Twin study refining psychotic symptom dimensions as phenotypes for genetic research

Cardno, Alastair G.; Rijsdijk, Frühling; Murray, Robin M.; McGuffin, Peter

doi:10.1002/ajmg.b.30756

Cited by 11 publications

(22 citation statements)

References 49 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…However, the point estimate of 0.34 was similar to that found in affected sib-pairs using the same symptom dimension definition (Spearman r ¼ 0.25) [Cardno et al, 1999a] and closer still using the same statistical approach (PCC ¼ 0.30, CI 0.07-0.51: calculated by AG Cardno), and also similar using other rating scales, analytical approaches and samples (0.19-0.32) [Burke et al, 1996;Loftus et al, 1998;Cardno et al, 1999a;Rietkerk et al, 2008]. The sib-pairs had a narrower range of phenotypes-schizophrenia and schizoaffective disorder-but in this twin sample correlations for the disorganized dimension are similar in MZ pairs concordant for psychotic disorder, and where one or both twins has schizophrenia [Cardno et al, 2008] (there are too few DZ twin pairs concordant for schizophrenia for this comparison). Caveats are the nonsystematic ascertainment of the sib-pair samples and the theoretical possibility of differences in familial aggregation between DZ twins and siblings.…”

Section: Symptom Dimensionsmentioning

confidence: 53%

“…Initial analysis of the Maudsley twin series [Cardno et al, 2001[Cardno et al, , 2008 showed similar correlations for positive dimension definitions in affected monozygotic (MZ) twin pairs (up Neuropsychiatric Genetics to 0.35), but trends towards higher correlations for some definitions of the negative and disorganized dimensions (up to 0.77). This suggests that there may be notable genetic influences on at least some dimensions, but these analyses did not include formal heritability estimates (see Supplementary Material).…”

Section: Introductionmentioning

confidence: 67%

“…Symptom dimensions were defined as ordinal symptom scores, based on the most characteristic symptoms found in previous factor analyses of global psychotic symptoms [Liddle, 1987;Andreasen et al, 1995;Peralta et al, 1997;Ratakonda et al, 1998], as previously employed in affected sib-pair analysis [Cardno et al, 1999a] and initial analysis of this twin sample [Cardno et al, 2001[Cardno et al, , 2008. All symptoms were coded as present or absent and we did not include mood symptoms or illness history variables.…”

Section: Participant Assessmentsmentioning

confidence: 99%

“…The positive dimension comprised (a) any delusions, and (b) any hallucinations [Cardno et al, 2008], and was scored as 0 if neither symptom was present, 1 if one was present, and 2 if both were present. The negative dimension comprised negative formal thought disorder and restricted affect.…”

Section: Participant Assessmentsmentioning

confidence: 99%

“…Analysis needs to take into account the fact that symptom dimensions are usually only measured in individuals with a psychotic disorder, so relatives without psychosis have unknown symptom dimension scores. In this case, genetic influences on a symptom dimension may be viewed as reflecting the level of genetic liability to psychosis and/or being due to modifying factors independent of psychosis liability [Cardno et al, 2001[Cardno et al, , 2008. These two types of influence are expected to result in different patterns of familial aggregation, and analysis needs to take both potential influences into account.…”

Section: Introductionmentioning

confidence: 99%

See 4 more Smart Citations

Heritability estimates for psychotic symptom dimensions in twins with psychotic disorders

Rijsdijk

Gottesman

McGuffin

et al. 2010

American J of Med Genetics Pt B

Self Cite

View full text Add to dashboard Cite

Factor analysis of psychotic symptoms frequently results in positive, negative, and disorganized dimensions, but heritability estimates have not yet been reported. Symptom dimensions are usually only measured in individuals with psychotic disorders. Here, it is valuable to assess influences acting via liability to psychosis and independent modifying effects. We estimated heritability for psychotic symptom dimensions, taking account of these issues. Two-hundred-and-twenty-four probandwise twin pairs (106 monozygotic, 118 same-sex dizygotic), where probands had psychoses, were ascertained from the Maudsley Twin Register in London (1948-1993). Lifetime history of DSM-III-R psychotic disorder and psychotic symptom dimensions was assessed from clinical records and research interviews and rated using the Operational Criteria Checklist. Estimates of heritability and environmental components of variance in liability were made with structural equation modeling using a causal-contingent common pathway model adapted for ascertainment from a clinical register. Significant heritability was found for DSM-III-R psychotic disorder (h² = 90%, 95%CI 68-94%) and the disorganized symptom dimension (h² = 84%, 95%CI 18-93%). The heritability for the disorganized dimension remained significant when influences acting through liability to psychosis were set to zero, suggesting that some influences on disorganization are modifying factors independent of psychosis liability. However, the relative extent of modifying factors versus influences acting through psychosis liability could not be clearly determined. To our knowledge, this study provides the first formal evidence of substantive heritability for the disorganized symptom dimension, and suggests that genetic loci influencing disorganization in individuals with psychoses are in some cases different from loci that influence risk of psychotic disorders themselves.

show abstract

Section: Symptom Dimensionsmentioning

confidence: 53%

Section: Introductionmentioning

confidence: 67%

Section: Participant Assessmentsmentioning

confidence: 99%

Section: Participant Assessmentsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Heritability estimates for psychotic symptom dimensions in twins with psychotic disorders

Rijsdijk

Gottesman

McGuffin

et al. 2010

American J of Med Genetics Pt B

Self Cite

View full text Add to dashboard Cite

show abstract

Consistent Etiology of Severe, Frequent Psychotic Experiences and Milder, Less Frequent Manifestations

et al. 2014

Self Cite

View full text Add to dashboard Cite

Context The onset of psychosis is usually preceded by psychotic experiences, but little is known about their causes. The present study investigated the degree of genetic and environmental influences on specific psychotic experiences, assessed dimensionally, in adolescence in the community and in individuals with many, frequent experiences (defined using quantitative cut-offs). The degree of overlap in etiological influences between specific psychotic experiences was also investigated Objective Investigate degree of genetic and environmental influences on specific psychotic experiences, assessed dimensionally, in adolescence in the community and in individuals having many, frequent experiences (defined using quantitative cut-offs). Test degree of overlap in etiological influences between specific psychotic experiences. Design Classic twin design. Structural equation model-fitting. Univariate and bivariate twin models, liability threshold models, DeFries-Fulker extremes analysis and the Cherny Method. Setting Representative community sample of twins from England and Wales. Participants 5059 adolescent twin pairs (Mean age: 16.31 yrs, SD: 0.68 yrs). Main outcome measure Psychotic experiences assessed as quantitative traits (self-rated paranoia, hallucinations, cognitive disorganization, grandiosity, anhedonia; parent-rated negative symptoms). Results Genetic influences were apparent for all psychotic experiences (15-59%) with modest shared environment for hallucinations and negative symptoms (17-24%) and significant nonshared environment (49-64% for the self-rated scales, 17% for Parent-rated Negative Symptoms). Three different empirical approaches converged to suggest that the etiology in extreme groups (most extreme-scoring 5%, 10% and 15%) did not differ significantly from that of the whole distribution. There was no linear change in the heritability across the distribution of psychotic experiences, with the exception of a modest increase in heritability for increasing severity of parent-rated negative symptoms. Of the psychotic experiences that showed covariation, this appeared to be due to shared genetic influences (bivariate heritabilities = .54-.71). Conclusions and Relevance These findings are consistent with the concept of a psychosis continuum, suggesting that the same genetic and environmental factors influence both extreme, frequent psychotic experiences and milder, less frequent manifestations in adolescents. Individual psychotic experiences in adolescence, assessed quantitatively, have lower heritability estimates and higher estimates of nonshared environment than those for the liability to schizophrenia. Heritability varies by type of psychotic experience, being highest for paranoia and parent-rated negative symptoms, and lowest for hallucinations.

show abstract

The Genetics of Schizophrenia

Walters

O'Donovan

2011

Schizophrenia

View full text Add to dashboard Cite

Schizophrenia is a common psychiatric disorder with a strong genetic component. Recent studies applying new genomic technology to large samples have yielded substantial advances in identifying specific, associated DNA variants as well as clarifying the underlying genetic architecture of the disorder. The genetic liability of schizophrenia is now established as polygenic, with risk alleles in many genes existing across the full allelic frequency spectrum. It has also become apparent that schizophrenia shares risk alleles with other neuropsychiatric phenotypes, such as bipolar disorder, major depressive disorder, autism spectrum disorder, intellectual disability and attention-deficit hyperactivity disorder. These risk variants aggregate in several sets of functionally related genes, thereby providing novel insights into disease pathogenesis and opportunities for research into discovering new treatments.

show abstract

Twin study refining psychotic symptom dimensions as phenotypes for genetic research

Cited by 11 publications

References 49 publications

Heritability estimates for psychotic symptom dimensions in twins with psychotic disorders

Heritability estimates for psychotic symptom dimensions in twins with psychotic disorders

Consistent Etiology of Severe, Frequent Psychotic Experiences and Milder, Less Frequent Manifestations

The Genetics of Schizophrenia

Contact Info

Product

Resources

About