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Early intervention in psychotic disorders: faith before facts?

Published online by Cambridge University Press:  02 July 2009

P. Bosanac
Affiliation:
The University of Melbourne, Melbourne, Australia
G. C. Patton
Affiliation:
Centre for Adolescent Health, Royal Children's Hospital; Murdoch Childrens Research Institute; and Department of Paediatrics, The University of Melbourne, Melbourne, Australia
D. J. Castle*
Affiliation:
St Vincent's Health and The University of Melbourne, Melbourne, Australia
*
*Address for correspondence: Professor D. J. Castle, Chair of Psychiatry, St Vincent's Health and The University of Melbourne, Level 2, 46 Nicholson Street, Fitzroy, Victoria 3065, Australia. (Email: david.castle@svhm.org.au)
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Abstract

This paper reviews the literature on early intervention in psychotic disorders, weighs the cons of this approach, and makes suggestions for clinicians and researchers regarding how to interpret and respond to what is still an embryonic evidence-base, notably in terms of any long-term benefits.

Type
Editorial
Copyright
Copyright © Cambridge University Press 2009

Introduction

One of the most striking developments in psychiatric services in the past decade has been the establishment of early intervention programmes for psychotic disorders around the world (McGorry et al. Reference McGorry, Killackey and Yung2007; McGorry, Reference McGorry2009). The attractiveness of these models of care is clear. For a group of disorders where there has been a pessimistic view of outcome, early intervention strategies offer patients, families and clinicians a more optimistic view of the future. One major aim in early intervention is to reduce the duration of untreated illness (DUP) by engaging affected individuals and their carers in flexible models of non-stigmatizing and minimally traumatic care, which in turn enhance recovery. The focus on recovery and relapse prevention involves intense individual, group and family psychological interventions appropriate to the individual, along with addressing psychiatric and substance abuse co-morbidities (Yung et al. Reference Yung, Phillips, Drew, McGorry and Jackson1999) and the judicious use of psychotropic medication (Drake & Lewis, Reference Drake, Lewis, Castle, Coplov, Wykes and Mueser2008). Yet there is still limited research into the effectiveness of such programmes, particularly around longer-term outcomes (Craig, Reference Craig2003), and overall the concept continues to fuel academic debate (e.g. McGorry, Reference McGorry2009; Pelosi, Reference Pelosi2009). Indeed, criticism has also emerged around the potential for ‘overmedicalizing’ problems. For health services policy, the development of early psychosis strategies raises important questions about where best to invest limited funds for psychiatric services and how to integrate early psychosis initiatives into broader services.

‘Caseness’ in early psychosis

Current targets for early psychosis are broad. They encompass the at-risk mental state (ARMS), which may extend to 5 years prior to the onset of frank psychosis; the first episode that satisfies threshold criteria for syndromal classification; and the ensuing early and late recovery phases in the first year after acute treatment (McGorry et al. Reference McGorry, Killackey and Yung2007). There are, however, considerable challenges in defining a ‘case’ for intervention. Even in those with clear-cut psychosis, definitive diagnosis is difficult. Schizophrenia is followed by bipolar and major depressive disorder with psychotic features in having the highest prospective diagnostic consistency over a 2-year period (Subramaniam et al. Reference Subramaniam, Pek, Verma, Chan and Chong2007). Criteria B and C of DSM-IV-TR (APA, 2000) preclude the diagnosis of schizophrenia close to onset and potentially skew early intervention to other psychotic disorders that are by their nature more transient and more amenable to intervention (McGlashan, Reference McGlashan2007). This is perhaps linked to a trend in the early psychosis literature to ‘Kraepelin bashing’, taking the father of dementia praecox to task for being overly negative about the outcomes of the disorder. Yet Kraepelin's delineation of dementia praecox was of an early onset, male predominant, severe illness with a poor longitudinal trajectory (Murray et al. Reference Murray, O'Callaghan, Castle and Lewis1992); this is only one subgroup in what ICD-10 and DSM-IV-TR call ‘schizophrenia’. Equating the two diagnostic constructs is misleading.

A ‘transdiagnostic’ approach to first-episode psychosis, with its inherent limitations in validity and reliability, affects the generalizability of outcome studies as the natural history of different disorders varies (Ketter et al. Reference Ketter, Wang, Becker, Nowakowska and Yang2003). For this reason phenomenological approaches to early schizophrenia that encompass altered subjective experiences, rather than relying entirely on syndromal diagnosis (as inherent in DSM-IV-TR and ICD-10), are emerging as attractive areas for further study (Parnas, Reference Parnas2005). However, this approach is limited by the high prevalence and low predictive power of psychotic experiences in the general population. Only a minority of these individuals can be considered to have a treatable ‘disorder’ (Konings et al. Reference Konings, Bak, Hanssen, van Os and Krabbendam2006).

The DUP conundrum

A recent consensus statement for gauging the effectiveness of early intervention programmes included the following objectives: reduction in DUP to <3 months; suicide rates <1% within the first 2 years from diagnosis; employment and education rates matched to non-affected peers at 5 years; reported satisfaction in these domains; and social attainment occurring in ⩽90% of affected people (Bertolote & McGorry, Reference Bertolote and McGorry2005). To what extent is such a desire supported by the available literature?

Reduction in DUP has been widely adopted as a surrogate for better clinical outcomes. Yet there are many difficulties in this approach. The accurate measurement of DUP in a disorder that often has its origins in early neurodevelopmental aberration and that carries disability, for some individuals, from very early in life is arbitrary (Jones et al. Reference Jones, Rodgers, Murray and Marmot1994). As Häfner et al. (Reference Häfner, Riecher-Rossler, Hambrecht, Maurer, Meissner, Schmidtke, Fatkenheuer, Loffler and van der Heiden1992) have shown, the prodrome of schizophrenia is commonly non-specific, with prominent mood and negative rather than positive psychotic symptoms. Attempts at refining the ‘ultra-high-risk’ mental state has not helped clinicians much in that most of those who transition to psychosis do so fairly early after detection. The transition rate is strongly dependent upon the base rate of psychosis in the sample population, making the predictive value very poor in general population or routine clinical samples (Yung et al. Reference Yung, Stanford, Cosgrave, Killackey, Phillips, Nelson and McGorry2006). Even in highly enriched samples the positive predictive value seems to be low, with around 10% making a transition within 6 months of first assessment (Yung et al. Reference Yung, Stanford, Cosgrave, Killackey, Phillips, Nelson and McGorry2006). Furthermore, the greater the need to define smaller ultra-high-risk groups to achieve sufficient predictive power within the clinic, the smaller the effect is likely to be on preventing transition to psychosis, as the majority of those potentially at risk will not be identified for clinic attendance (see Rose, Reference Rose1992).

There are also challenges in the identification of young people most at risk of the adverse outcomes of psychotic illness. It is clear that early detection strategies can recruit people with lower levels of symptomatology and less deteriorating social function than mainstream mental health services. Yet there is little evidence that they recruit a high proportion of patients with the worst prognosis, that is those with a prodrome of >2 years (Friis et al. Reference Friis, Vaglum, Haahr, Johannessen, Larsen, Melle, Opjordsmoen, Rund, Simonsen and McGlashan2005). Thus, it is possible that early detection is likely to identify individuals with an inherent tendency to better outcomes. For those who do progress to psychosis there are further difficulties. Given the high rate of non-transition, many will be exposed to antipsychotic medications, which carry their own risks and side-effects, in addition to the potential stigmatizing effects of being identified as ‘at risk’.

The extent to which DUP independently predicts outcomes remains a problem, as the onset for the most severe illnesses may be insidious, with flattened affectual responses and impaired social functioning being the early features (Morgan et al. Reference Morgan, Abdul-Al, Lappin, Jones, Fearon, Leese, Croudace, Morgan, Dazzan, Craig, Leff and Murray2006). Whether early intervention programmes have a greater impact on DUP in this group of patients than usual mental health services is questionable.

Finally, despite reports of associations between DUP and clinical and functional outcomes (Norman et al. Reference Norman, Lewis and Marshall2005; Perkins et al. Reference Perkins, Gu, Boteva and Lieberman2005), the impact of reduced DUP on longer-term outcomes is equivocal, and the mechanism whereby such an effect might be mediated is open to conjecture (Marshall et al. Reference Marshall, Lewis, Lockwood, Drake, Jones and Croudace2005). One suggested mechanism is that clinical interventions are ‘neuroprotective’. This term has been applied to interventions that may reduce the loss of, or promulgate, glial or neuronal progenitor cells that otherwise would have been affected during the transition to psychotic illness such as schizophrenia (Berger et al. Reference Berger, Wood and McGorry2003). Early and late neurodevelopmental processes, with the latter occurring during the transition to illness, have been implicated in schizophrenia. The evidence for late neurodevelopmental changes comes from progressive magnetic resonance imaging (MRI) changes, particularly in the prefrontal and medial temporal regions, of people at ultra-high risk of developing schizophrenia, and increased prefrontal grey matter loss in first-episode psychosis patients compared with normal controls (Pantelis et al. Reference Pantelis, Velakoulis, Wood, Yucel, Yung, Phillips, Sun and McGorry2007). However, other studies have not found an association between DUP and brain volume, including in the hippocampi (Ho et al. Reference Ho, Alicata, Carmencita and Andreasen2005). At this juncture, the aetiology of late neurodevelopmental changes is speculative (Pantelis et al. Reference Pantelis, Velakoulis, Wood, Yucel, Yung, Phillips, Sun and McGorry2007), as is the scope for interventions that ameliorate such changes with associated clinical benefit.

Longer-term outcomes

Developmentally appropriate and accessible models of care (McGorry, Reference McGorry2002) and the development of clinical staging (McGorry, Reference McGorry2007) have been proposed as important elements of optimal care in early psychosis, but the evaluation of these interventions in randomized controlled trials is difficult. The challenges include defining an appropriate ‘control’ condition; statistical power; and operationalizing experimental and control interventions. The OPUS trial in Denmark and the Lambeth Early Onset (LEO) study in London (Craig et al. Reference Craig, Garety, Power, Rahaman, Colbert, Fornells-Ambrojo and Dunn2004) both compared specialist early psychosis interventions with ‘usual care’. The OPUS study recruited people aged 18 to 45 years with ICD-10 (WHO, 1993) schizophrenia or related disorders who had not been on continuous antipsychotic medication for more than 12 weeks. In that study, there were short-term benefits for the intervention group in terms of independent living and homelessness; improved psychotic symptoms; lower levels of substance abuse; and better global functioning at 2 years follow-up. However, as Patton et al. (Reference Patton, Hetrick and McGorry2007) point out, outcome measurements were not blinded and there was high attrition that might well have biased outcomes. Furthermore, and more importantly to the current discourse, benefits on positive and negative symptoms of schizophrenia, global functioning, secondary substance use and antipsychotic were not sustained at the 5-year follow-up (Bertelsen et al. Reference Bertelsen, Jeppesen, Petersen, Thorup, Ohlenschlaeger, Quach, Christensen, Krarup, Jorgensen and Nordentoft2008). Participants in the LEO study were aged 16–40 years, and had presented to mental health services for the first or second time (the latter having disengaged without treatment after presenting once) with ICD-10 non-affective psychoses and the absence of organic psychosis or primarily substance addiction. Beneficial 12- and 18-month outcomes were found for the specialist intervention in global functioning, hospitalization rates, and vocational and social parameters (Garety et al. Reference Garety, Craig, Dunn, Fornells-Ambrojo, Colbert, Rahaman, Read and Power2006). However, controlling for differences in baseline parameters such as previous psychotic episodes and ethnicity obviated the advantage in terms of relapse rates (Patton et al. Reference Patton, Hetrick and McGorry2007). At 5 years follow-up any benefit in terms of reduced hospital use had disappeared (Gafoor et al. Reference Gafoor, Craig, Garety, Power and McGuire2008). In an earlier 9-month comparison of an assertive outreach model of care and treatment as usual for people who had first service contact for a psychotic disorder within the preceding 5 years, Kuipers et al. (Reference Kuipers, Holloway, Rabe-Hesketh and Tennakoon2004) found there were no significant differences on measures of psychopathology, quality of life and overall functioning. Thus, it seems that short-term benefits of early psychosis interventions are not consistently translating into longer-term gains.

A further challenge lies in determining which elements of early intervention programmes have any effect. Most studies have used multifaceted interventions with little possibility of disaggregating the elements. It seems that cognitively orientated psychological interventions have a significant role in the management of early psychotic disorders, but further empirical study of their type and utility in terms of illness phase and cost-effectiveness is necessary (Haddock & Lewis, Reference Haddock and Lewis2005). Similarly, family interventions, including combination with cognitive behavioural therapy, require further evaluation of their effectiveness in this population (Lewis et al. Reference Lewis, Tarrier and Drake2005), as do comprehensive and group interventions (Penn et al. Reference Penn, Waldheter, Perkins, Mueser and Lieberman2005). There is preliminary evidence that vocational interventions, centred on individual placement and support, may confer better employment outcome at 6 months than treatment as usual, in early psychotic disorders (Killackey et al. Reference Killackey, Jackson and McGorry2008), but the impact on longer-term vocational functioning is not known, and in any event, such interventions may be effective in the short term at any stage of illness (McGurk et al. Reference McGurk, Twamley, Sitzer, McHugo and Mueser2007).

A reduction in suicide rates is a worthy aim of early psychosis services, yet again the evidence that they are effective in this regard, expressly over longer time intervals, is limited. Suicidal plans and attempts in early psychosis are linked with suicidal ideation, psychotic and depressive symptomatology and are thus potentially amenable to early clinical intervention (Melle et al. Reference Melle, Johannesen, Friis, Haahr, Joa, Larsen, Opjordsmoen, Rund, Simonsen, Vaglum and McGlashan2006; Bertelsen et al. Reference Bertelsen, Jeppesen, Petersen, Thorup, Ohlenschlaeger, Quach, Christensen, Krarup, Jorgensen and Nordentoft2007). A retrospective, population-based study of people who had contact with specialized mental health services for early psychotic disorders found that the suicide rate was half that of those with similar disorders without specialized intervention over the initial 3 years, but the risk was not diminished beyond this and up to a period of 8.5 years (Harris et al. Reference Harris, Burgess, Chant, Pirkis and McGorry2008). In addition, observational studies of this type suffer from the problem of ‘zero time shift’, such that the simple fact that the intervention is at an earlier stage of illness makes outcomes appear more favourable (Sackett et al. Reference Sackett, Haynes, Guyatt and Tugwell1991).

The problem of labelling, and potential treatment-related harm

Another set of issues is the ethical considerations of early intervention such as stigma and avoiding iatrogenic harms, particularly in intervention during a pre-psychotic phase (McGlashan, Reference McGlashan2005). In a study of comparative attitudes about early intervention in psychotic disorders, young people and their parents were found to be more likely than clinicians to favour informal social support, generic counselling and stress reduction over seeking help from psychiatrists, mental health services and antipsychotic medication (Jorm et al. Reference Jorm, Morgan and Wright2008). Although these findings may not seem surprising, they may represent both an impediment to accessing help and treatment adherence and an opportunity for improving mental health literacy. However, the labelling of young people as ‘mentally ill’, an inevitable consequence of engagement with clinical services, is potentially damaging in terms of personal and family stigma, and pathologizes what might be normal developmental processes.

Despite reported clinical benefits in controlled studies of antipsychotic medications in the ARMS, including olanzapine versus placebo for symptoms over 8 weeks (Woods et al. Reference Woods, Brier, Zipursky, Perkins, Addington, Miller, Hawkins, Marquez, Lindborg, Tohen and McGlashan2003), and risperidone and cognitive therapy versus supportive case management for progression to psychosis over 6 months (McGorry et al. Reference McGorry, Phillips, Yung, Francey, Germano, Bravin, MacDonald, Hearn, Amminger and O'Dwyer2002), the unequivocal clinical benefit of antipsychotic medication in the ARMS has not been demonstrated (Remington, Reference Remington2005). In addition, the superior clinical response of antipsychotics in early psychotic disorders (Perkins et al. Reference Perkins, Gu, Boteva and Lieberman2005) compared with later illness is counterbalanced by the limitations of diagnostic specificity and sensitivity of this temporal phase, greater sensitivity to side-effects, and ongoing increased risk of relapse potentially heightened by cessation of medication (Remington, Reference Remington2005). There is also the spectre of adverse sequelae of treatment with some antipsychotic medications, including psychotropic-related metabolic disturbance (including weight gain, hyperlipidaemia and diabetes), leading to potential early death (Buckley et al. Reference Buckley, Foster and Miller2008). Most recently, findings of an excess of sudden cardiac death associated with antipsychotics has led to caution being advocated about the over-liberal use of such drugs (Schneeweiss & Avorn, Reference Schneeweiss and Avorn2009).

Service delivery implications

Health service planners worldwide have accepted early intervention frameworks as core features of the psychiatric service system, even though there is no evidence for improvement in longer-term outcomes (discussed above). There is also the risk of diverting funding away from those with the most severe forms of illness who are still likely to require concerted ongoing comprehensive care well beyond the early years of illness (Harrison et al. Reference Harrison, Hopper, Craig, Laska, Siegel, Wanderling, Dube, Ganev, Giel, van der Heiden, Holmberg, Janca, Lee, Leon, Malhotra, Marsella, Nakane, Sartorius, Shen, Skoda, Thara, Tsirkin, Varma, Walsh and Wiersma2001). In addition, there is a difficulty that commitment to rolling out early intervention services on a large scale may make the conduct of further large-scale, longer-term studies infeasible in many countries in the future.

Specialized treatment plans for early psychosis patients are arguably no different to those that would be considered best practice by multidisciplinary psychiatry teams, and should be provided to all patients. Yet the creation of specialized early psychosis intervention programmes may disrupt the continuity of care by transfer back to referring mental health or primary care clinicians after a crucial or designated period of intervention (Pelosi, Reference Pelosi2009). The latter referral back to other mental health agencies following intensive, but finite, intervention in early schizophrenia is unlikely to be sufficient to maintain any early clinical and functional improvements (Linszen et al. Reference Linszen, Lenior, De Haan, Dingemans and Gersons1998).

Conclusions

In this review, we ask whether the early psychosis movement, however well-intentioned, has over-reached itself, setting dogma before evidence. Although it is likely that there are early clinical outcome benefits from early intervention for some individuals with psychotic disorders, the evidence that such benefits are sustained and meaningful in the longer term is equivocal. There is a lack of evidence that early interventions do much for those who have illnesses that are, from the outset, likely to have a poor longitudinal trajectory. Given both the low rates of transition to psychosis and the small proportion of psychosis cases that pass through ARMS clinics, it is difficult to justify this strategy outside of a research setting.

Clinicians and researchers might be better to concentrate their attention on advocating for the provision of better, fully integrated services for all people with psychotic disorders, irrespective of the stage of their illness. Such an approach would prevent the evolution of further silos within mental health services; avoid patients having to negotiate additional barriers such as transitioning from early psychosis to ‘general adult’ services; and prevent further erosion of the expertise of ‘generic’ services as skilled and well-intentioned clinicians succumb to the allure of boutique early psychosis services.

Declaration of Interest

None.

References

APA (2000). Diagnostic and Statistical Manual of Mental Disorders, 4th edn, text revision (DSM-IV-TR). American Psychiatric Association: Washington, DC.Google Scholar
Berger, GE, Wood, S, McGorry, PD (2003). Incipient neurovulnerability and neuroprotection in early psychosis. Psychopharmacology Bulletin 37, 79–101.Google ScholarPubMed
Bertelsen, M, Jeppesen, L, Petersen, L, Thorup, A, Ohlenschlaeger, P, Quach, PL, Christensen, TO, Krarup, G, Jorgensen, J, Nordentoft, M (2007). Suicidal behaviour and mortality in first-episode psychosis: the OPUS trial. British Journal of Psychiatry 191 (Suppl. 51), s140s146.CrossRefGoogle Scholar
Bertelsen, MT, Jeppesen, L, Petersen, A, Thorup, A, Ohlenschlaeger, P, Quach, PL, Christensen, TO, Krarup, G, Jorgensen, J, Nordentoft, M (2008). Five-year follow-up of a randomized multicenter trial of intensive early intervention vs standard treatment for patients with a first episode of psychotic illness. Archives of General Psychiatry 65, 762771.CrossRefGoogle ScholarPubMed
Bertolote, J, McGorry, P (2005). Early intervention and recovery for young people with early psychosis: consensus statement. British Journal of Psychiatry 187, s116s119.CrossRefGoogle Scholar
Buckley, PF, Foster, A, Miller, B (2008). Schizophrenia host vulnerability and risk of metabolic disturbances during treatment with antipsychotics. Focus 6, 172179.CrossRefGoogle Scholar
Craig, T (2003). A step too soon or a step too far? Early intervention in psychosis. Journal of Mental Health 12, 335339.CrossRefGoogle Scholar
Craig, TJ, Garety, P, Power, P, Rahaman, N, Colbert, S, Fornells-Ambrojo, M, Dunn, G (2004). The Lambeth Early Onset (LEO) Team: randomised controlled trial of the effectiveness of specialised care for early psychosis. British Medical Journal 329, 1067.CrossRefGoogle ScholarPubMed
Drake, R, Lewis, S (2008). A treatment approach to the patient with first episode schizophrenia. In Pharmacological and Psychosocial Treatments in Schizophrenia, 2nd edn (ed. Castle, D. J., Coplov, D. L., Wykes, T. and Mueser, K. T.), pp. 205219. Informa Healthcare: London.Google Scholar
Friis, S, Vaglum, P, Haahr, U, Johannessen, JO, Larsen, TK, Melle, I, Opjordsmoen, S, Rund, BR, Simonsen, E, McGlashan, T (2005). Effect of an early detection programme on duration of untreated psychosis. British Journal of Psychiatry 187, s29s32.CrossRefGoogle Scholar
Gafoor, R, Craig, T, Garety, P, Power, P, McGuire, P (2008). Do the benefits of early intervention (EI) treatments persist? 5-year follow-up. Schizophrenia Research 98, 8388.CrossRefGoogle Scholar
Garety, PA, Craig, TK, Dunn, G, Fornells-Ambrojo, M, Colbert, S, Rahaman, N, Read, J, Power, P (2006). Specialised care for early psychosis: symptoms, social functioning and patient satisfaction: randomised controlled trial. British Journal of Psychiatry 188, 3745.CrossRefGoogle ScholarPubMed
Haddock, G, Lewis, S (2005). Psychological interventions in early psychosis. Schizophrenia Bulletin 31, 697704.CrossRefGoogle ScholarPubMed
Häfner, H, Riecher-Rossler, A, Hambrecht, M, Maurer, K, Meissner, S, Schmidtke, A, Fatkenheuer, B, Loffler, W, van der Heiden, W (1992). IRAOS: an instrument for the retrospective assessment of the onset of schizophrenia. Schizophrenia Research 6, 209223.CrossRefGoogle Scholar
Harris, MG, Burgess, PM, Chant, DC, Pirkis, JE, McGorry, PD (2008). Impact of a specialized early psychosis treatment programme on suicide. Retrospective cohort study. Early Intervention in Psychiatry 2, 1121.CrossRefGoogle ScholarPubMed
Harrison, G, Hopper, K, Craig, T, Laska, E, Siegel, C, Wanderling, J, Dube, KC, Ganev, K, Giel, R, van der Heiden, W, Holmberg, SK, Janca, A, Lee, PWH, Leon, A, Malhotra, S, Marsella, AJ, Nakane, Y, Sartorius, N, Shen, Y, Skoda, C, Thara, R, Tsirkin, SJ, Varma, VK, Walsh, D, Wiersma, D (2001). Recovery from psychotic illness: a 15- and 25-year international follow-up study. British Journal of Psychiatry 178, 506517.CrossRefGoogle ScholarPubMed
Ho, B-C, Alicata, D, Carmencita, M, Andreasen, NC (2005). Hippocampus volume and treatment delays in first-episode schizophrenia. American Journal of Psychiatry 162, 15271529.CrossRefGoogle ScholarPubMed
Jones, P, Rodgers, B, Murray, R, Marmot, M (1994). Child developmental risk factors for adult schizophrenia in the British 1946 birth cohort. Lancet 344, 13981402.CrossRefGoogle ScholarPubMed
Jorm, AF, Morgan, AJ, Wright, A (2008). A comparison of clinician, youth, and parent beliefs about helpfulness of interventions for early psychosis. Psychiatric Services 59, 11151120.CrossRefGoogle ScholarPubMed
Ketter, TA, Wang, PW, Becker, OV, Nowakowska, C, Yang, Y (2003). Psychotic bipolar disorders: dimensionally similar to or categorically different from schizophrenia? Journal of Psychiatric Research 38, 4761.CrossRefGoogle Scholar
Killackey, E, Jackson, HJ, McGorry, PD (2008). Vocational intervention in first-episode psychosis: individual placement and support v. treatment as usual. British Journal of Psychiatry 193, 114120.CrossRefGoogle ScholarPubMed
Konings, M, Bak, M, Hanssen, M, van Os, J, Krabbendam, L (2006). Validity and reliability of the CAPE: a self-report instrument for the measurement of psychotic experiences in the general population. Acta Psychiatrica Scandinavica 114, 5561.CrossRefGoogle Scholar
Kuipers, E, Holloway, F, Rabe-Hesketh, S, Tennakoon, L (2004). An RCT of early intervention in psychosis: Croydon Outreach and Assertive Support Team (COAST). Social Psychiatry and Psychiatric Epidemiology 39, 358363.CrossRefGoogle ScholarPubMed
Lewis, S, Tarrier, N, Drake, RJ (2005). Integrating non-drug treatments in early schizophrenia. British Journal of Psychiatry 187, s65s71.CrossRefGoogle Scholar
Linszen, D, Lenior, M, De Haan, L, Dingemans, P, Gersons, P (1998). Early intervention, untreated psychosis and the course of early schizophrenia. British Journal of Psychiatry 172 (Suppl. 33), s84s89.CrossRefGoogle ScholarPubMed
Marshall, M, Lewis, S, Lockwood, A, Drake, R, Jones, P, Croudace, T (2005). Association between duration of untreated psychosis and outcome in cohorts of first-episode patients. Archives of General Psychiatry 62, 975983.CrossRefGoogle ScholarPubMed
McGlashan, TH (2005). Early detection and intervention in psychosis: an ethical paradigm shift. British Journal of Psychiatry 187, s113s115.CrossRefGoogle Scholar
McGlashan, TH (2007). The DSM-IV version of schizophrenia may be harmful to patients' health. Early Intervention in Psychiatry 1, 289293.CrossRefGoogle ScholarPubMed
McGorry, P (2002). The recognition and optimal management of early psychosis: an evidence-based reform. World Psychiatry 1, 7683.Google ScholarPubMed
McGorry, P (2007). Issues for DSM-V: clinical staging: a heuristic pathway to valid nosology and safer, more effective treatment in psychiatry. American Journal of Psychiatry 164, 859860.CrossRefGoogle ScholarPubMed
McGorry, P (2009). Is early intervention in the major psychiatric disorders justified? Yes. British Medical Journal 337, a695.CrossRefGoogle Scholar
McGorry, P, Killackey, E, Yung, AR (2007). Early intervention in psychotic disorders: detection and treatment of the first episode and the critical early stages. Medical Journal of Australia 187, s8–s10.CrossRefGoogle ScholarPubMed
McGorry, PD, Phillips, LJ, Yung, AR, Francey, S, Germano, D, Bravin, J, MacDonald, A, Hearn, N, Amminger, P, O'Dwyer, L (2002). A randomised controlled trial of interventions in the pre-psychotic phase of psychotic disorders. Archives of General Psychiatry 59, 921928.CrossRefGoogle Scholar
McGurk, SR, Twamley, EW, Sitzer, DI, McHugo, GJ, Mueser, KT (2007). A meta-analysis of cognitive remediation in schizophrenia. American Journal of Psychiatry 164, 17911802.CrossRefGoogle ScholarPubMed
Melle, I, Johannesen, JO, Friis, S, Haahr, U, Joa, I, Larsen, TK, Opjordsmoen, S, Rund, BR, Simonsen, E, Vaglum, R, McGlashan, T (2006). Early detection of the first episode of schizophrenia and suicidal behaviour. American Journal of Psychiatry 163, 800804.CrossRefGoogle Scholar
Morgan, C, Abdul-Al, R, Lappin, JM, Jones, P, Fearon, P, Leese, M, Croudace, T, Morgan, K, Dazzan, P, Craig, T, Leff, J, Murray, R (2006). Clinical and social determinants of duration of untreated psychosis in the ÆSOP first episode psychosis study. British Journal of Psychiatry 189, 446452.CrossRefGoogle ScholarPubMed
Murray, RM, O'Callaghan, E, Castle, DJ, Lewis, SW (1992). A neurodevelopmental approach to the classification of schizophrenia. Schizophrenia Bulletin 3, 319332.CrossRefGoogle Scholar
Norman, RM, Lewis, SW, Marshall, M (2005). Duration of untreated psychosis and its relationship to clinical outcome. British Journal of Psychiatry. Supplement 187, s19s23.CrossRefGoogle ScholarPubMed
Pantelis, C, Velakoulis, D, Wood, SJ, Yucel, M, Yung, AR, Phillips, LJ, Sun, DQ, McGorry, PD (2007). Neuroimaging and emerging psychotic disorders: the Melbourne ultra-high risk studies. International Review of Psychiatry 19, 71–381.CrossRefGoogle ScholarPubMed
Parnas, J (2005). Clinical detection of schizophrenia-prone individuals. British Journal of Psychiatry 187, s111s112.CrossRefGoogle Scholar
Patton, G, Hetrick, SE, McGorry, P (2007). Service responses for youth onset mental disorders. Current Opinion in Psychiatry 20, 319324.CrossRefGoogle ScholarPubMed
Pelosi, A (2009). Is early intervention in the major psychiatric disorders justified? No. British Medical Journal 337, a710.CrossRefGoogle Scholar
Penn, DL, Waldheter, EJ, Perkins, DO, Mueser, KT, Lieberman, JA (2005). Psychosocial treatment for first-episode psychosis: a research update. American Journal of Psychiatry 162, 22202232.CrossRefGoogle ScholarPubMed
Perkins, DO, Gu, H, Boteva, K, Lieberman, JA (2005). Relationship between duration of untreated psychosis and outcome in first-episode schizophrenia: a critical review and meta-analysis. American Journal of Psychiatry 162, 17851804.CrossRefGoogle ScholarPubMed
Remington, G (2005). Rational pharmacotherapy in early psychosis. British Journal of Psychiatry 187, s77s84.CrossRefGoogle Scholar
Rose, G (1992). The Strategy of Preventive Medicine. Oxford University Press: Oxford.Google Scholar
Sackett, DL, Haynes, RB, Guyatt, GH, Tugwell, P (1991). Clinical Epidemiology: A Basic Science for Clinical Medicine. Little Brown & Company: London.Google Scholar
Schneeweiss, S, Avorn, J (2009). Antipsychotic agents and sudden cardiac death: how should we manage the risk? New England Journal of Medicine 360, 294296.CrossRefGoogle ScholarPubMed
Subramaniam, M, Pek, E, Verma, S, Chan, YH, Chong, SA (2007). Diagnostic stability 2 years after treatment initiation in the Early Psychosis Intervention Programme in Singapore. Australian and New Zealand Journal of Psychiatry 41, 495500.CrossRefGoogle ScholarPubMed
WHO (1993). The Tenth Revision of the International Classification of Diseases and Related Health Problems (ICD-10): Diagnostic Criteria for Research. World Health Organization: Geneva.Google Scholar
Woods, S, Brier, A, Zipursky, R, Perkins, DO, Addington, J, Miller, TJ, Hawkins, KA, Marquez, E, Lindborg, SR, Tohen, M, McGlashan, TH (2003). Randomized trial of olanzapine versus placebo in the symptomatic treatment of the schizophrenic prodrome. Biological Psychiatry 54, 453464.CrossRefGoogle ScholarPubMed
Yung, AR, Phillips, LJ, Drew, LT (1999). Promoting access to care in early psychosis. In The Recognition and Management of Early Psychosis (ed. McGorry, P. and Jackson, H.), pp. 8084. Cambridge University Press: Cambridge.Google Scholar
Yung, AR, Stanford, C, Cosgrave, E, Killackey, E, Phillips, L, Nelson, B, McGorry, PD (2006). Testing the ultra high risk (prodromal) criteria for the prediction of psychosis in a clinical sample of young people. Schizophrenia Research 84, 5766.CrossRefGoogle Scholar