Hostname: page-component-76fb5796d-2lccl Total loading time: 0 Render date: 2024-04-26T10:39:54.029Z Has data issue: false hasContentIssue false
  • English
  • Français

Overlooking the transition elephant in the ultra-high-risk room: are we missing functional equivalents of transition to psychosis?

Published online by Cambridge University Press:  29 November 2019

Andrea Raballo Open the ORCID record for Andrea Raballo [Opens in a new window]  and
Michele Poletti
Andrea Raballo*
Affiliation:
Department of Medicine, Division of Psychiatry, University of Perugia, Perugia, Italy Center for Translational, Phenomenological and Developmental Psychopathology, Perugia University Hospital, Perugia, Italy
Michele Poletti
Affiliation:
Department of Mental Health, Azienda Unità Sanitaria Locale-IRCCS di Reggio Emilia, Reggio Emilia, Italy
*
Author for correspondence: Andrea Raballo, E-mail: andrea.raballo@unipg.it
Rights & Permissions [Opens in a new window]

Abstract

In the wake of the almost quarter of a century since the conceptualization of ultra-high-risk (UHR) states for psychosis, empirical evidences in the field are constantly scrutinized and re-assessed through meta-analytic lens. Briefly, such scrutiny converges on three major evidences: pretest risk enrichment, risk hierarchy within UHR states, and declining transition rates. While the former two are intuitive, the dilution effect remains elusive and might be rather symptomatic of unsolved issues in the field. Those include the heterogeneously reported antipsychotic (AP) exposure in UHR samples and the almost univocal focus on purely psychometric transition to psychosis. Both issues lead to the neglect of functional equivalents of transition, i.e. that of a mental state at immediate need for AP medication, and might have a cascading confounding effect on the predictive value of contemporary risk calculators centered on criterial transition as a unique outcome.

Keywords

Antipsychoticconversionpredictionpsychosisrisk calculationthreshold
Type
Correspondence
Information
Psychological Medicine , Volume 52 , Issue 1 , January 2022 , pp. 184 - 187
Check for updates
Copyright
Copyright © Cambridge University Press 2019

Partly amplifying previous observations by Ajnakina, David, and Murray (Reference Ajnakina, David and Murray2018), Moritz, Gaweda, Heinz, and Gallinat (Reference Moritz, Gaweda, Heinz and Gallinat2019) systematically press central trigger points in contemporary early detection conceptual landscape. They highlight four reasons, including decreasing transition rates, why early detection centers for psychosis should be renamed and their treatment targets reconsidered. Transition to psychosis could be a more faceted outcome than usually thought and it is crucial to discuss potential limits of the concept itself and how these limits may have influenced the judgment on the early detection paradigm. Indeed, in the wake of the almost quarter of a century since the conceptualization of ultra-high-risk (UHR) states for psychosis (Yung & McGorry, Reference Yung and McGorry1996), empirical evidences are constantly re-assessed through meta-analytic lens, which converge on three key-points: (1) pre-test risk enrichment (Fusar-Poli et al., Reference Fusar-Poli, Schultze-Lutter, Cappucciati, Rutigliano, Bonoldi, Stahl and McGuire2016a), (2) stratification of risk among UHR subgroups (Fusar-Poli et al., Reference Fusar-Poli, Cappucciati, Borgwardt, Woods, Addington, Nelson and McGuire2016b), and (3) progressive decline of transition rates to psychosis, aka ‘dilution effect’ (Fusar-Poli et al., Reference Fusar-Poli, Cappucciati, Borgwardt, Woods, Addington, Nelson and McGuire2016b; Hartmann et al., Reference Hartmann, Yuen, McGorry, Yung, Lin, Wood and Nelson2016; Simon, Umbricht, Lang, & Borgwardt, Reference Simon, Umbricht, Lang and Borgwardt2014; Yung et al., Reference Yung, Yuen, Berger, Francey, Hung, Nelson and McGorry2007).

The dilution effect and the Janus-faced nature of transition

Whereas pre-test risk enrichment and within-UHR gradient are rather intuitive phenomena, the dilution effect remains rather obscure in its genesis and multi-causality. Several concurrent and non-mutually exclusive factors have been hypothesized: the decrease of duration of symptoms prior to first clinical contact (Yung et al., Reference Yung, Yuen, Berger, Francey, Hung, Nelson and McGorry2007), the possible preventive role of focused interventions [i.e. psychological therapy or antipsychotic (AP) medication] (Nelson et al., Reference Nelson, Yuen, Lin, Wood, McGorry, Hartmann and Yung2016; van der Gaag et al., Reference van der Gaag, Smit, Bechdolf, French, Linszen, Yung and Cuijpers2013) as well as the different clinical intake of recent UHR cohorts in comparison with earlier cohorts (Hartmann et al., Reference Hartmann, Yuen, McGorry, Yung, Lin, Wood and Nelson2016). However, none of these factors, although all empirically plausible and partly substantiated, is explanatory enough or satisfactory at a conceptual level. A better understanding of the dilution effect is mandatory for the field of early detection/intervention, since it would impact its evidence-basis as well as its strategic societal goals. In this perspective the mere criterial approach to define transition to psychosis has been criticized (van Os & Guloksuz, Reference van Os and Guloksuz2017) and a more radical and widespread aspect (i.e. the classical ‘elephant in the room’) could have been often overlooked, namely the prescription of antipsychotics (AP) in UHR samples (Raballo, Poletti, & Carpenter, Reference Raballo, Poletti and Carpenter2019).

In the UHR model, in addition to the criterial transition (based on rating scales), a functional equivalent of transition has been explicitly mentioned as the threshold at which AP treatment would be commenced in common clinical practice (Yung et al., Reference Yung, Phillips, Yuen, Francey, McFarlane, Hallgrem and McGorry2003). Albeit apparently subjective and arbitrary, such threshold is based on the real-world, collegial decision making of the treating staff and reflects a global apprehension of the severity of a clinical status requiring AP medication. Clearly, this indicates the end-point of the UHR state and signals ‘the threshold for onset of a psychotic episode’ (Yung et al., Reference Yung, Yuen, McGorry, Phillips, Kelly, Dell'Olio and Buckby2005).

Just a little bit like Janus Bifrons, conversion to psychosis could have two complementary faces, one looking to escalating positive symptoms (i.e. the criterial psychometric transition), and the other to the complexity of the global clinical trajectory (i.e. the functional equivalent indexed by the therapeutic need of AP medication).

Lost in transition: the glaring evidence of a clinical–conceptual scotoma

The concept of functional transition is crucial considering that AP need is rather frequent in the clinical management of UHR subjects. Of the 33 studies included in a recent meta-analysis addressing psychosis risk stratification (Fusar-Poli et al., Reference Fusar-Poli, Cappucciati, Borgwardt, Woods, Addington, Nelson and McGuire2016b), 24 studies (72.7%) reported exposure to AP during follow-up, yet without justifying it on the basis of worsened clinical severity or considering it a functional equivalent of conversion to psychosis; among these studies, at least seven (above 20%) included in the UHR sample subjects already on AP at the baseline assessment (i.e. in ostensible contradiction with the original UHR definition).

Considering the threshold at which AP medication would be commenced in common clinical practice as a functional equivalent to threshold for onset of psychosis episode, would substantially change the overall transition rates reported in the literature, since basically all the studies merely report criterial (i.e. psychometric) transitions neglecting the functional ones (Table 1). While this mismatch between criterial and functional equivalents of transition may depend on several, context-dependent factors, it is undeniable that its magnitude cannot be further ignored. For example, just considering the 11 studies in which it was possible to clearly extract the absolute number of both criterial transitions and functional transitions, we found that the amount of functional transitions (n = 350) is 215% larger than one of the criterial transitions (n = 163).

Table 1. Synopsis of criterial and functional equivalents of transitions to psychosis in studies reporting exposure to AP at follow-up (censed in Fusar-Poli et al., Reference Fusar-Poli, Cappucciati, Borgwardt, Woods, Addington, Nelson and McGuire2016b)

AP, antipsychotics; BS, basic symptoms; CAARMS, Comprehensive Assessment of At Risk Mental States; CBT, cognitive behavioral therapy; CHR, clinical high risk; CT, Criterial transition based on CHR instrument; FT, functional transition based on AP exposure during follow-up; SIPS, Structured Interview for prodromal symptoms; UHR, ultra-high risk.

a % of survival rate of transition calculated on the basis of UHR sample at baseline.

c Studies detailing the raw numbers of criterial transitions and AP exposure.

d Transition spread: % functional transitions minus % of criterial transitions.

e Ratio between functional transitions and criterial transitions.

Note: Criterial (psychometric) transition:

Functional equivalent of transition = mental state requiring AP therapy, derived from the reported exposure to AP during the follow-up.

Transition spread = Functional minus Criterial transition, is an index of:

  1. (1) Mismatch between positive symptoms based psychometric assessment and real world clinical severity requiring immediate AP treatment as a collegial decision of the treating staff.

  2. (2) When positive, indicates the amount of undetected psychotic-equivalent mental states.

  3. (3) When negative, indicates the proportion of individuals converting to psychosis not receiving appropriate treatment.

Functional v. criterial transition ratio = proportion between individual exposed to AP medication and individuals reaching psychometric criteria for psychosis, is an alternative index of the amount of undetected psychotic-equivalent mental states relative to the psychometric ones.

This might be due to the fact that dimensional rating scales, when evaluating transition from UHR to psychosis, mainly focus on positive symptoms. In clinical practice, however, the need for AP medication is established through a global clinical evaluation of the ongoing mental state, including overall clinical severity as consensually perceived by the treating staff. Such global evaluation would typically consider not only the level of positive symptoms but also concurrent disorganized, negative and accessory psychopathology as well as subtler features of role functioning and quality of life. This is further corroborated by the fact that, if we focus only on UHR criteria, BLIPS appear at higher risk than APS, while if we include symptom severity, negative symptoms, affective symptoms and psychosocial functioning, no clear differences emerge (at the baseline as well as at the follow-up) between UHR subgroups (McHugh et al., Reference McHugh, McGorry, Yuen, Hickie, Thompson, de Haan and Nelson2018), indicating that clinically-meaningful features of UHR mental state reside outside the positive dimension and need full consideration together with the risk/benefit ratio with AP medication (Raballo et al., Reference Raballo, Poletti and Carpenter2019).

Redeeming the elephant in the room and rethinking the transition paradigm

On the basis of this rather disillusioning photograph (i.e. an average AP exposure that is almost the double of the declared conversion rate: about 40% v. 22%, see Table 1) we could either hypothesize that UHR subjects are unduly over-exposed to off-label AP (although they do not reach the psychometric threshold for psychosis) or – in line with the original PACE criteria – that functional equivalents of transition to psychosis (i.e. a mental state requiring immediate AP medication) are systematically ignored. This widespread clinical and conceptual flaw could be involved in the surface-level phenomenon of dilution effect of criterial transition rate, or – at least – contribute substantially to its magnification. Indeed, when considering both criterial and functional transitions, the magnitude of the overall transition to psychosis almost redoubles and the dilution effect may vary substantially. Even more crucially, mainstream prediction models (typically limited to psychometric transitions and counting UHR undergoing AP treatment as simple non-converters) presumably underestimate natural course transition rates. Therefore, while a re-analysis of available datasets is highly recommendable, a new wave of UHR studies with more transparent and systematic reporting of AP exposure is clearly necessary, with AP continuation without apparent criterial transition being rigorously examined. Finally, the possible underestimation of transition to psychosis in UHR subjects should be considered in the current debate on resource allocation within early detection centers.

References

Ajnakina, O., David, A. S., & Murray, R. M. (2018). ‘At risk mental state’ clinics for psychosis – an idea whose time has come – and gone!. Psychological Medicine, 26, 16.Google Scholar
Fusar-Poli, P., Cappucciati, M., Borgwardt, S., Woods, S. W., Addington, J., Nelson, B.McGuire, P. K. (2016b). Heterogeneity of psychosis risk within individuals at clinical high risk: a meta-analytical stratification. JAMA Psychiatry, 73, 113120.CrossRefGoogle Scholar
Fusar-Poli, P., Schultze-Lutter, F., Cappucciati, M., Rutigliano, G., Bonoldi, I., Stahl, D.McGuire, P. (2016a). The dark side of the moon: meta-analytical impact of recruitment strategies on risk enrichment in the clinical high risk state for psychosis. Schizophrenia Bulletin, 42, 732743.CrossRefGoogle Scholar
Hartmann, J. A., Yuen, H. P., McGorry, P. D., Yung, A. R., Lin, A., Wood, S. J.Nelson, B. (2016). Declining transition rates to psychotic disorder in ‘ultra-high risk’ clients: investigation of a dilution effect. Schizophrenia Research, 170, 130136.CrossRefGoogle Scholar
McHugh, M. J., McGorry, P. D., Yuen, H. P., Hickie, I. B., Thompson, A., de Haan, L.Nelson, B. (2018). The ultra-high risk for psychosis groups: evidence to maintain the status quo. Schizophrenia Research, 195, 543548.CrossRefGoogle ScholarPubMed
Moritz, S., Gaweda, L., Heinz, A., & Gallinat, J. (2019). Four reasons why early detection centers for psychosis should be renamed and their treatment targets reconsidered: we should not catastrophize a future we can neither reliably predict nor change. Psychological Medicine, 49, 21342140.CrossRefGoogle Scholar
Nelson, B., Yuen, H. P., Lin, A., Wood, S. J., McGorry, P. D., Hartmann, J. A., & Yung, A. R. (2016). Further examination of the reducing transition rate in ultra high risk for psychosis samples: the possible role of earlier intervention. Schizophrenia Research, 174, 4349.CrossRefGoogle ScholarPubMed
Raballo, A., Poletti, M., & Carpenter, W. (2019). Rethinking the psychosis threshold in clinical high risk. Schizophrenia Bulletin, 45, 12.CrossRefGoogle ScholarPubMed
Simon, A. E., Umbricht, D., Lang, U. E., & Borgwardt, S. (2014). Declining transition rates to psychosis: the role of diagnostic spectra and symptom overlaps in individuals with attenuated psychosis syndrome. Schizophrenia Research, 159, 292298.CrossRefGoogle ScholarPubMed
van der Gaag, M., Smit, F., Bechdolf, A., French, P., Linszen, D. H., Yung, A. R.Cuijpers, P. (2013). Preventing a first episode of psychosis: meta-analysis of randomized controlled prevention trials of 12 month and longer-term follow-ups. Schizophrenia Research, 149, 5662.CrossRefGoogle ScholarPubMed
van Os, J., & Guloksuz, S. A. (2017). Critique of the ‘ultra-high risk’ and ‘transition’ paradigm. World Psychiatry, 16, 200206.CrossRefGoogle Scholar
Yung, A., & McGorry, P. D. (1996). The prodromal phase PF first-episode psychosis: past and current conceptualizations. Schizophrenia Bulletin, 22, 353370.CrossRefGoogle Scholar
Yung, A., Yuen, H. P., Berger, G., Francey, S., Hung, T. C., Nelson, B.McGorry, P. (2007). Declining transition rates in ultra high risk (prodromal) services: dilution or reduction of risk? Schizophrenia Bulletin, 33, 673681.CrossRefGoogle ScholarPubMed
Yung, A. R., Phillips, L. J., Yuen, H. P., Francey, S. M., McFarlane, C. A., Hallgrem, M., & McGorry, P. D. (2003). Psychosis prediction: 12-month follow up of a high-risk (‘prodromal’) group. Schizophrenia Research, 60, 2132.CrossRefGoogle Scholar
Yung, A. R., Yuen, H. P., McGorry, P. D., Phillips, L. J., Kelly, D., Dell'Olio, M.Buckby, J. (2005). Mapping the onset of psychosis: the comprehensive assessment of at-risk mental states. Australian and New Zealand Journal of Psychiatry, 39, 964971.10.1080/j.1440-1614.2005.01714.xCrossRefGoogle ScholarPubMed
Figure 0

Table 1. Synopsis of criterial and functional equivalents of transitions to psychosis in studies reporting exposure to AP at follow-up (censed in Fusar-Poli et al., 2016b)