Skip to main content
Full access
New Research
Published Online: 1 September 2010

Early Expression of Negative/Disorganized Symptoms Predicting Psychotic Experiences and Subsequent Clinical Psychosis: A 10-Year Study

This article has been corrected.
VIEW CORRECTION

Abstract

Objective:

The cognitive and motivational impairments observed in psychotic disorders may reflect early developmental alterations that, when combined with later environmental exposures, may drive the onset of positive psychotic symptoms. The epidemiological predictions of this model were tested.

Method:

A longitudinal prospective cohort study (the Early Developmental Stages of Psychopathology Study) was conducted with a representative general population sample of adolescents and young adults from Munich (N=3,021), who were 14–24 years of age at baseline. Sociodemographic factors, environmental exposures, and measures of psychopathology and associated clinical relevance were assessed across three waves, covering a period of up to 10 years, by clinical psychologists using the Composite International Diagnostic Interview.

Results:

Both negative/disorganized and positive psychotic symptoms were frequent (5-year cumulative prevalence rates of around 12%) and occurred in combination more often than predicted by chance. Negative/disorganized symptoms revealed a pattern of sociodemographic associations indicative of developmental impairment, whereas the positive symptoms were associated with environmental exposures such as trauma, cannabis use, and urbanicity. Negative/disorganized symptoms predicted positive symptoms over time, and co-occurrence of positive and negative/disorganized symptoms was predictive of clinical relevance in terms of secondary functional impairment and help-seeking behavior.

Conclusion:

The results suggest that the negative/disorganized features associated with psychotic disorder are distributed at the population level and drive the ontogenesis of positive psychotic experiences after exposure to environmental risks, increasing the likelihood of impairment and need for care.
Systematic review of general population surveys indicates that the experiences associated with psychotic disorder, such as paranoid delusional thinking and auditory hallucinations, are observed—in an attenuated form—in 5%–8% of respondents (1, 2). These attenuated expressions may be conceived as the behavioral expression of an underlying distributed liability for psychosis (3). There is evidence from a range of representative general population samples (49) as well as high-risk samples (10, 11) that low-grade psychotic experiences may precede affective and nonaffective clinical psychotic states by many years. Therefore, a dimensional focus, following the expression of different symptom domains and their relation to the onset of dysfunction and help-seeking over time, may be productive.
The aforementioned population-based work has focused on experiences resembling positive psychotic symptoms; it is not known if and how attenuated negative/disorganized symptoms may play a role over time. There is evidence that negative symptoms are expressed, in attenuated form, in otherwise “healthys” individuals and that the combination of attenuated positive and negative symptoms predicts onset of need for care (12).
In this article, we present a longitudinal, 10-year study of young people. Hypotheses were derived from the suggestion that negative/disorganized symptoms (13) associated with schizophrenia (14) may represent alterations in brain development (1517) associated with distributed genetic risk (18), influencing a hypothesized final common pathway of neurotransmitter dysregulation (19), resulting in the onset of positive psychotic symptoms, particularly when combined with environmental exposures (20). It was hypothesized that 1) subclinical expressions of positive and negative/disorganized symptoms would be distributed in the general population and occur more often together than predicted by chance; 2) positive symptoms would be associated with environmental risks and negative/disorganized features with indices of developmental impairment; 3) negative/disorganized symptoms would predict psychotic experiences over time but not the other way around; and, finally, 4) “comorbid” expression of positive and negative/disorganized experiences would be associated with impairment and risk for patient status.

Method

Sample and Study Design

The Early Developmental Stages of Psychopathology Study collected data on the prevalence, incidence, risk factors, comorbidity, and course of mental disorders in a representative random population sample of adolescents and young adults, age 14–24 years, from the general population in Munich, Germany. The baseline sample, following ethics committee approval, was randomly drawn in 1994 from the respective population registry offices of Munich and its 29 counties to mirror the distribution of individuals expected to be 14–24 years of age at the time of the baseline (T0) interview in 1995. The base population were all those born between June 1, 1970, and May 31, 1981, registered as residents in these localities and having German citizenship. These registers can be regarded as highly accurate because 1) each German is registered by his town, 2) the registers are regularly updated, 3) in the interest of scientific studies, any number of randomly drawn addresses with a given sex and age group can be obtained, and 4) strict enforcement of registration by law and the police applies. More details on the sampling, representativeness, instruments, procedures, and statistical methods of the sample have previously been presented (21).
The longitudinal prospective design consisted of a baseline and three follow-up surveys (time 1, time 2, and time 3), covering a time period of on average 1.6, 3.5, and 8.4 years (range=7.3–10.5), respectively, from baseline. As the primary goal of the study was to examine developmental aspects of psychopathology, the younger group (14 and 15 years of age) was sampled at twice the rate of persons 16–21 years of age, and the oldest group (22–24 years) was sampled at half this rate. For the same reason, subjects 14–17 years of age at baseline were examined at all four time points, whereas the full baseline sample was only assessed at three time points (baseline, time 2, and time 3).
The present study is based on the three assessments that were available for the full baseline sample: 3,021 individuals 14–24 years of age at baseline and their follow-up assessments at time 2 (N=2,548; response rate=84%) and time 3 (N=2,210; 73%). Written informed consent was obtained from all participants.
Participants were interviewed with the Munich Composite International Diagnostic Interview (22). Trained and experienced clinical psychologists conducted the interviews at baseline (lifetime version) and follow-up assessments (interval version: covering the assessment period from the previous interview).

Psychopathology Assessment

Information from the psychosis section and the clinical interview rating section, with its embedded Brief Psychiatric Rating Scale (23), were used to derive measures of psychopathological clusters. In order to calculate measures of frequency, discrete variables indicating presence or absence of clusters across interview waves were, per definition, necessary.

Negative/disorganized symptom cluster.

A combined cluster of negative and disorganized symptoms was designed, in accordance with psychopathological findings in the early course of psychosis, showing that the “Bleulerian blend” of negative, catatonic/motor, and disorganization symptoms load on a single factor, while positive symptoms load on another (24) in agreement with Kraepelin's description in which avolition and disorganization were joined as the two defining features of the syndrome (25). Although negative, disorganized, positive, and affective clusters consistently load on separate domains in factor analytical studies of chronic psychotic patients (26, 27), meta-analysis indicates that negative and disorganized dimensions are conflated in their association with neurocognitive alterations, contrary to the positive and affective dimensions (28). A sensitivity analysis was planned, reanalyzing essential results for the negative cluster and the single disorganized item separately.
At baseline and time 3, two items concerning classic negative and disorganized symptoms from the interview ratings section were used: indifference (X11) and thought incoherence or illogicality (X12). These two items were rated on a 7-point scale (1=absent, 2=very little, 3=a little, 4=moderately, 5=moderately strong, 6=a lot, 7=very much). Each item was dichotomized: absent (coded as 0) versus present (coded as 1, indicating any score above “1”). For the purpose of the analyses, presence of the negative/disorganized cluster at baseline and time 3 was defined as a rating of “present” on either of the two items.
At time 2, not only the two previous items but also five items from the interview observation section were available: flat affect (P3), slow speech (P5), slow movement (P6), poverty of speech (P7), and avolition (P8). These five items were dichotomously rated: absent (coded as 0) versus present (coded as 1). Presence of the negative/disorganized cluster at time 2 was defined as a rating of “present” on any of the seven items.

Positive symptom cluster.

Interview ratings from the psychosis section (items G1, G2a, G3–G5, G7–G13, G13b, G14, G17, G18, G20, G20C, G21, and G22a) on delusions (15 items) and hallucinations (5 items) were collected at time 2 (lifetime) and time 3 (interval version). These 20 items concern classic psychotic symptoms, including Schneiderian first-rank symptoms such as audible thoughts, thought insertion, thought withdrawal, and made acts and impulses. Participants were first invited to read a list of all the psychotic experiences and asked whether they had ever experienced such symptoms. Each psychosis item was rated absent or present. Presence of the positive cluster was defined as a rating of “present” on any of the 20 psychosis items (6).

Depressive symptoms.

At time 2 and time 3, the 28 symptom items of the depression section were used. Items were rated either yes or no as being present for at least 2 weeks. A sum score of “depressive symptoms” was formed, with a minimum of 0 and a maximum score of 28 endorsements (29).

Cluster persistence.

The time 2 (lifetime) and time 3 (interval) ratings for the positive cluster were used to create a three-level summary “positive cluster persistence” variable: no occurrence (coded as 0), present at one assessment (coded as 1), and present at two assessments (coded as 2). In order to have a comparable longitudinal measure of “negative/disorganized cluster persistence,” the baseline (lifetime) and time 2 (interval) measures were combined into a cumulative lifetime variable. Together with the information at time 3 (interval), this resulted in a similar three-level summary score of persistence: no occurrence (coded as 0), present at one assessment (coded as 1), and present at two assessments (coded as 2)

Other Clinical Assessments

Age, gender, social status, marital status, level of education, urbanicity, cannabis exposure, and self-reported trauma were considered.
As part of the treatment module, participants were shown a list of different types of medication and were asked to endorse those they had been given for any psychopathological or psychosomatic problem. The acknowledgment of any antipsychotic medication (item Q1EA4) reported at time 2 and time 3 was used to derive the antipsychotic treatment variable (coded as 1 for yes).
Clinical relevance of positive psychotic symptoms was assessed with interview ratings of the psychosis section (6). Three help-seeking items assessed whether participants had ever sought help because of psychotic symptoms: seeking doctors' help because of delusions (G16) or hallucinations (G23) or seeking help from other mental health professionals, ranging from a general practitioner or school psychologist to psychiatric sheltered housing (Q1DG). A dichotomous “help-seeking” variable was created, indicating a positive answer to any of the three questions (coded as 1) versus negative answers on all.
The diagnostic interview also assesses the effect of psychotic experiences on feeling upset or unable to work, go places, or enjoy oneself at the time of having these experiences (G28); being less able to work (G29) or less able to make friends or enjoy social relationships (G29a) since these experiences began; and how much their life and everyday activities were impaired when these experiences were at their worst (G36). A dichotomous “dysfunction” variable was created representing a positive answer on any of the four questions (coded as 1) versus negative answers on all.
Finally, a dichotomous variable “psychotic impairment” was created, coded as 1 for subjects with psychotic experiences who had ratings of “1” on either help-seeking or dysfunction or both.
The interviewer's opinion regarding clinical evidence of psychological ill health (item X16) was rated according to four levels: 0=essentially not noticeable, 1=not very noticeable, 2=clearly ill, and 3=very ill. The dichotomous variable “caseness” indicated individuals with a noticeable level of psychiatric caseness (i.e., any score above “1”).

Statistical Analyses

All analyses were conducted using the software package STATA 10.1 (StataCorp, 2008).
First, in order to investigate the reliability and the rate of the variables representing the positive and the negative/disorganized psychopathological domains, the Cronbach alpha coefficient was used as a measure of internal consistency for each symptom cluster: the negative/disorganized cluster (24), the negative cluster (excluding the disorganized item), and the positive cluster (6) at time 2. Alpha values of 0.7 are regarded as satisfactory. Lifetime cumulative incidence and interval prevalence estimates of the positive cluster were calculated. Prevalence estimates of the negative/disorganized cluster were calculated, with and without additional sensitivity analyses excluding 1) participants exposed to antipsychotic treatment or 2) individuals with a DSM-IV diagnosis of depression (secondary negative symptoms). The distribution of symptom clusters was examined at time 2 and time 3, distinguishing individuals with only negative/disorganized symptoms, only positive symptoms, or a combination of the two. Because additional exclusion of participants exposed to antipsychotic treatment or individuals with a DSM-IV diagnosis of depression revealed no change in the rates, no sensitivity analysis was conducted.
Second, associations between psychopathology and risk factors were examined. It was hypothesized that the negative/disorganized cluster would be associated with younger age (30), male sex (31), and single marital status and low educational level (32), whereas female sex (31), cannabis exposure (33), urbanicity (34), self-reported trauma (34), and low level of education (32) would show significant associations with the positive cluster. Logistic regression analyses were conducted with the data in the “long” format, i.e., each individual contributing two timepoint observations (time 2 and time 3). Clustering within subjects was controlled for by including a variable reflecting measurement occasion in the model. Associations were expressed as odds ratios and their 95% confidence intervals (95% CI).
Third, in order to examine the natural association between the positive and negative/disorganized clusters (24), cross-sectional associations between the two were examined, controlling for depressive symptoms. Again, logistic regression analyses were carried out with the data in the “long” format (time 2 and time 3), adjusting for the indicator variable representing measurement occasion. Given that cross-sectional associations between symptoms may arise as a function of shared interview variance or represent chronicity effects, associations between clusters were also carried out in longitudinal predictive models across measurement occasions. Thus, logistic regression was used to calculate 1) the association between the negative/disorganized cluster at time 2 and the positive cluster at time 3, controlling for depressive symptoms and excluding individuals in whom the positive cluster was present at time 2; and 2) the association between the positive cluster at time 2 and the negative/disorganized cluster at time 3, controlling for depressive symptoms and excluding individuals in whom the lifetime negative/disorganized cluster was present at time 2.
Fourth, the null hypothesis of independence of the natural courses of the two psychopathological domains (35) was examined, analyzing the influence of the degree of persistence (from the interview assessing lifetime presence to time 3) of one psychosis cluster (i.e., positive cluster or negative/disorganized cluster) on time 3 onset of the other cluster and vice versa. To this end, logistic regression analyses were performed to examine the associations between 1) the degree of negative/disorganized persistence on the one hand and first onset (incidence) of positive cluster at time 3 on the other in individuals without lifetime positive cluster present at time 2, and 2) the degree of negative/disorganized persistence on the one hand and positive cluster at time 3 on the other in individuals with lifetime positive cluster present at time 2 and vice versa, controlling for depressive symptoms at time 3.
Fifth, the clinical relevance of the combination of positive and negative/disorganized experiences was calculated by examining whether the association between the positive cluster and its associated psychotic impairment rating was moderated by the negative/disorganized cluster. Consistent with previous work, the interaction between the positive cluster and the negative/disorganized cluster was calculated on the additive scale (33, 34, 36) using the STATA BINREG command, controlling for depression, with the data in the “long” format. In order to validate psychosis impairment, logistic regression analyses were conducted against the caseness and antipsychotic treatment variables.

Results

The average age of the participants at baseline was 18.3 years (range=14–24). Demographic characteristics are depicted in Table 1.
TABLE 1. Demographic Characteristics of a General Population Sample of Adolescents and Young Adults (N=3,021) Followed Longitudinally for the Early Developmental Stages of Psychopathology Study
CharacteristicN%
Gender  
    Male1,53350.74
    Female1,48849.26
Level of educationa  
    Low (mandatory basic school or learning a profession)47515.72
    Medium (high school)91530.29
    High (university or high school preparing for university)1,63153.99
Social statusb  
    Lower (lower class; lower middle class)2076.85
    Middle (middle middle class)1,80459.72
    Upper (higher middle class; upper class)95031.45
    Other (none of the above or missing values)601.99
Urbanicityc  
    Rural (surrounding areas of Munich)85928.43
    Urban (city of Munich)2,16271.57
a
The participants were asked which level of education they were attending or, in the case of discontinuation, which was the highest level they had attended (Munich-CIDI item A3).
b
The participants were asked to choose from the specified options the class he or she believed to be in (Munich-CIDI item A16).
c
Obtained through German government population registries. The population density of the Munich surrounding areas was 553 persons per square mile, and that of the city 4,061 persons per square mile.

Natural Rates

Items in each psychopathological cluster were strongly correlated, yielding satisfactory internal consistency (seven negative/disorganized cluster items: Cronbach alpha=0.75; six negative cluster items [excluding the disorganized item]: Cronbach alpha=0.76; 20 positive cluster items: Cronbach alpha=0.67). The association between the disorganized item and negative cluster yielded an odds ratio of 13.9 (95% CI=6.5–29.6), against an odds ratio of 2.47 (95% CI=1.18–5.19) for the association between the disorganized item and positive cluster, supporting the a priori choice for a single negative/disorganized cluster.
The positive cluster cumulative lifetime incidence was 22.7% (N=574) at time 2 while the interval prevalence was 12.4% (N=274) at time 3. The baseline prevalence of the negative/disorganized cluster was 11.4% (N=345) while the follow-up prevalences were 12.8% (N=325) at time 2 and 12.2% (N=270) at time 3. No impact was seen on these rates following exclusion of individuals exposed to antipsychotic treatment (N=3 at time 2 and N=1 at time 3 for revised rates of 12.7% and 12.2%, respectively) or individuals with a DSM-IV diagnosis of depression (N=41 at baseline, N=43 at time 2, and N=32 at time 3 for revised rates of 11.3%, 12.3%, and 12.1%).
In terms of population distribution (Table 2), 15.7% of the 2,548 participants reported lifetime cumulative incidence of only negative/disorganized symptoms at time 2 and 17.0% reported only positive symptoms, whereas 5.5% reported both, more than twice what would be expected by chance alone (2.6%). Interval prevalence rates at time 3 were, respectively, 9.9%, 10.1%, and 2.3% of a total of 2,210 participants, again more than twice the expected rate (1%).
TABLE 2. Psychopathological Clusters and Risk for Psychotic Impairmenta
Psychosis Variable and TimepointTotal NNegative/Disorganized OnlyPositive OnlyCo-Occurrence of Both Clusters
  N%N%N%
Symptom cluster rate       
    Time 2 (lifetime cumulative incidence)2,54840015.743417.01405.5
    Time 3 (interval prevalence)2,2102209.922410.1502.3
Psychotic impairment rate       
    Time 2 (lifetime cumulative incidence)226  15535.7b7150.7b
    Time 3 (interval prevalence)115  8839.3c2754.0c
  Risk Difference (%)d95% CIRisk Difference (%)d95% CIRisk Difference (%)d95% CI
Excess risk for psychotic impairment       
    Time 2 0 3732–415343–64
    Time 3 0 3933–465439–67
    Both time 2 and time 3 0 3734–415345–62
a
Psychotic experiences resulting in help-seeking or dysfunction.
b
Of subjects with symptom cluster at time 2.
c
Of subjects with symptom cluster at time 3.
d
Risk difference expresses excess risk for psychotic impairment given presence of symptom cluster or co-occurrence symptom cluster; as psychotic impairment was only assessed in the context of positive symptoms, rates are 0% for negative/disorganized only.

Cluster Associations

The negative/disorganized cluster was significantly associated with younger age, male sex, single marital status, and low educational level, whereas the positive cluster was significantly associated with low educational level, cannabis exposure, urbanicity, and self-reported trauma. The combination of both clusters was significantly associated with all variables except gender (Table 3).
TABLE 3. Association of Sociodemographic and Environmental Risk Factors With Psychopathological Symptom Clusters at Time 2 (N=2,548) and Time 3 (N=2,210)
Risk FactorNegative/Disorganized ClusterPositive ClusterCo-occurrence of Both Symptom Clusters
Odds Ratio95% CIOdds Ratio95% CIOdds Ratio95% CI
Age0.91**0.89–0.930.990.97–1.010.88**0.84–0.93
Gender (male versus female)0.69**0.61–0.790.900.77–1.050.730.52–1.03
Single marital status (never married, living apart, divorced, or widowed versus married)2.13**1.51–3.011.280.97–1.7015.16**2.11–108.91
Lower level of education (low versus medium and high)1.90**1.62–2.231.36**1.09–1.681.75*1.14–2.67
Cannabis exposurea1.120.91–1.392.10**1.61–2.752.05**1.18–3.59
Urbanicity (rural versus urban)1.120.97–1.291.19*1.01–1.411.51*1.01–2.27
Traumab0.980.85–1.131.50**1.29–1.761.67**1.17–2.40
a
A dichotomous variable defined as cannabis use of 5 times or more (33) since the previous interview (time 2 and time 3).
b
Self-reported trauma at time 2 and time 3 was labeled with any affirmative response of exposure to any of the nine traumata from the Trauma module (Munich-CIDI item N1A) (34). Respondents indicated a positive response on a visually presented list of nine groups of specified traumatic events.
*p<0.05.
**p<0.01.
Cross-sectionally, the negative/disorganized cluster was significantly associated with the positive cluster, controlling for depressive symptoms (odds ratio=1.4, 95% CI=1.1–1.7). The prospective association between the negative/disorganized cluster at time 2 and the positive cluster at time 3, excluding individuals with presence of lifetime positive cluster at time 2 and controlling for depressive symptoms, was significant (odds ratio=2.3, 95% CI=1.5–3.7). In contrast, the prospective association between the positive cluster at time 2 and the negative/disorganized cluster at time 3, excluding individuals with the lifetime negative/disorganized cluster present at time 2 and controlling for depressive symptoms, was neither large nor significant (odds ratio=0.8, 95% CI=0.5–1.2).

Independence of Natural Course

After depressive symptoms were controlled, persistence of the negative/disorganized symptom cluster not only predicted positive cluster persistence but also time 3 incident psychotic experiences in a dose-response fashion. In contrast, persistence of the positive symptom cluster predicted neither negative/disorganized cluster persistence nor incident negative/disorganized symptoms at time 3 (Table 4).
TABLE 4. Longitudinal Association of Symptom Cluster Courses
Exposure Variable: Symptom Cluster PersistenceaOutcome Variable: Incidence or Persistence of Symptoms
Odds Ratio95% CIOdds Ratio95% CI
Positive Symptom ClusterIncident Negative/Disorganized ClusterPersistent Negative/Disorganized Cluster
    0    
    10.80.6–1.31.30.7–2.3
    21.30.7–2.61.40.6–3.3
Negative/Disorganized Symptom ClusterIncident Positive ClusterPersistent Positive Cluster
    0    
    11.6*1.1–2.41.7*1.1–2.8
    24.5**2.3–8.73.4**1.3–9.0
a
0=no occurrence; 1=present at one assessment point; 2=present at two assessment points.
*p<0.05.
**p<0.01.

Clinical Relevance

Psychotic impairment was strongly associated with the variables of caseness (odds ratio=10.3, 95% CI=6.9–15.2) and antipsychotic treatment (odds ratio=15.3, 95% CI=6.1–38.4).
Table 2 depicts the proportions of individuals with psychotic impairment among those in whom the positive cluster was present at time 2 and time 3. Differences in risk for psychotic impairment for each psychopathological cluster were statistically significant in the combined time 2 and time 3 data analysis, as evidenced by the estimated additive interaction between the two clusters in the model of impairment (risk difference=16.2%, 95% CI=7.3%–25.2%). Analyzing time 2 and time 3 separately revealed replication at both time points (Table 2).

Separating Negative and Disorganized Symptoms

The rate of the separate negative cluster at the different time points was similar to that of the combined negative/disorganized cluster (prevalence rates around 12%), whereas the rate of the single item of disorganization was around 1%–3%. The pattern of associations with sociodemographic and environmental risk factors found for the combined negative/disorganized cluster was similar when analyzed separately for the negative cluster and disorganization item. Similarly, the cross-sectional associations between the positive cluster on the one hand and the separate negative cluster and disorganization item on the other was similar as observed for the original negative/disorganized cluster.
With regard to prospective associations, the negative cluster predicted onset and persistence of the positive cluster similar to the combined negative/disorganized cluster, whereas results for the single item of disorganization were directionally similar but less clear-cut (all results available upon request).

Discussion

Even after exclusion of ill individuals using antipsychotic medication, positive and negative/disorganized experiences resembling the symptoms of psychotic disorder occurred in the general population (5-year interval rates of around 12%). Positive and negative/disorganized experiences clustered together more often than predicted by chance, independent of depression, yet displayed a differential pattern of associations with sociodemographic and environmental risk factors. The negative/disorganized cluster was associated with a profile indicative of developmental impairment and the positive cluster with environmental risks. Their pattern over time revealed that persistent expression of the negative/disorganized cluster predicted onset of psychotic experiences; in contrast, persistent expression of psychotic experiences did not predict onset of negative/disorganized features. Finally, “comorbid” expression of the two clusters increased the risk for impairment and, by implication, need for care.

Negative/Disorganized Features Predict Positive Features and Onset of Clinical Psychosis

The negative/disorganized symptoms (13) associated with schizophrenia (14) may represent alterations in brain development (1517) associated with distributed genetic risk (18), influencing a hypothesized final common pathway of neurotransmitter dysregulation (19) resulting in the onset of positive psychotic symptoms, particularly when combined with environmental exposures (20). Several elements in the current epidemiological analysis support this model.
First, the pattern of associations for the negative/disorganized cluster with young age, male sex, single marital status, and lower educational level resembles the pattern seen in clinical samples (30, 31). A profile indicative of developmental impairment is concordant with meta-analytic work demonstrating a unique association of the negative/disorganized domain with neurocognitive impairment (28), poorer social functioning (37), poorer response to antipsychotic treatment (38), and a worse prognosis (39).
Second, the sociodemographic associations of the positive cluster are in agreement with previous reports linking positive psychotic experiences to environmental risk factors such as cannabis exposure, urbanicity, self-reported trauma, and lower educational level (3234).
Third, in most of the individuals both symptom clusters did not overlap. Nonetheless, the positive and negative/disorganized symptom domains clustered together more often than could be expected by chance alone. Thus, psychotic disorders such as schizophrenia may not be the result of the chance cross-section of the separate liabilities of developmental impairment on the one hand and reality distortion on the other; they are linked together in a way that suggests fundamental overlap or interaction of underlying mechanisms (Figure 1).
FIGURE 1. Negative/Disorganized Features Predict Positive Features and Onset of Clinical Psychosis
a The longitudinal analysis suggested that the negative/disorganized cluster associated with a sociodemographic pattern indicative of developmental impairment reflects an underlying vulnerability that, when combined with environmental exposures such as cannabis use, trauma, and urbanicity, results in positive psychotic symptoms increasing the risk of impairment and clinical relevance.
Fourth, importantly, the longitudinal analysis suggested that in this community sample negative/disorganized features—the negative features more than the disorganized—preceded positive features rather than the other way round. This finding is in agreement with follow-back studies showing that negative features frequently represent an initial symptom of schizophrenia, occurring more than 2 years before the emergence of positive symptoms (40).

Methodological Issues

First, assessment of psychotic experiences was based on self-report information by the respondents in diagnostic interviews, complemented by clinical ratings of core features of positive, negative, and disorganized symptoms derived from the clinical rating section and selected items from the Brief Psychiatric Rating Scale (23). False positive psychotic experiences are likely to have occurred, increasing random error; nevertheless, there is a substantial literature on the (predictive and other forms of) validity of self-reported psychotic experiences (1, 49).
Second, despite the hazard of under/overestimation of true positive, clinically relevant psychotic experiences (6), the validation of the outcome variable against caseness and antipsychotic treatment supports the validity of psychotic impairment as a proxy measure of clinical relevance.
Third, the definition of clinically relevant psychosis was contingent on the presence of positive psychotic experiences. This, however, is in line with the diagnostic criteria for schizophrenia, which require positive psychotic experiences for making the diagnosis.
Fourth, the measures of negative/disorganized symptoms were varying between measurement occasions. This is likely to have generated more random error resulting in a more conservative estimate of associations (i.e., the overlap between positive cluster and negative/disorganized cluster may be stronger than reported and the predictive value for positive psychotic experiences may be higher).
Finally, the threshold of the negative/disorganized cluster may be considered too low. However, a sensitivity analysis using a higher threshold (any score above “3”) yielded similar results (data not shown, available upon request).

Footnotes

Received June 24, 2009; revisions received October 6, 2009, and Jan. 25 and March 1, 2010; accepted March 22, 2010
This article is featured in this month's AJP Audio and is discussed in an editorial by Dr. Carpenter (p. 1013).
Dr. can Saka reports having consulted for Janssen-Cilag and receiving speaker honoraria from Janssen-Cilag, Abdi İbrahim, and Sanovel. Dr. Lieb reports receiving speaker honoraria from Wyeth. Dr. Wittchen reports receiving research support from Novartis, Pfizer, Schering-Plough; having consulted for Novartis, Pfizer, Wyeth, Organon, and Lundbeck; and receiving speaker honoraria from Novartis, Schering-Plough, Pfizer, Wyeth, and Servier. Dr. van Os reports having been an unrestricted research grant holder with, or having received financial compensation as an independent symposium speaker from Eli Lilly, BMS, Lundbeck, Organon, Janssen-Cilag, GSK, AstraZeneca, Pfizer, and Servier—companies that have an interest in the treatment of psychosis. Dr. Dominguez reports no financial relationships with commercial interests.
This work is part of the Early Developmental Stages of Psychopathology (EDSP) Study and is supported by the German Federal Ministry of Education and Research (BMBF) project no. 01EB9405/6, 01EB9910/6, EB10106200, 01EB0140, and 01EB0440. Part of the field work and analyses were also additionally supported by grants of the Deutsche Forschungsgemeinschaft (DFG) LA1148/1-1, WI2246/7-1, and WI709/8-1.
Principal investigators of the EDSP Study are Drs. Wittchen and Lieb. Both take responsibility for the integrity of the study data. All authors and co-authors had full access to all study data. Data analysis and manuscript preparation were completed by the authors and co-authors of this article, who take responsibility for its accuracy and content. Core staff members of the EDSP group are Dr. Katja Beesdo; Dr. Petra Zimmermann; Dr. Axel Perkonigg, Ph.D., Dipl.-Stat; Michael Höfler, Dipl.-Psych.; Tanja Brückl, Dipl.-Psych.; Agnes Nocon, Dipl.-Inf.; Hildegard Pfister, Dipl.-Soz.; Barbara Spiegel, Dipl.-Psych.; and Andrea Schreier. Scientific advisors are Dr. Jules Angst (Zurich), Dr. Kathleen Merikangas (NIMH, Bethesda), Dr. Ron Kessler (Harvard, Boston), and Dr. Jim van Os (Maastricht).

References

1.
van Os J, Linscott RJ, Myin-Germeys I, Delespaul P, Krabbendam L: A systematic review and meta-analysis of the psychosis continuum: evidence for a psy-chosis proneness-persistence-impairment model of psychotic disorder. Psychol Med 2009; 39:179–195
2.
Polanczyk G, Moffitt TE, Arseneault L, Cannon M, Ambler A, Keefe RS, Houts R, Odgers CL, Caspi A: Etiological and clinical features of childhood psychotic symptoms: results from a birth cohort. Arch Gen Psychiatry 2010; 67:328–338
3.
Lataster T, Myin-Germeys I, Derom C, Thiery E, van Os J: Evidence that self-reported psychotic experiences represent the transitory developmental expres-sion of genetic liability to psychosis in the general population. Am J Med Genet B Neuropsychiatr Genet 2009; 150B:1078–1084
4.
Welham J, Scott J, Williams G, Najman J, Bor W, O'Callaghan M, McGrath J: Emotional and behavioural antecedents of young adults who screen positive for non-affective psychosis: a 21-year birth cohort study. Psychol Med 2009; 39:625–634
5.
Poulton R, Caspi A, Moffitt TE, Cannon M, Murray R, Harrington H: Children's self-reported psychotic symptoms and adult schizophreniform disorder: a 15-year longitudinal study. Arch Gen Psychiatry 2000; 57:1053–1058
6.
Dominguez MD, Wichers M, Lieb R, Wittchen HU, van Os J: Evidence that onset of clinical psychosis is an outcome of progressively more persistent subclini-cal psychotic experiences: an 8-year cohort study. Schizophr Bull [Epub ahead of print: May 21, 2009]
7.
Hanssen M, Bak M, Bijl R, Vollebergh W, van Os J: The incidence and outcome of subclinical psychotic experiences in the general population. Br J Clin Psy-chol 2005; 44(Pt 2):181–191
8.
Weiser M, Werbeloff N, Drukker M, van Os J, Dohrenwend BP, Yoffe R, Levav I, Davidson M: Self-reported psychotic symptoms in the community, and risk of later hospitalization for non-affective psychotic disorders, in Abstracts for the 12th International Congress on Schizophrenia Research (ICOSR). Schizophr Bull 2009; 35(March suppl):74
9.
Chapman LJ, Chapman JP, Kwapil TR, Eckblad M, Zinser MC: Putatively psychosis-prone subjects 10 years later. J Abnorm Psychol 1994; 103:171–183
10.
Cannon TD, Cadenhead K, Cornblatt B, Woods SW, Addington J, Walker E, Seidman LJ, Perkins D, Tsuang M, McGlashan T, Heinssen R: Prediction of psy-chosis in youth at high clinical risk: a multisite longitudinal study in North America. Arch Gen Psychiatry 2008; 65:28–37
11.
McGorry PD, Yung AR, Bechdolf A, Amminger P: Back to the future: predicting and reshaping the course of psychotic disorder. Arch Gen Psychiatry 2008; 65:25–27
12.
Maric N, Myin-Germeys I, Delespaul P, de Graaf R, Vollebergh W, Van Os J: Is our concept of schizophrenia influenced by Berkson's bias? Soc Psychiatry Psychiatr Epidemiol 2004; 39:600–605
13.
Flaum M, Andreasen N: The reliability of distinguishing primary versus secondary negative symptoms. Compr Psychiatry 1995; 36:421–427
14.
Kirkpatrick B, Buchanan RW, Ross DE, Carpenter WT: A separate disease within the syndrome of schizophrenia. Arch Gen Psychiatry 2001; 58:165–171
15.
Heckers S, Goff D, Schacter DL, Savage CR, Fischman AJ, Alpert NM, Rauch SL: Functional imaging of memory retrieval in deficit vs nondeficit schizophre-nia. Arch Gen Psychiatry 1999; 56:1117–1123
16.
Buchanan RW, Breier A, Kirkpatrick B, Elkashef A, Munson RC, Gellad F, Carpenter WT: Structural abnormalities in deficit and nondeficit schizophrenia. Am J Psychiatry 1993; 150:59–65
17.
Rowland LM, Spieker EA, Francis A, Barker PB, Carpenter WT, Buchanan RW: White matter alterations in deficit schizophrenia. Neuropsychopharmacology 2009; 34:1514–1522
18.
Goldman AL, Pezawas L, Mattay VS, Fischl B, Verchinski BA, Chen Q, Weinberger DR, Meyer-Lindenberg A: Widespread reductions of cortical thickness in schizophrenia and spectrum disorders and evidence of heritability. Arch Gen Psychiatry 2009; 66:467–477
19.
Morrison PD, Murray RM: From real-world events to psychosis: the emerging neuropharmacology of delusions. Schizophr Bull 2009; 35:668–674
20.
van Os J, Kapur S: Schizophrenia. Lancet 2009; 374(9690):635–645
21.
Lieb R, Isensee B, von Sydow K, Wittchen HU: The Early Developmental Stages of Psychopathology study (EDSP): a methodological update. Eur Addict Res 2000; 6:170–182
22.
Wittchen HU, Pfister H: DIS-X-Interviews: Manual für Screening-Verfahren und Interview; Interviewheft Längsschnittuntersuchung (DIA-X-Lifetime); Er-gänzungsheft (DIA-X-Lifetime); Interviewheft Querschnittsuntersuchung (DIA-X-12. Monats-Version); Ergänzungsheft (DIA-X-12. Monats-Version); PC-Programm zur Durchführung der Interviews (Längsund Querschnittsuntersuchung); Auswertungsprogramm. Frankfurt, Germany, Swets & Zeitlinger, 1997
23.
Overall JE, Gorham DR: The Brief Psychiatric Rating Scale. Psychol Rep 1962; 10:799–812
24.
McGorry PD, Bell RC, Dudgeon PL, Jackson HJ: The dimensional structure of first episode psychosis: an exploratory factor analysis. Psychol Med 1998; 28:935–947
25.
Kraepelin E: Demential Praecox and Paraphrenia. New York, Robert E Krieger, 1971
26.
Liddle PF: The symptoms of chronic schizophrenia: a re-examination of the positive- negative dichotomy [see comments]. Br J Psychiatry 1987; 151:145–151
27.
Bilder RM, Mukherjee S, Rieder RO, Pandurangi AK: Symptomatic and neuropsychological components of defect states. Schizophr Bull 1985; 11:409–419
28.
Dominguez MDG, Viechtbauer W, Simons CJP, Van Os J, Krabbendam L: Are psychotic psychopathology and neurocognition orthogonal? a systematic re-view of their associations. Psychol Bull 2009; 135:157–171
29.
Krabbendam L, Myin-Germeys I, De Graaf R, Vollebergh W, Nolen WA, Iedema J, Van Os J: Dimensions of depression, mania and psychosis in the general population. Psychol Med 2004; 34:1177–1186
30.
Schultz SK, Miller DD, Oliver SE, Arndt S, Flaum M, Andreasen NC: The life course of schizophrenia: age and symptom dimensions. Schizophrenia Res 1997; 23:15–23
31.
Leung A, Chue P: Sex differences in schizophrenia: a review of the literature. Acta Psychiatr Scand Suppl 2000; 401:3–38
32.
van Os J, Hanssen M, Bijl RV, Ravelli A: Strauss (1969) revisited: a psychosis continuum in the general population? Schizophr Res 2000; 45(1–2):11–20
33.
Henquet C, Krabbendam L, Spauwen J, Kaplan C, Lieb R, Wittchen HU, van Os J: Prospective cohort study of cannabis use, predisposition for psychosis, and psychotic symptoms in young people. BMJ 2005; 330:11
34.
Spauwen J, Krabbendam L, Lieb R, Wittchen HU, van Os J: Evidence that the outcome of developmental expression of psychosis is worse for adolescents growing up in an urban environment. Psychol Med 2006; 36:407–415
35.
Eaton WW, Thara R, Federman B, Melton B, Liang KY: Structure and course of positive and negative symptoms in schizophrenia. Arch Gen Psychiatry 1995; 52:127–134
36.
Darroch J: Biologic synergism and parallelism. Am J Epidemiol 1997; 145:661–668
37.
Macdonald EM, Hayes RL, Baglioni AJ: The quantity and quality of the social networks of young people with early psychosis compared with closely matched controls. Schizophr Res 2000; 46:25–30
38.
Erhart SM, Marder SR, Carpenter WT: Treatment of schizophrenia negative symptoms: future prospects. Schizophr Bull 2006; 32:234–237
39.
McGlashan TH, Fenton WS: The positive-negative distinction in schizophrenia: review of natural history validators. Arch Gen Psychiatry 1992; 49:63–72
40.
Hafner H, Maurer K: Early detection of schizophrenia: current evidence and future perspectives. World Psychiatry 2006; 5:130–138

Information & Authors

Information

Published In

Go to American Journal of Psychiatry
Go to American Journal of Psychiatry
American Journal of Psychiatry
Pages: 1075 - 1082
PubMed: 20634371

History

Received: 24 June 2009
Revision received: 6 October 2009
Revision received: 25 January 2010
Revision received: 1 March 2010
Accepted: 11 March 2010
Published online: 1 September 2010
Published in print: September 2010

Authors

Details

Maria-de-Gracia Dominguez, M.D.
From the Department of Psychiatry and Neuropsychology, School of Mental Health and Neuroscience, Maastricht University Medical Centre; Department of Psychiatry, School of Medicine, Ankara University, Ankara, Turkey; Max Planck Institute of Psychiatry, Clinical Psychology and Epidemiology Unit, Munich, Germany; Institute of Clinical Psychology and Psychotherapy, Technical University Dresden, Dresden, Germany; Division of Psychological Medicine, Institute of Psychiatry, London; Department of Epidemiology and Health Psychology, Institute of Psychology, University of Basel, Basel, Switzerland.
Meram Can Saka, M.D.
From the Department of Psychiatry and Neuropsychology, School of Mental Health and Neuroscience, Maastricht University Medical Centre; Department of Psychiatry, School of Medicine, Ankara University, Ankara, Turkey; Max Planck Institute of Psychiatry, Clinical Psychology and Epidemiology Unit, Munich, Germany; Institute of Clinical Psychology and Psychotherapy, Technical University Dresden, Dresden, Germany; Division of Psychological Medicine, Institute of Psychiatry, London; Department of Epidemiology and Health Psychology, Institute of Psychology, University of Basel, Basel, Switzerland.
Roselind Lieb, Ph.D.
From the Department of Psychiatry and Neuropsychology, School of Mental Health and Neuroscience, Maastricht University Medical Centre; Department of Psychiatry, School of Medicine, Ankara University, Ankara, Turkey; Max Planck Institute of Psychiatry, Clinical Psychology and Epidemiology Unit, Munich, Germany; Institute of Clinical Psychology and Psychotherapy, Technical University Dresden, Dresden, Germany; Division of Psychological Medicine, Institute of Psychiatry, London; Department of Epidemiology and Health Psychology, Institute of Psychology, University of Basel, Basel, Switzerland.
Hans-Ulrich Wittchen, Ph.D.
From the Department of Psychiatry and Neuropsychology, School of Mental Health and Neuroscience, Maastricht University Medical Centre; Department of Psychiatry, School of Medicine, Ankara University, Ankara, Turkey; Max Planck Institute of Psychiatry, Clinical Psychology and Epidemiology Unit, Munich, Germany; Institute of Clinical Psychology and Psychotherapy, Technical University Dresden, Dresden, Germany; Division of Psychological Medicine, Institute of Psychiatry, London; Department of Epidemiology and Health Psychology, Institute of Psychology, University of Basel, Basel, Switzerland.
Jim van Os, M.D., Ph.D.
From the Department of Psychiatry and Neuropsychology, School of Mental Health and Neuroscience, Maastricht University Medical Centre; Department of Psychiatry, School of Medicine, Ankara University, Ankara, Turkey; Max Planck Institute of Psychiatry, Clinical Psychology and Epidemiology Unit, Munich, Germany; Institute of Clinical Psychology and Psychotherapy, Technical University Dresden, Dresden, Germany; Division of Psychological Medicine, Institute of Psychiatry, London; Department of Epidemiology and Health Psychology, Institute of Psychology, University of Basel, Basel, Switzerland.

Notes

Address correspondence and reprint requests to Prof. van Os, Department of Psychiatry and Neuropsychology, Maastricht University Medical Centre, PO BOX 616 (DRT 10), 6200 MD Maastricht, the Netherlands; [email protected] (e-mail).

Metrics & Citations

Metrics

Citations

Export Citations

If you have the appropriate software installed, you can download article citation data to the citation manager of your choice. Simply select your manager software from the list below and click Download.

For more information or tips please see 'Downloading to a citation manager' in the Help menu.

Format
Citation style
Style
Copy to clipboard

View Options

View options

PDF/EPUB

View PDF/EPUB

Get Access

Login options

Already a subscriber? Access your subscription through your login credentials or your institution for full access to this article.

Personal login Institutional Login Open Athens login
Purchase Options

Purchase this article to access the full text.

PPV Articles - American Journal of Psychiatry

PPV Articles - American Journal of Psychiatry

Not a subscriber?

Subscribe Now / Learn More

PsychiatryOnline subscription options offer access to the DSM-5-TR® library, books, journals, CME, and patient resources. This all-in-one virtual library provides psychiatrists and mental health professionals with key resources for diagnosis, treatment, research, and professional development.

Need more help? PsychiatryOnline Customer Service may be reached by emailing [email protected] or by calling 800-368-5777 (in the U.S.) or 703-907-7322 (outside the U.S.).

Media

Figures

Other

Tables

Share

Share

Share article link

Share