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Response to the commentary by Buoli et al., EURPSY-D-18-00265

Published online by Cambridge University Press:  28 July 2018

Paolo Fusar-Poli
Paolo Fusar-Poli*
Affiliation:
aEarly Psychosis: Interventions and Clinical Detection (EPIC) lab, Department of Psychosis Studies, Institute of Psychiatry, Psychology & Neuroscience, King's College London, London, United Kingdom bOASIS service, South London and Maudsley NHS Foundation Trust, London, United Kingdom cDepartment of Brain and Behavioral Sciences, University of Pavia, Pavia, Italy
*
*Correspondence to: Department of Psychosis Studies, 5th Floor, Institute of Psychiatry, Psychology & Neuroscience, PO63, 16 De Crespigny Park, SE5 8AF, London, United Kingdom. E-mail address: paolo.fusar-poli@kcl.ac.uk (P. Fusar-Poli).

Abstract

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Type
Commentary
Information
European Psychiatry , Volume 54 , October 2018 , pp. 100 - 101
Copyright
Copyright © European Psychiatric Association 2018

Dear Editor,

We read with interest the commentary by Buoli et al. [Reference Buoli, Esposito and Caldiroli1], on our study “Long-term validity of the At Risk Mental State (ARMS) for predicting psychotic and non-psychotic mental disorders”, which was published in European Psychiatry [Reference Fusar-Poli, Rutigliano and Stahl2]. In our prospective 6-year cohort study we followed up 710 individuals undergoing an assessment for a suspected Clinical High Risk state for Psychosis (CHR-P)3. We investigated their risk of developing psychotic and non-psychotic mental disorders. We concluded that the CHR-P designation [Reference Fusar-Poli, Cappucciati and Rutigliano4] is not associated with an increased risk of developing mental disorders other than psychosis [Reference Fusar-Poli3], replicating earlier independent findings [Reference Webb, Addington and Perkins5].

Overall, we feel that critical appraisals of published studies such as the commentary by Buoli et al are greatly beneficial to the scientific advancement of knowledge in the field of the CHR-P state [Reference Fusar-Poli3]. However, we also note some inaccuracies, that are discussed below.

Firstly, Buoli et al note that “cognitive strategies” –which should rather have been referred to as cognitive behavioural therapies- have yielded hopeful results for the prevention of psychosis. This is not completely correct, given that the most recent network meta-analyses found no evidence for superior efficacy of any specific treatments compared to each other to prevent the onset of psychosis [Reference Davies, Cipriani and Ioannidis6] or reduce the severity of symptoms [Reference Davies, Radua and Cipriani7] in CHR-P individuals.

Secondly, Buoli et al argued that we have classified bipolar disorders with psychotic features as non-psychotic conditions. This is incorrect: as clearly indicated in our eMethods, our category of bipolar disorders included ICD-10 non-psychotic bipolar disorder (F31.x, excluding F31.2 and F31.5) and cyclothymia (F34.0) [Reference Fusar-Poli3]. In our eMethods we have also provided the specific ICD-10 codes that were used to define the psychotic disorders that were considered as outcome in our prospective cohort analysis [Reference Fusar-Poli3]. Conversely, Buoli et al presented some retrospective data taken from a sample of patients affected with psychotic and non-psychotic bipolar disorders but did not clarify whether ICD or DSM diagnoses were used nor the specific diagnostic types.

Thirdly, there was some degree of conceptual confusion which was inherited by the retrospective vs prospective approach adopted by Buoli et al. The authors stated that, by retrospectively looking at the medical notes of 235 bipolar patients, about 80% were found to satisfy the CHR-P criteria. This is only highly hypothetical and of limited clinical value because the help-seeking criterion that is implicitly necessary to meet a CHR-P state in the real world [Reference Falkenberg, Valmaggia and Byrnes8] is not considered by the retrospective analysis of Buoli et al. [Reference Fusar-Poli9]. In fact, the prospective detection and recruitment of CHR-P individuals is the most challenging area in the field of psychosis prevention [Reference Fusar-Poli, Rutigliano and Stahl10Reference Fusar-Poli, Werbeloff and Rutigliano13].

Fourthly, the conclusions by Buoli et al are not particularly innovative. They concluded that the presence of CHR-P criteria is more frequently associated with a future diagnosis of psychotic bipolar disorders; however this is just confirming the core finding of our study [Reference Fusar-Poli, Rutigliano and Stahl2]. Buoli et al also speculated that bipolar disorders should not be considered a psychotic condition like schizophrenia in the light of “different biomarkers”. Unfortunately, no reference to support these putative differential biomarkers is provided, and to our best knowledge, no biomarker to distinguish bipolar disorders vs schizophrenia has been validated to date. Buoli et al also recommended distinguishing affective psychoses within the group of psychotic outcomes that are traditionally measured in the CHR-P field. However, this is already done as part of clinical routine to the point that it has alraedy received some meta-analytical demonstration [Reference Fusar-Poli, Nelson, Valmaggia, Yung and McGuire14]. Buoli et also incorrectly concluded that it is not currently possible to know the extent to which CHR-P individuals are at risk of developing schizophrenia-spectrum vs affective-spectrum psychotic disorders. However, our previous meta-analysis has clearly demonstrated that the 73% of CHR-P individuals who will develop psychotic disorders will actually develop schizophrenia spectrum disorders [Reference Fusar-Poli, Nelson, Valmaggia, Yung and McGuire14].

Fifthly, as indicated above, retrospective analyses such as those presented by Buoli et al. are unlike to impact the early detection of individuals at risk of bipolar disorders and their preventive care. Our Early Psychosis: Intervention and Clinical-detection (EPIC) lab has recently developed and validated one of the few psychometric tools which can be used to prospectively identify individuals at risk of developing bipolar disorders [Reference Fusar-Poli, De Micheli and Rocchetti15]: the Semistructured Interview for Bipolar At Risk States (SIBARS [Reference Fusar-Poli, De Micheli and Rocchetti15]). The SIBARS has demonstrated good prognostic accuracy and is being currently validated in different clinical scenarios. We hope that research centers such as that the team led by Buoli et al will further leverage on our initial study to refine and improve it, to advance the scientific knowledge in the field of early bipolar disorders and to ultimately benefit the lives of many young patients worldwide.

References

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