Abstract
Introduction:
To date, among individuals meeting ultra-high risk criteria for psychosis, the relationship between the presence of anxiety disorders and the risk of psychotic transition raises several unanswered questions.
Case description:
This case report describes the clinical progression of a 17-year-old male initially presenting anxious symptoms meeting the DSM-V criteria for panic disorder. The patient also reported social withdraw, mild depressive symptoms, insomnia and fatigue. Over a 6 month period, a gradual onset of subthreshold psychotic symptoms suggested a prodromal phase of a psychotic disorder.
Diagnostic assessment and therapeutic intervention:
A detailed assessment of UHR criteria for psychosis was performed. The overall level of social and occupational functioning was assessed by the SOFAS, which showed a 35% drop over a 12 months period. The CAARMS, has also been administered. The patient met the diagnostic criteria for UHR, APS group. The care plan included psychiatric follow-up, pharmacologic treatment, individual psychological follow-up and individual and familial psychoeducation. Over a 6 months period, the patient did not experienced a first psychotic episode and presented a partial improvement of psychotic symptoms.
Conclusion:
The DSM-V categorical approach does not seem to adapt well to early clinical presentations in transitional age youth. A transdiagnostic and dimensional approach allows to better identify at-risk patients of psychiatric disorders and implement early intervention strategies.
Introduction
As the onset of most psychiatric disorders typically occurs during late adolescence and early adulthood, transitional age youth (TAY) are an at-risk population in terms of mental health (1). Early intervention in mental health is crucial, as it seems promising in modifying long-term outcomes and reducing illness severity (2).
Recent research recognizes that current categorical frameworks for classification and treatment in psychiatry are inadequate, particularly in TAY. Trans-diagnostic clinical staging models have gained prominence, by allowing a multidimensional assessment and taking into account a continuum of illness (3).
Categorical diagnosis such as anxiety and schizophrenia have been considered as completely distinct entities for years, even if the comorbidity between them has long been recognized. Regarding schizophrenia, the initial diagnosis frequently occurs at the time of the first psychotic episode. However, the diagnosis is often preceded by a prodromal phase where several symptoms gradually emerge. Early symptoms may be non-specific and include anxiety, as well as depressed mood, social withdrawal and academic difficulties. Non-specific symptoms may be followed by the basic symptoms, subtle subclinical disturbances in cognition, perception, language, emotional reactivity and stress tolerance. Later, these abnormalities become more pronounced and subthreshold positive symptoms of psychosis also emerge (4). The broad range of symptoms present in these early stages of schizophrenia include a wide variety of anxiety symptoms and comorbid entities are often present (5). Thus, the identification of anxiety symptoms seems to be an essential step in the assessment of a potential prodromal phase, in particular, when evaluating a patient also presenting impaired cognitive or social functioning. Recent epidemiological studies also show that anxiety disorders, such as social anxiety disorder, panic disorder and obsessive-compulsive disorder, are more common among people diagnosed with psychotic disorders compared to the general population (6).
Current research establishes a new paradigm for schizophrenia prodrome, which is currently considered a flexible entity where symptoms can completely disappear, persist or progress in several possible directions. The term ultra-high risk (UHR) for psychosis has therefore been used to designate individuals who potentially present prodromal symptoms and may benefit from early intervention strategies (7). Most evidence-based recommendations for UHR point out cognitive-behavioral therapy (CBT) as the most efficacious intervention, improving social functioning, allowing reduction of psychotic symptomatology and preventing or delaying transition to psychosis. Studies on the benefit/ risk balance of antipsychotic medication were not conclusive and existing clinical guidelines do not recommend systematic antipsychotic use (8, 9).
To date, among UHR individuals, the relationship between the onset of anxiety symptoms and the risk of psychotic transition raises several unanswered questions and remains a topic of scientific interest. This case report presents the clinical situation of a 17-year-old adolescent complaining with anxious symptoms meeting the DSM-V criteria for panic disorder [300.01 (F41.0)]. The progressive emergence of prodromal symptoms, possibly suggesting a psychotic disorder, led to reflexions about anxiety disorders and psychosis as comorbid conditions or manifestations of the same clinical entity. The authors propose to include some considerations about the clinical and epistemological complexity of these categorical diagnoses. A trans-diagnostic dimensional approach is preferable in order to comprehensively assess the ever-changing clinical presentation and to provide appropriate care.
Case description
We describe the clinical case of a white Caucasian 17-year-old male adolescent referred to an outpatient child and adolescent mental health service in the Brussels urban area, Belgium, after an initial psychological assessment in a private outpatient clinic. At the time of the first psychiatric assessment, the patient was the main requester of the consultation. He presented, for about 3 months, panic attacks, characterized mainly by trembling, palpitations, a sensation of shortness of breath and a fear of losing control, without a trigger factor. These episodes, which had increased in frequency and intensity since their onset, were accompanied by a persistent worry of further panic attacks and an increase in social withdrawal that had been gradually increase in intensity over about 3 years. This posture described by the patient as voluntary self-isolation and avoidance of interactions with peers and family, was not associated with fear or anxiety related to social interactions. The patient also reported mild depressive symptoms, a sleep disorder characterized by initial insomnia, and fatigue.
Early childhood development was described as normal by parents and there was no history of perinatal complications. The patient received speech therapy, from age 3 to, for speech delay (first words at 24-months old) and articulation disorders. He took his first steps at around 12 months of age. Social interactions with peers were spontaneous during childhood and early adolescence. Regarding scholar functioning, no learning difficulties had ever been reported and he was attending, at the time of the first consultation, the last year of secondary school.
Prior to the onset of symptoms, there were no known family stressors or any significant life events, apart from the emigration of the family, from another European country, 7 years later, for professional reasons. Family psychiatric history was also not relevant.
His medical history included a primary spontaneous pneumothorax at the age of 16. He was admitted to hospital for 1 week and a chest tube was inserted, without complications. Physical examination (including cardiovascular screening) was normal, with a body mass index of 19 kg/m2. All laboratory results (blood and urine tests) were within normal limits. There was no history of alcohol, tobacco or drug use and he had not been on any medications.
Intelligence quotient (IQ) was assessed using the Wechsler Intelligence Scale for Adults, 4th Edition (10) and revealed a very superior IQ (140, percentile >99).
At the time of the first psychiatric assessment, Beck Depression Inventory II (BDI-II), was administered to measure the severity of depressive symptoms (11, 12). The patient scored for “mild depression” (score: 19). The Panic Disorder Severity Scale (PDSS), was also administered (13, 14). This self-report scale, assessing the severity of panic attacks and panic disorder symptoms, revealed a moderate intensity of symptoms (score: 12). Initial assessment outcomes are described in Table 1. The patient met the Diagnostic and Statistical Manual of Mental Disorders, 5th edition (DSM-V) criteria for panic disorder [300.01 (F41.0)] (15).
Table 1
| Tools and subtest(s) | Score | Interpretation |
|---|---|---|
| WAIS-IV | Percentile | |
| IQ | 140 | >99 |
| VCI | 122 | 93 |
| PRI | 134 | 99 |
| WMI | 137 | 99 |
| PSI | 145 | >99 |
| BDI-II | 19 | Mild depression |
| PDSS | 12 | Moderately ill |
Initial assessment results.
BDI-II, Beck Depression Inventory, second version; IQ, Intelligence Quotient; PDSS, Panic Disorder Severity Scale; PRI, Perceptual Reasoning Index; PSI, Processing Speed Index; VCI, Verbal Comprehension Index; WAIS-IV, Wechsler Adult Intelligence Scale, fourth edition; WMI, Working Memory Index.
Pharmacologic and psychotherapeutic treatment options were discussed with the patient and parents (16). Since the patient was not motivated to start CBT, a selective serotonergic reuptake inhibitor, Sertraline 50 mg per day, was initiated, with a substantial improvement of anxiety and depressive symptoms, over a 3 months period. No unexpected side effects were described.
Approximately 6 months after starting antidepressant treatment, parents reported a more pronounced decrease in social functioning, despite continued pharmacologic treatment and complete remission of panic attacks. In particular, parents observed a global decrease in social interactions, including family interactions, and the onset of clinophilia. The patient additionally reported aboulia and concentration problems related to school but only a slight drop in school results was observed at this stage. Besides, the patient reported, for the first time, having, for about 4 months, subthreshold psychotic symptoms, such as suspiciousness ideas, visual distortions, and subjective changes in speech, such as thought blockage and intrusive thoughts. These recent symptoms caused a significant distress and fear to “go crazy”.
Figure 1 shows a timeline of psychiatric symptoms and pharmacologic treatment.
Figure 1
Diagnostic assessment, therapeutic intervention
Further clinical evaluation was performed and included a detailed assessment of UHR criteria for psychosis as showed in Table 2. The 16-item Version of the Prodromal Questionnaire (PQ-16), a routine screening tool for UHR of developing psychosis (17) was administered and showed a total score of 11 points (above the distress threshold of 6 or more points). The overall level of psychosocial functioning was assessed by the Social and Occupational Functioning Assessment Scale (SOFAS) (18), showing a sustained 35% drop in SOFAS score over a 12 months period. The Comprehensive Assessment of at Risk Mental States (CAARMS), was also administered. The CAARMS is a semi-structured assessment tool used by mental health professionals to identify help-seeking youth who are at UHR of psychosis and to identify the onset of the first episode of psychosis (19). Patient presented subthreshold intensity and frequency scores on non-bizarre ideas subtest and perceptual abnormalities subtest. Based on both SOFAS and CAARMS scores, the patient met the diagnostic criteria for UHR, attenuated psychosis group (APS). He did not met the diagnostic criteria for brief, limited intermittent psychotic symptoms (BLIPS), neither trait vulnerability criteria (20). Based on presenting clinical features and the clinical staging model of mental disorders, the patient was assigned a stage 1b (21).
Table 2
| Tools and subtest(s) | Score | Interpretation | Qualitative data | |
|---|---|---|---|---|
| PQ-16 | 11 | Positive screening | Mild to moderate distress in all positive items | |
| SOFAS | −35% (12 months) | Significant decrease | Premorbid level: 80% | |
| CAARMS | ||||
| Unusual thought content | ||||
| Intensity | 0 | Not at risk | / | |
| Frequency | 0 | |||
| Non-Bizarre ideas | ||||
| Intensity | 3 | Attenuated psychosis | Suspiciousness and persecutory ideas “it seems that people look at me weirdly, that they talk about me in secret, that they could hurt me,” “this is probably an interpretation” | |
| Frequency | 4 | |||
| Perceptual abnormalities | ||||
| Intensity | 3 | Attenuated psychosis | Visual changes (distortions and/or illusions) “sometimes colors of the objects turn too intense,” “I do not understand why this is happening to me” | |
| Frequency | 4 | |||
| Disorganized speech | ||||
| Intensity | 2 | Not at risk | Subjective changes (chaotic intrusive thoughts and/or thought blockage) “sometimes my mind stops and my thoughts disappear suddenly,” “sometimes this blocks my ability to speak,” “my mind goes chaotic, there are too many thoughts at the same time” | |
| Frequency | 3 | |||
| Clinical stage | 1b | UHR (APS) | / |
UHR for psychosis assessment results.
APS, Attenuated Psychotic Syndrome; CAARMS, Comprehensive Assessment of At Risk Mental States; PQ-16, Prodromal Questionnaire, 16-item; SOFAS, Social and Occupational Functioning Assessment Scale; UHR, Ultra-High Risk for Psychosis.
In line with recent recommendations for UHR patients (8, 9), information about the diagnosis and early intervention strategies was provided and an individualized and multidisciplinary care plan was proposed. The patient still refused CBT and the follow-up included regular psychiatric monitorisation and supportive therapy, every 2–4 weeks. In order to better manage comorbid symptoms, sertraline was increased to 100 mg per day. Antipsychotic treatment was not initiated since the patient did not present severe and/ progressive UHR symptomatology (9). Both individual and family psychoeducational approaches were started even if evidence in UHR patient is still lacking and they focused on enhancing the understating of psychotic and non-psychotic symptoms, psychoeducation about the nature of anxiety and stress, engagement in treatment and increase adherence to treatment.
Over a 6 months period after the diagnosis and about a year after the onset of APS, a partial improvement of APS was observed by the clinician and the patient. The patient did not experienced a first psychotic episode over the same period.
During the initial psychiatric evaluation and the psychiatric follow-up, even if the patient was seeking care, he had a hard time in the therapeutic alliance and in explaining the symptoms, because of fear of stigmatization and of being diagnosed with a serious chronic disease. He also presented some difficulties in understanding the implications of the diagnosis and the therapeutic objectives, and in accepting the therapeutic strategies (CBT and pharmacological treatment). Both individual and family psychoeducational sessions were, according to the patient, unproductive at first, because he presented lack of motivation, but after that period, essential in order to finally understand available treatments and reduce stress and anxiety.
CARE case report guidelines were followed in the redaction of all sections the manuscript (Table 3).
Table 3
| Topic | Item | Checklist item description | Reported |
|---|---|---|---|
| Title | 1 | The diagnosis or intervention of primary focus followed by the words “case report” | Yes |
| Key words | 2 | 2–5 key words that identify diagnoses or interventions in this case report, including “case report” | Yes |
| Abstract | 3a | Introduction: What is unique about this case and what does it add to the scientific literature? | Yes |
| 3b | Main symptoms and/or important clinical findings | Yes | |
| 3c | The main diagnoses, therapeutic interventions and outcomes | Yes | |
| 3d | Conclusion—What is the main “take-away” lesson(s) from this case? | Yes | |
| Introduction | 4 | One or two paragraphs summarizing why this case is unique | Yes |
| Patient information | 5a | De-identified patient specific information | Yes |
| 5b | Primary concerns and symptoms of the patient | Yes | |
| 5c | Medical, family, and psycho-social history including relevant genetic information | Yes | |
| 5d | Relevant past interventions with outcomes | n/a | |
| Clinical findings | 6 | Describe significant physical examination (PE) and important clinical findings | Yes |
| Timeline | 7 | Historical and current information from this episode of care organized as a timeline | Yes |
| Diagnostic assessment | 8a | Diagnostic testing (such as PE, laboratory testing, imaging, surveys) | Yes |
| 8b | Diagnostic challenges (such as access to testing, financial, or cultural) | n/a | |
| 8c | Diagnosis (including other diagnoses considered) | Yes | |
| 8d | Prognosis (such as staging in oncology) where applicable | n/a | |
| Therapeutic intervention | 9a | Types of therapeutic intervention (such as pharmacologic, surgical, preventive, self-care) | Yes |
| 9b | Administration of therapeutic intervention (such as dosage, strength, duration) | Yes | |
| 9c | Changes in therapeutic intervention (with rationale) | Yes | |
| Follow-up and outcomes | 10a | Clinician and patient-assessed outcomes (if available) | Yes |
| 10b | Important follow-up diagnostic and other test results | Yes | |
| 10c | Intervention adherence and tolerability | Yes | |
| 10d | Adverse and unanticipated events | Yes | |
| Discussion | 11a | A scientific discussion of the strengths and limitations associated with this case report | Yes |
| 11b | Discussion of the relevant medical literature with references | Yes | |
| 11c | The scientific rationale for any conclusions | Yes | |
| 11d | The primary “take-away” lessons of this case report (without references) in a one paragraph conclusion | Yes | |
| Patient perspective | 12 | The patient should share their perspective in one to two paragraphs on the treatment(s) they received | Yes |
| Informed consent | 13 | Did the patient give informed consent? | Yes |
CARE case report guidelines.
n/a, non-applicable.
Discussion
Psychiatric clinical cases are often characterized by interactions and overlaps between different diagnostic entities. Initially, this clinical case met the DSM-V criteria for panic disorder. However, the evolution of the disease has raised questions regarding a possible schizophrenia prodrome. Non-specific negative symptoms, including sleep disturbances, depressed mood, fatigue and social withdrawal were already present at the time of initial clinical presentation. Still, it was the gradual onset of positive symptoms, the attenuated psychotic symptoms, in particularly persecutory ideas and visual perceptual abnormalities, that suggested a prodromal phase of a psychotic disorder.
The DSM-V categorical approach, usually applied in clinical practice and research, is based on a list of signs and symptoms drawing a clear line between normality and psychopathology, according to a defined threshold (15). This approach is being increasingly criticized by scientific community for multiple reasons such as the excessive comorbidity between syndromes and the lack of emphasis on developmental, social, cultural and environmental context. Dimensional approaches seem to better adapt to TAY psychopathology, often characterized by early clinical presentations which include non-specific or subthreshold intensity/frequency symptoms and by the high incidence of comorbid disorders (22). In recent years, trans-diagnostic clinical staging models have gained importance, by allowing a multidimensional assessment while considering illness as a dynamic continuum from its absence to its most extreme expression (3). This broader strategy to identify at-risk patients may ultimately permit to recognize early stages of severe mental disorders, offering new management strategies tailored to patient's clinical stage, preventing the onset and/or progression of mental disorders (23). More specifically, with regard to psychotic disorders, UHR criteria represents a milestone in early detection and intervention field. The prodromal phase, previously described retrospectively, is now approached as a prospective phase. Moreover, UHR individual have a high risk to develop psychotic disorders but this pathway is neither inevitable nor the only diagnostic possibility (2). Recent scientific efforts permitted to develop clinical criteria and tools to identify UHR individuals, including the SOFAS and the CAAMS. The use of these standardized instruments can be extremely helpful to enable an early transdiagnostic approach but also to complement differential diagnosis evaluations.
More studies are needed to better identify risk and protective factors involved in transition from UHR to first episode of psychosis and schizophrenia. In this particular situation, authors questioned whether these two clinical entities are comorbid disorders or dimensional manifestations of a same disorder and whether the presence of an anxiety disorder could increase the risk of psychotic transition in UHR individuals. Prospective studies conducted in UHR individuals have found high prevalence of psychiatric comorbidities, in particular depressive (between 31 and 34%) and anxiety disorders (between 28 and 39%) (24, 25). A study on 509 UHR individuals revealed that comorbid anxiety and depressive disorders do not appear to have an effect on the risk of psychotic transition (26). Conversely, a recent study showed that, in individuals presenting psychotic experiences, non-psychotic comorbidity increases the risk of psychotic transition (27). Furthermore, in adolescents and young adults, the presence of psychotic symptoms is frequent in depressive and anxiety disorders (28).
There is still limited knowledge of the mechanisms involved in the simultaneous presence of psychotic and anxiety symptoms, including if the treatment of anxiety disorders could decrease the frequency and intensity of subthreshold psychotic symptoms and the risk of psychotic transition. Additionally, in TAY, it is particularly important to take into account developmental, social, cultural and environmental contexts. According to cohort studies, individuals who develop schizophrenia in adulthood often show developmental abnormalities in early childhood, such as speech and motor disorders and social adjustment difficulties (29). However, there are many common risk factors between psychotic and anxiety symptoms (30). Nevertheless, the knowledge of identified risk factors may provide additional clues and guide diagnostic reasoning.
Individualized and multidisciplinary assessment and management, according to the clinical stage, should be offered to the patient and the family, ideally in a specialized center. However, to date, in Brussels, Belgium, there is no service or program specifically design to UHR patients, despite scientific evidence showing the role of these structures in reducing the risk of psychotic transition and reducing the duration of untreated psychosis, compared to conventional services (31). There is, therefore, a substantial difficulty in access to current treatment strategies. Antipsychotic medication prescription to UHR patients is not recommended in clinical practice guidelines based on the current evidence. Nevertheless, pharmacological treatment of comorbidities (principally depressive and anxiety disorders) and CBT seem to decline the rate of psychotic transition (32).
In conclusion, this case report illustrates frequent difficulties on psychiatric clinical practice, particularly in transition age youth. In UHR individuals, psychiatric comorbidities, including anxiety disorders, are common and may be responsible for additional distress. The DSM-V categorical approach does not seem to adapt well to TAY psychopathology, often characterized by early clinical presentations, non-specific and/or subthreshold symptoms. A transdiagnostic and dimensional approach could better identify at-risk patients of psychiatric disorders and allow a personalized targeted-care.
Funding
This study is part of the University Chair Psychiatry in Transition in a World in Transition (Université Libre de Bruxelles, Brussels, Belgium), supported by the Julie Renson Fund, the Queen Fabiola Fund and the King Baudouin Foundation. Apart from the financial contribution in research activities, the funding institutions have no role in data collection, diagnostic assessment, or therapeutic strategies.
Publisher's note
All claims expressed in this article are solely those of the authors and do not necessarily represent those of their affiliated organizations, or those of the publisher, the editors and the reviewers. Any product that may be evaluated in this article, or claim that may be made by its manufacturer, is not guaranteed or endorsed by the publisher.
Statements
Data availability statement
The original contributions presented in the study are included in the article/supplementary material, further inquiries can be directed to the corresponding author.
Ethics statement
Ethical review and approval was not required for the study on human participants in accordance with the local legislation and institutional requirements. Written informed consent to participate in this study was provided by the participants' legal guardian/next of kin.
Author contributions
JR and SM contributed to the manuscript draft and research on the topic. JR was responsible for the psychiatric assessment and follow-up of the patient. HN provided clinical advice to JR. HN and VD reviewed the case report and article as senior authors. All authors approved the submitted version.
Conflict of interest
The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.
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Summary
Keywords
anxiety disorders (AD), ultra-high risk (UHR), psychosis, schizophrenia—spectrum disorders, transitional age youth, case report
Citation
Reis J, Marchini S, Nicolis H and Delvenne V (2022) Case report: From anxiety disorders to psychosis, a continuum in transitional age youth?. Front. Psychiatry 13:990138. doi: 10.3389/fpsyt.2022.990138
Received
09 July 2022
Accepted
29 August 2022
Published
03 October 2022
Volume
13 - 2022
Edited by
Laura Fusar-Poli, University of Catania, Italy
Reviewed by
Alessandro Rodolico, University of Catania, Italy; Cecilia Maria Esposito, IRCCS Ca 'Granda Foundation Maggiore Policlinico Hospital, Italy
Updates
Copyright
© 2022 Reis, Marchini, Nicolis and Delvenne.
This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
*Correspondence: Joana Reis joana.figueiredooliveirareis@huderf.be
This article was submitted to Schizophrenia, a section of the journal Frontiers in Psychiatry
Disclaimer
All claims expressed in this article are solely those of the authors and do not necessarily represent those of their affiliated organizations, or those of the publisher, the editors and the reviewers. Any product that may be evaluated in this article or claim that may be made by its manufacturer is not guaranteed or endorsed by the publisher.