Introduction
Diagnosis in psychiatry has frequently come under fire. Robins & Guze (Reference Robins and Guze1970) discussed how clinical features, outcome and family history can be used to create nosological categories in the absence of clinical tests. The National Institute of Mental Health recently criticized the validity of the Diagnostic and Statistical Manual of Mental Disorders (DSM), stating ‘Unlike our definitions of ischemic heart disease, lymphoma, or AIDS, the DSM diagnoses are based on a consensus about clusters of clinical symptoms, not any objective laboratory measure’ (Lane, Reference Lane2013). This lack of aetiologically based psychiatric classification has contributed to instability in psychiatric diagnoses over time.
A number of studies have examined diagnostic stability over time. Early research was heterogeneous in nature, reporting on differing diagnostic criteria, different diagnostic processes and differing methods of reporting results. More recently, however, researchers have followed the lead of Schwartz et al. (Reference Schwartz, Fennig, Tanenberg-Karant, Carlson, Craig, Galambos, Lavelle and Bromet2000) in reporting prospective and retrospective consistencies of diagnoses between two time points. Prospective consistency is the proportion of cases that receives a diagnosis at baseline and retains that diagnosis at follow-up. Retrospective consistency is the proportion of cases that receives a diagnosis at follow-up that they also had at baseline.
The prospective consistencies of schizophrenia and bipolar affective disorder have been reported at 80–100% in studies with up to 4 years of follow-up using first admission or first contact samples and more recent criteria [International Classification of Diseases (ICD)-10 or DSM-III onwards] (Amin et al. Reference Amin, Singh, Brewin, Jones, Medley and Harrison1999; Schwartz et al. Reference Schwartz, Fennig, Tanenberg-Karant, Carlson, Craig, Galambos, Lavelle and Bromet2000; Veen et al. Reference Veen, Selten, Schols, Laan, Hoek, van der Tweel and Kahn2004; Baldwin et al. Reference Baldwin, Browne, Scully, Quinn, Morgan, Kinsella, Owens, Russell, O'Callaghan and Waddington2005; Whitty et al. Reference Whitty, Clarke, McTigue, Browne, Kamali, Larkin and O'Callaghan2005; Salvatore et al. Reference Salvatore, Baldessarini, Tohen, Khalsa, Sanchez-Toledo, Zarate, Vieta and Maggini2009, Reference Salvatore, Baldessarini, Tohen, Khalsa, Sanchez-Toledo, Zarate, Vieta and Maggini2011). Studies with shorter follow-up periods report that diagnoses are more stable over time. Longer-term follow-up of the cohorts, identified by the Determinants of Outcome of Severe Mental Disorder (DOSMeD), World Health Organization Collaborative Study on the Assessment and Reduction of Social Disability (RAPyD) and International Pilot Study of Schizophrenia (IPSS) samples reported by Craig et al. (Reference Craig, Wanderling, Janca, Hopper, Harrison, Janca and Sartorius2007) identified prospective consistencies for schizophrenia of about 85% over 12–26 years of follow-up, using ICD-10 diagnoses converted using a World Health Organization algorithm from previous classification systems. Bromet et al. (Reference Bromet, Kotov, Fochmann, Carlson, Tanenberg-Karant, Ruggero and Chang2011) reported on the 10-year follow-up of a first admission cohort and identified similar diagnostic stability findings for schizophrenia and bipolar affective disorder.
Findings with regards to other psychotic categories are more variable. Depressive psychosis prospective consistencies are reported to be between 45 and 55% (Baca-Garcia et al. Reference Baca-Garcia, Perez-Rodriguez, Basurte-Villamor, Fernandez Del Moral, Jimenez-Arriero, Gonzalez De Rivera, Saiz-Ruiz and Oquendo2007a , Reference Baca-Garcia, Perez-Rodriguez, Basurte-Villamor, Lopez-Castroman, Fernandez Del Moral, Jimenez-Arriero, Gronzalez De Rivera, Saiz-Ruiz, Leiva-Murillo, De Prado-Cumplido, Santiago-Mozos, Artes-Rodriguez, Oquendo and De Leon b ; Bromet et al. Reference Bromet, Kotov, Fochmann, Carlson, Tanenberg-Karant, Ruggero and Chang2011) in long-term follow-up studies (10–12 years), compared with 75–100% in shorter-term follow-up studies (1.5–4 years; Schwartz et al. Reference Schwartz, Fennig, Tanenberg-Karant, Carlson, Craig, Galambos, Lavelle and Bromet2000; Schimmelmann et al. Reference Schimmelmann, Conus, Edwards, McGorry and Lambert2005; Whitty et al. Reference Whitty, Clarke, McTigue, Browne, Kamali, Larkin and O'Callaghan2005; Salvatore et al. Reference Salvatore, Baldessarini, Tohen, Khalsa, Sanchez-Toledo, Zarate, Vieta and Maggini2009, Reference Salvatore, Baldessarini, Tohen, Khalsa, Sanchez-Toledo, Zarate, Vieta and Maggini2011). Smaller diagnostic categories (where studied) demonstrate more variation still. Schizo-affective disorder, for example, has reported prospective consistencies ranging from 35% (Schwartz et al. Reference Schwartz, Fennig, Tanenberg-Karant, Carlson, Craig, Galambos, Lavelle and Bromet2000; Craig et al. Reference Craig, Wanderling, Janca, Hopper, Harrison, Janca and Sartorius2007) to 95–100% (Schimmelmann et al. Reference Schimmelmann, Conus, Edwards, McGorry and Lambert2005; Salvatore et al. Reference Salvatore, Baldessarini, Tohen, Khalsa, Sanchez-Toledo, Zarate, Vieta and Maggini2011). This variation probably reflects differences in the diagnostic system adopted, cohort (first contact v. first hospitalization) and length of follow-up. Further studies have attempted to address stability in less prevalent diagnoses such as acute and transient psychosis. These studies also show considerable variability in prospective consistency: 30% (Aadamsoo et al. Reference Aadamsoo, Saluveer, Kuunarpuu, Vasar and Maron2011); 73% (Sajith et al. Reference Sajith, Chandrasekaran, Sadanandan Unni and Sahai2002).
Many studies mentioned above used non-incidence samples. Incidence studies give a less biased estimate of diagnostic stability, as studies that recruit cases from non-first-episode samples are effectively sampling chronic cases in treatment, biasing the investigation towards those who are more unwell and excluding others who recover. One study has examined long-term diagnostic stability (13 years) in an incidence sample of psychosis patients but only including schizophrenia cases (Mason et al. Reference Mason, Harrison, Croudace, Glazebrook and Medley1997). To date, no study has yet examined diagnostic stability of all psychosis diagnoses specifically in incident cases over a follow-up period of longer than 8 years using current diagnostic criteria.
Identification of predictors of diagnostic change over time is important because predictors may aid in understanding why diagnoses change and indicate to clinical teams when to be attentive to potential change and adjust treatment accordingly. Studies of relatively short duration have examined predictors of diagnostic change in an incidence cohort, but only one study has looked at a long-term follow-up of diagnostic categories, in first admission cases (Schwartz et al. 2000; Salvatore et al. Reference Salvatore, Baldessarini, Tohen, Khalsa, Sanchez-Toledo, Zarate, Vieta and Maggini2009; Bromet et al. Reference Bromet, Kotov, Fochmann, Carlson, Tanenberg-Karant, Ruggero and Chang2011).
In this study we sought to complement the knowledge obtained from previous research, using a geographically defined incident sample of all psychoses diagnoses made using DSM-IV-TR and ICD-10 criteria, followed up and rediagnosed 10 years later, to fulfil two main aims: (1) to examine the stability of diagnostic categories 10 years after the first episode of psychosis; and (2) to examine which demographic and clinical characteristics are associated with diagnostic change.
Method
Baseline
This paper is based on data from the ÆSOP study (Kirkbride et al. Reference Kirkbride, Fearon, Morgan, Dazzan, Morgan, Tarrant, Lloyd, Holloway, Hutchinson, Leff, Mallett, Harrison, Murray and Jones2006; Morgan et al. Reference Morgan, Lappin, Heslin, Donoghue, Lomas, Reininghaus, Onyejiaka, Croudace, Jones, Murray, Fearon, Doody and Dazzan2014), an incidence study of all first-episode psychosis cases presenting for the first time to specialist mental health services in defined catchment areas in Nottingham and London.
At baseline, clinical and demographic data were collected from clinical records and, where possible, from interview with cases using the Schedules for Clinical Assessment in Neuropsychiatry (SCAN version 2; World Health Organization, 1994) and the Personal and Psychiatric History Schedule (World Health Organization, 1996). The SCAN was used to elicit symptom-related data at the time of presentation. Where an interview with the patient was not possible, case notes were used to complete the Item Group Checklist (IGC) part of the SCAN. Case summaries collated all relevant clinical information and were made available to consensus diagnostic meetings alongside the schedules above. ICD-10 (World Health Organization, 1993) and DSM-IV-TR (American Psychiatric Association, 2000) psychotic diagnoses were determined using all available clinical information (excluding clinical diagnosis) on the basis of consensus meetings involving at least one of the principal investigators with other members of the research team (at least one psychiatrist and one other member of the research team). Conflicting opinions on diagnosis were discussed in detail until a consensus was reached. This was made as soon as possible after first contact (generally within a few weeks). Cases with a dual diagnosis had their substance use disorder diagnosed separately. Diagnoses were made blind to ethnicity. Factor analyses of the SCAN and IGC data generated the following symptom dimensions: manic; depressive; disorganized; negative; and reality distortion (Demjaha et al. Reference Demjaha, Morgan, Morgan, Landau, Dean, Reichenberg, Sham, Fearon, Hutchington, Jones, Murray and Dazzan2009).
Follow-up
Cases were followed up 10 years after first contact with services in ÆSOP-10 (Morgan et al. Reference Morgan, Lappin, Heslin, Donoghue, Lomas, Reininghaus, Onyejiaka, Croudace, Jones, Murray, Fearon, Doody and Dazzan2014). The World Health Organization Life Chart (Susser et al. Reference Susser, Finnerty, Mojtabai, Yale, Conover, Goetz and Amador2000; Harrison et al. Reference Harrison, Hopper, Craig, Laska, Siegel, Wanderling, Dube, Ganey, Giel, an der Heiden, Holmberg, Janca, Lee, Leon, Malhotra, Marsella, Nakane, Sartorius, Shen, Skoda, Thara, Tsirkin, Varma, Walsh and Wiersma2001) was completed for each case using case notes and clinical interview where possible, to map course of illness and symptom history. The SCAN was also completed in relation to the preceding month where possible. Lifetime diagnosis (based on information from baseline to follow-up) using a consensus approach was based on all this clinical information, and blind to ethnicity and baseline diagnoses.
Ethical approval was granted by the Institute of Psychiatry and South London and Maudsley (SLaM) Research Ethics Committee and by the North Nottingham Healthcare NHS Trust Ethics Committee.
Analyses
Data were analysed using STATA 10 (StataCorp, 2009). Differences between followed-up and not-followed-up cases were analysed using χ2 and Wilcoxon rank-sum tests as appropriate. Prospective and retrospective consistencies were calculated as the percentage of cases with the same diagnosis at follow-up as at baseline, and the percentage of cases with the same diagnosis at baseline as at follow-up, respectively.
Predictors of diagnostic change were assessed in two steps: unadjusted univariate logistic regression analyses; and models of independent predictors. Models of independent predictors were built by starting with a single variable and adding in additional variables, one at a time to examine their effect on the model. Only variables with p < 0.1 in the unadjusted analyses were entered into the adjusted regression model starting with the variable with the biggest effect. Each additional variable was then added to the model in turn using likelihood ratio tests to determine if that variable significantly improved the model or not. Variables that did not improve the model were excluded from the model. Predictors were simplified into binary factors where possible in order to simplify analyses and increase power. As well as analysing age as a continuous variable, it was reclassified into a binary variable (in the age risk period: males under the age of 40 years or females under the age of 50 years) as this has been indicated as an important predictor in the development of schizophrenia (Häfner et al. Reference Häfner, Hambrecht, Löffler, Munk-Jørgensen and Riecher-Rössler1998).
Results
Sample
At baseline, a total of 557 first-episode psychosis cases were identified. Data here are based on the incidence sample collected over the first 2 years (excluding: non-incidence cases collected for the brain imaging component of the study; cases oversampled in the third year in order to increase the numbers for the ethnicity component of the study; and cases excluded post-baseline). This led to a total number of 505 cases: 304 from London and 201 from Nottingham.
Of the 505 patients eligible for follow-up, 79.8% (403) had sufficient information to make a lifetime diagnosis based on at least 8 years of information (including 33 cases who had died during the follow-up period but had sufficient information to have a lifetime diagnosis made). Therefore, a total of 102 cases had no follow-up diagnostic information. The mean follow-up in years of those who had a lifetime diagnosis and were still alive was 10.74 years (s.d. = 1.17, range 8.08–13.70).
Table 1 shows the differences in demographic and clinical variables between those with and without a diagnosis at 8 or more years. Centre and place of birth were associated with lifetime diagnosis status. Cases who were born abroad were more likely to move abroad over the follow-up period than cases born in the UK and therefore less likely to be followed up. More cases from London were not born in the UK (38%, 112/297) compared with Nottingham (9%, 18/201; p < 0.01), and so a lower lifetime diagnosis rate in London could be linked to place of birth.
df, Degrees of freedom; NOS, not otherwise specified; IQR, interquartile range; DUP, duration of undiagnosed psychosis.
Diagnostic change: prospective and retrospective consistency
Of cases, 59.6% (240/403) had the same baseline and lifetime ICD diagnosis, and 55.3% (223/403) of cases had the same baseline and lifetime DSM diagnosis. A substantial proportion of patients had a baseline and lifetime diagnosis of schizophrenia in both the ICD (33%) and DSM (28%) (Tables 2 and 3). The DSM system produced four cases with a baseline or lifetime diagnosis of either ‘unknown’ or ‘other’. This was due to the fact that although there was a large amount of information for 8 or more years, the diagnostic team was unable to agree upon a diagnosis.
ICD, International Classification of Diseases; NOS, not otherwise specified.
DSM, Diagnostic and Statistical Manual of Mental Disorders; NOS, not otherwise specified.
Table 4 presents the prospective and retrospective consistency of the ICD-10 and DSM-IV-TR. The DSM and ICD had very similar prospective consistencies for most diagnoses, with schizophrenia, psychotic bipolar disorder and drug-induced psychosis having the highest prospective consistency. In terms of retrospective consistency, schizophrenia diagnosed using the DSM had almost 10% lower consistency than schizophrenia diagnosed using the ICD. This difference is accounted for by the use of schizophreniform disorder in the DSM but not in the ICD. Drug-induced psychosis had a marginally higher prospective consistency compared with schizophrenia when using both the ICD and DSM. There were more cases at follow-up than at baseline with the following diagnoses: schizophrenia, schizo-affective disorder, bipolar disorder and drug-induced psychosis.
DSM, Diagnostic and Statistical Manual of Mental Disorders; ICD, International Classification of Diseases; NOS, not otherwise specified.
Predictors of change
The unadjusted regression analyses for key baseline demographic, clinical and social variables revealed that five baseline variables were associated with change in ICD diagnosis (see online Supplementary Appendix S1 for full details). Likelihood ratio tests revealed that the variables which together created the most parsimonious model associated with change were: having a diagnosis of delusional disorder [odds ratio (OR) 23.42, 95% confidence interval (CI) 4.15–132.03], acute and transient psychosis (OR 73.84, 95% CI 8.52–639.80), schizo-affective disorder (OR 9.00, 95% CI 2.33–34.71) or psychosis not otherwise specified (NOS) (OR 12.74, 95% CI 2.24–72.39); being from London (Nottingham: OR 0.50, 95% CI 0.25–1.04); and having depressive symptoms (OR 1.92, 95% CI 1.11–3.32).
Eight baseline variables were associated with change in DSM diagnosis in the unadjusted analyses. Likelihood ratio tests revealed that the variables which together created the most parsimonious model of change were: having a diagnosis of psychotic major depression (OR 2.54, 95% CI 0.87–7.41), schizo-affective disorder (OR 12.21, 95% CI 2.16–69.00), delusional disorder (OR 40.02, 95% CI 6.39–250.73), psychosis NOS (OR 22.95, 95% CI 3.88–135.76) and brief psychotic disorder (OR 39.38, 95% CI 3.53–439.13); being from London (Nottingham: OR 0.46, 95% CI 0.22–0.98); having a lower age at onset (OR 0.17, 95% CI 0.05–0.54); having contact with friends (less than weekly contact with friends: OR 0.34, 95% CI 0.13–0.90); and having depressive symptoms (OR 2.35, 95% CI 1.30–4.26).
Predictors of change to schizophrenia
Considering the high number of cases moving to a diagnosis of schizophrenia over the follow-up period and the implied increase in need this may engender (Carr et al. Reference Carr, Lewin, Neil, Halpin and Holmes2004), a separate analysis of predictors of change to a diagnosis of schizophrenia was undertaken. This is shown in Table 5. For the ICD analyses, all diagnoses were used. However, given the overlap between DSM-IV-TR schizophreniform psychosis and schizophrenia, schizophreniform cases were excluded from the DSM analysis.
ICD, International Classification of Diseases; DSM, Diagnostic and Statistical Manual of Mental Disorders; OR, odds ratio; CI, confidence interval; NOS, not otherwise specified; DUP, duration of undiagnosed psychosis.
* p < 0.1, ** p < 0.05.
The unadjusted analyses revealed that many more variables were associated with ICD and DSM diagnosis change to schizophrenia. For the ICD, there was some evidence that 14 baseline variables were associated with a change to schizophrenia. There was strong evidence that the following were associated with change to schizophrenia: being from London (Nottingham OR 0.31, 95% CI 0.16–0.58); being in the age risk period (OR 3.43, 95% CI 1.16–10.14); being black African (OR 3.03, 95% CI 1.25–7.35); longer duration of undiagnosed psychosis (DUP) (OR 1.16, 95% CI 0.99–1.35); having symptoms of reality distortion (OR 1.73, 95% CI 1.07–2.81); having negative symptoms (OR 1.84, 95% CI 1.15–2.93); living along (not living alone OR 0.49, 95% CI 0.26–0.89); being single (not single OR 0.27, 95% CI 0.12–0.59); and having contact with friends less than weekly (OR 4.49, 95% CI 1.54–13.05).
There was strong evidence that the following baseline variables were associated with not changing diagnosis to schizophrenia: having a diagnosis of bipolar disorder (OR 0.04, 95% CI 0.01–0.21) or drug-induced psychoses (OR 0.19, 95% CI 0.05–0.80); and having manic symptoms (OR 0.35, 95% CI 0.21–0.57).
There was some weak evidence that the following were associated with changing to a diagnosis of schizophrenia: being male (female OR 0.57, 95% CI 0.31–1.03); having psychotic major depression (OR 0.43, 95% CI 0.17–1.12); being unemployed (other OR 0.55, 95% CI 0.28–1.06); and not being in further education (further education OR 0.52, 95% CI 0.25–1.11).
For the DSM, there was some evidence that 13 baseline variables were associated with a change to schizophrenia. There was strong evidence that the following were associated with change to schizophrenia: being from London (Nottingham OR 0.34, 95% CI 0.18–0.65); being male (female OR 0.50, 95% CI 0.27–0.92); being in the age risk period (OR 3.46, 95% CI 1.17–10.24); being black African (OR 2.77, 95% CI 1.15–6.65); having a diagnosis of delusional disorder (OR 4.44, 95% CI 0.94–21.00); having symptoms of reality distortion (OR 1.77, 95% CI 1.08–2.91); having negative symptoms (OR 1.77, 95% CI 1.10–2.87); living alone (not living alone OR 0.47, 95% CI 0.25–0.87); being single (not being single OR 0.28, 95% CI 0.13–0.61); not being in further education (further education OR 0.46, 95% CI 0.21–0.99); and having contact with friends less than weekly (OR 3.50, 95% CI 1.24–9.85).
There was strong evidence that the following were associated with not changing diagnosis: having a diagnosis of bipolar disorder (OR 0.13, 95% CI 0.02–0.85); and having manic symptoms (OR 0.37, 95% CI 0.23–0.60). There was some weak evidence that longer DUP was associated with changing diagnosis (OR 1.14, 95% CI 0.98–1.33). For both the ICD and DSM, the numbers were too small to perform multivariate analyses.
Discussion
The prospective consistencies of both diagnostic systems were comparable at 55–60%. Few demographic, clinical and social factors were associated with overall change in diagnosis but many factors were associated with change to schizophrenia in both DSM and ICD analyses. However, low numbers did not allow for multivariate analysis of variables associated with change to schizophrenia.
Strengths and limitations
As with most cohort studies, loss to follow-up is a potential bias. Not all incident cases could be given a lifetime diagnosis. However, there was no difference in the proportions followed up between the diagnoses and the overall prevalence of follow-up was respectable at 80%. A further limitation was that missing data in the predictors of change analysis limited the power of the analyses. Despite these limitations, this study contributes evidence beyond previous research because of the incidence sample and 10-year follow-up using both the ICD and DSM diagnoses. Furthermore, it is based on consensus diagnoses made blind to ethnicity and baseline diagnoses and is the first study to examine so many potential predictors of diagnostic change across a range of domains (demographic, clinical and social).
Findings and implications
An important finding was that schizophrenia, schizo-affective disorder, bipolar disorder and drug-induced psychosis had higher numbers at follow-up, indicating a tendency for other diagnoses to migrate to these categories. This means that the incidence of these diagnoses may be underestimated in incidence studies and this may confuse the aetiological picture.
The prospective consistencies for schizophrenia, bipolar disorder and drug-induced psychosis were significantly higher than the overall stability (>70%). The high stability of drug-induced psychosis is surprising. This category represents a specific subgroup of individuals who demonstrate a clear temporal relationship between onset and recovery of psychotic symptoms and substance use. Rates of co-morbid substance misuse are significant in first-episode psychosis cohorts at around 30–50% (Cantwell et al. Reference Cantwell, Brewin, Glazebrook, Dalkin, Fox, Medley and Harrison1999; Van Mastrigt et al. Reference Van Mastrigt, Addington and Addington1999; Barnett et al. Reference Barnett, Werners, Secher, Hill, Brazil, Masson, Pernet, Kirkbride, Murray, Bullmore and Jones2007), whereas drug-induced psychosis often represents less than 10% of a first-episode psychosis cohort (Whitty et al. Reference Whitty, Clarke, McTigue, Browne, Kamali, Larkin and O'Callaghan2005; Addington et al. Reference Addington, Chaves and Addington2006; Bromet et al. Reference Bromet, Kotov, Fochmann, Carlson, Tanenberg-Karant, Ruggero and Chang2011). This suggests that often drug use is considered by assessors to be co-morbid rather than a sole cause of first-episode psychosis but that where it is identified to be the sole cause, this is often correct.
Depressive psychosis shows lower prospective consistency (45–50%). This might be expected given the anticipation that a substantial percentage of cases will develop bipolar affective disorder over time. However, approximately twice as many cases eventually receive a diagnosis of schizophrenia compared with bipolar disorder. Previous literature is consistent with this finding where consensus diagnosis was used over long periods of follow-up (Bromet et al. Reference Bromet, Kotov, Fochmann, Carlson, Tanenberg-Karant, Ruggero and Chang2011). It is well recognized that there are prominent symptoms of both anxiety and depression in both prodromal and early psychosis (Birchwood et al. Reference Birchwood, Iqbal, Chadwick and Trower2000) and this is further useful to clinicians considering treatment and prognosis.
The minimal crossover between the bipolar and schizophrenia categories illustrated in the movement matrix is further supported by the finding that a diagnosis of bipolar disorder is associated with reduced odds of changing diagnosis to schizophrenia over time. This taken with the propensity of depressive psychosis cases to change to schizophrenia suggests a complicated relationship between affective and ‘so-called’ non-affective psychosis.
The prospective and retrospective consistencies of the remaining categories were poor (<40%; with the exception of retrospective consistency for delusional disorder). Schizophreniform psychosis greatly overlaps with schizophrenia (duration of symptoms being the only difference) and explains the lower retrospective consistency of the DSM-IV-TR schizophrenia category, perhaps suggesting that it is an unnecessary extra category. Delusional disorder has significantly higher retrospective consistency (50–66%), suggesting less crossover than the other unstable categories. The movement matrix showed more than half of cases with delusional disorder at baseline eventually receive a diagnosis of schizophrenia, and the ICD analysis revealed it is associated with changing diagnosis to schizophrenia. Given this, it may best be considered an attenuated form of schizophrenia.
Examination of the remaining categories in light of their instability – schizo-affective disorder, acute/brief psychosis and psychosis NOS – reveal no immediately obvious patterns or utility in terms of describing a course of symptoms. These categories represent approximately 15% of our sample (ICD 68 cases at baseline, 77 cases at follow-up; DSM-IV 64 cases at baseline, 63 cases at follow-up). This suggests that as well as lacking aetiologically driven diagnoses in psychiatry, for a significant minority of our patients we still lack an adequate descriptive framework, a challenge for new and future revisions of current classification systems.
Change to diagnosis of schizophrenia
While few characteristics were associated with diagnostic change in general, many factors were associated with change to schizophrenia in both DSM and ICD analyses. Perhaps unsurprisingly, these included variables associated with schizophrenia: symptoms of reality distortion, negative symptoms, and variables indicative of social isolation: living alone, being single and having contact with friends less than weekly. However, low numbers did not allow for multivariate analysis of variables associated with change to schizophrenia. This is in line with previous research that has reported negative symptoms (Mason et al. Reference Mason, Harrison, Croudace, Glazebrook and Medley1997) to be associated with a change in diagnosis to schizophrenia. The finding that social isolation (as measured by contact with friends) was associated with change to schizophrenia may be associated with negative symptoms, as less contact with friends could stem from negative symptoms, and lead to isolation (Schwartz et al. Reference Schwartz, Fennig, Tanenberg-Karant, Carlson, Craig, Galambos, Lavelle and Bromet2000).
Conceptual considerations
The findings from this and other studies on diagnostic stability raise two salient issues. The first is validity: there is an implicit assumption in papers on diagnosis that patients exhibiting stable diagnoses will demonstrate the same as-yet undiscovered physiological abnormalities. The finding that a number of diagnoses change over time is assumed to mean that the initial diagnosis was incorrect and thus the diagnostic systems are flawed, hence research into the causes of these conditions will be hampered. However, in the context of wider medicine, it is a common occurrence for diagnosis to change over time as a disorder develops, or as the clinical picture emerges. It is common that an acute condition precedes a chronic condition, for example, demyelination and multiple sclerosis. In this case, even information on aetiology and mechanism do not indicate outcome, as the mechanism for chronicity is separate. After an initial episode of this neuro-inflammatory disorder, there is little certainty as to prognosis – some people never relapse, for others further episodes occur and the diagnosis becomes multiple sclerosis (McDonald & Compston, Reference McDonald and Compston2001). That acute cases of demyelination reoccur and can lead to a diagnosis of multiple sclerosis does not undermine the usefulness of this diagnosis.
This brings us to the second issue of clinical utility. It can be argued that diagnosis informs clinical management of the patient and is therefore useful. However, these results indicate that changes in diagnosis that would probably result in a change of management (e.g. from schizophrenia to bipolar disorder) are minimal, and the changes that do occur are less likely to result in a substantial change in management (e.g. delusional disorder to schizophrenia). Therefore, it could be argued that diagnosis is of little clinical relevance, and specific symptom change is the important thing to be aware of. However, knowledge of how these diagnoses might change over time may prove clinically useful for both doctors and patients in understanding prognosis early in the course of an illness, and, as ever, in quickly communicating the nature of a cluster of symptoms between clinicians.
This raises the question of whether we should be ignoring diagnosis, giving no prognosis to patients and families, and be treating based on symptoms rather than diagnosis. In some early intervention practices, it is now commonplace to assign a broad clinical diagnosis of psychosis early in the course of illness. This avoids using stigmatizing terms such as schizophrenia with its association with poor outcome, promoting the recovery model, and being optimistic about outcomes. It also acknowledges what we have demonstrated in the current study: early on in the course of psychotic illness, the precise diagnosis is often provisional. However, previous research suggests that diagnosis is very strongly associated with outcome (Hegarty et al. Reference Hegarty, Baldessarini, Tohen, Waternaux and Oepen1994), and thus not to share this with patients and their families could be unethical. Perhaps a better approach would be to acknowledge the provisional nature of initial diagnosis and be cautious in making inferences regarding prognosis based on diagnosis, as it may not reflect the long-term picture, and to be vigilant for changes in the clinical picture.
The stability of the current classification systems varies widely between diagnoses. Schizophrenia, bipolar disorder, drug-induced psychosis, delusional disorder and depressive psychosis all show relative stability and consistent patterns of change where change does occur. The findings on diagnostic change in depressive and bipolar cases poses a challenge to the distinction of affective/non-affective categories. Psychosis NOS, schizo-affective disorder and acute/brief psychosis perform poorly, yet still provide the best-fit diagnosis for 15% of our cohort, posing a significant challenge in the revision of these categories.
Supplementary material
For supplementary material accompanying this paper visit http://dx.doi.org/10.1017/S0033291715000720
Acknowledgements
This work was supported by the UK Medical Research Council (reference G0500817) and the Department of Health through the National Institute for Health Research (NIHR) Specialist Biomedical Research Centre for Mental Health award to the SLaM NHS Foundation Trust and the Institute of Psychiatry at King's College London.
Declaration of Interest
R.M.M. has received speaker honoraria from Janssen, Astra-Zeneca, Lilly, BMS and Roche. P.B.J. is a member of scientific advisory boards for Roche and Otsuke. The other authors have nothing to disclose.