major depression (MD) in individuals with DD, AP, PNOS, and SAD, thereby clarifying their genetic relationships. Design, Setting, and Participants: This cohort study included all individuals born in Sweden between 1950 and 2000 to Swedish-born parents followed up until 2018 with diagnoses of MD, BD, SZ, SAD, AP, PNOS, and DD, based on diagnosis codes from national registries. Exposures: FGRS for SZ, BD, and MD calculated from first- through fifth-degree relatives, controlling for cohabitation. Main Outcomes and Measures: Diagnoses of DD, AP, PNOS, and SAD. Results: In the cohort, 667 012 individuals had MD (420 142 females [63%] and 246 870 males [37.0%]), 58 385 had BD (36 344 females [62%] and 22 041 males [38%]), 17 465 had SZ (6330 females [36%] and 11 135 males [64%]), 7597 had SAD (4125 females [54%] and 3472 males [46%]), 16 315 had AP (7907 females [49%] and 8408 males [51%]), 27 127 had PNOS (12 277 females [45%] and 14 850 males [55%]), and 11 560 had DD (5060 females [44%] and 6500 males [56%]). On "genetic maps" of SZ FGRS, BD FGRS, and MD FGRS, DD stood alone with approximately half the genetic risk for SZ compared with SZ cases and similar levels of BD and MD risk. SAD was also distinct as the only disorder with quite high genetic risks for both SZ and BD and was clearly separable from psychotic BD. AP and PNOS had similar genetic profiles with levels of SZ FGRS similar to DD but higher levels of genetic risk for BD and MD. Subdividing psychoses by outcome produced minimal effects on the DD genetic profile, moderate effects on AP and PNOS, and large effects on SAD, with good social outcomes associated with decreased SZ FGRS and increased BD FGRS. Conclusions and Relevance: In a Swedish population, none of the 4 disorders appeared, from a genetic perspective, to be subtypes of SZ, BD, or MD. Further genetics research on the syndromes of DD, AP, PNOS, and SAD have much to teach about the relationship between dimensions of genetic risks and the clinical presentation and course of psychotic illness.</p>}},
  author       = {{Kendler, Kenneth S. and Ohlsson, Henrik and Sundquist, Jan and Sundquist, Kristina}},
  issn         = {{2168-622X}},
  language     = {{eng}},
  number       = {{9}},
  pages        = {{926--933}},
  publisher    = {{American Medical Association}},
  series       = {{JAMA Psychiatry}},
  title        = {{Profiles of Genetic Risks for Psychotic Disorders}},
  url          = {{http://dx.doi.org/10.1001/jamapsychiatry.2025.1289}},
  doi          = {{10.1001/jamapsychiatry.2025.1289}},
  volume       = {{82}},
  year         = {{2025}},
}

Lund University Publications

LUND UNIVERSITY LIBRARIES

Profiles of Genetic Risks for Psychotic Disorders