Psychiatric disorders in 22q11.2 deletion syndrome are prevalent but undertreated

Tang, Sunny X.; Yi, James; Calkins, Monica E.; Whinna, Daneen A.; Kohler, Christian G.; Souders, Margaret C.; McDonald‐McGinn, Donna M.; Zackai, Elaine H.; Emanuel, Beverly S.; Gur, Ruben C.; Gur, Raquel E.

doi:10.1017/s0033291713001669

Cited by 136 publications

(101 citation statements)

References 32 publications

(69 reference statements)

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“…Twenty-two of them (24.7%) fully met UHR criteria (i.e., including frequency and onset/ worsening requirements). Both rates are broadly consistent with previous studies in 22q11DS, reporting rates between 45 and 56% for UHR symptoms and between 10 and 21% for UHR criteria 10,11,[16][17][18]33 . Thus, our findings confirm that patients with 22q11DS are at increased risk of experiencing attenuated symptoms of psychosis, regardless of transition to psychosis 23,34 .…”

Section: Uhr Symptoms and Criteriasupporting

confidence: 91%

“…Moreover, 22q11DS was found in 0.3 to 2.0% of patients with schizophrenia [12][13][14] , with rates of up to 5.7% in patients with childhood-onset schizophrenia 15 . Taken together, these findings indicate that 22q11DS is a highly relevant genetic risk factor for schizophrenia and the most promising human model for studying risk factors and states at risk for schizophrenia 5 .Several studies have investigated prodromal symptoms in patients with 22q11DS, reporting rates between 45 and 56% for UHR symptoms and between 10 and 21% for UHR criteria (including frequency and onset/worsening requirements) 8,10,11,[16][17][18] . Armando et al 8 compared the symptom profile of UHR patients with (N530) vs. without (N581) 22q11DS and found no significant group difference in positive symptoms, while negative symptoms were more severe in patients with 22q11DS.…”

mentioning

confidence: 92%

“…Several studies have investigated prodromal symptoms in patients with 22q11DS, reporting rates between 45 and 56% for UHR symptoms and between 10 and 21% for UHR criteria (including frequency and onset/worsening requirements) 8,10,11,[16][17][18] . Armando et al 8 compared the symptom profile of UHR patients with (N530) vs. without (N581) 22q11DS and found no significant group difference in positive symptoms, while negative symptoms were more severe in patients with 22q11DS.…”

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confidence: 99%

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Ultra High Risk Status and Transition to Psychosis in 22q11.2 Deletion Syndrome

et al. 2017

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The 22q11.2 deletion syndrome (22q11DS) is characterized by high rates of psychotic symptoms and schizophrenia, making this condition a promising human model for studying risk factors for psychosis. We explored the predictive value of ultra high risk (UHR) criteria in a sample of patients with 22q11DS. We also examined the additional contribution of socio-demographic, clinical and cognitive variables to predict transition to psychosis within a mean interval of 32.5 6 17.6 months after initial assessment. Eighty-nine participants with 22q11DS (age range: 8-30 years; mean 16.1 6 4.7) were assessed using the Structured Interview for Psychosis-Risk Syndromes. Information on Axis I diagnoses, internalizing and externalizing symptoms, level of functioning and IQ was also collected. At baseline, 22 (24.7%) participants met UHR criteria. Compared to those without a UHR condition, they had a significantly lower functioning, more frequent anxiety disorders, and more severe psychopathology. Transition rate to psychosis was 27.3% in UHR and 4.5% in non-UHR participants. Cox regression analyses revealed that UHR status significantly predicted conversion to psychosis. Baseline level of functioning was the only other additional predictor. This is the first study investigating the predictive value of UHR criteria in 22q11DS. It indicates that the clinical path leading to psychosis is broadly comparable to that observed in other clinical high-risk samples. Nevertheless, the relatively high transition rate in non-UHR individuals suggests that other risk markers should be explored in this population. The role of low functioning as a predictor of transition to psychosis should also be investigated more in depth. . This syndrome is characterized in most cases by a microdeletion of 3 million base pairs on chromosome 22 band q11, and has an estimated prevalence of 1:2.000-4.000 live births 6 . From a clinical perspective, 22q11DS is associated with high rates of psychiatric disorders, especially schizophrenia 7 . While 23 to 45% of affected adolescents report transient psychotic experiences [8][9][10][11] , up to 40% of affected adults are diagnosed with a psychotic disorder 7 . Moreover, 22q11DS was found in 0.3 to 2.0% of patients with schizophrenia [12][13][14] , with rates of up to 5.7% in patients with childhood-onset schizophrenia 15 . Taken together, these findings indicate that 22q11DS is a highly relevant genetic risk factor for schizophrenia and the most promising human model for studying risk factors and states at risk for schizophrenia 5 .Several studies have investigated prodromal symptoms in patients with 22q11DS, reporting rates between 45 and 56% for UHR symptoms and between 10 and 21% for UHR criteria (including frequency and onset/worsening requirements) 8,10,11,[16][17][18] . Armando et al 8 compared the symptom profile of UHR patients with (N530) vs. without (N581) 22q11DS and found no significant group difference in positive symptoms, while negative symptoms were more severe in patients with 22q11DS. Yet, few stud...

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Section: Uhr Symptoms and Criteriasupporting

confidence: 91%

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confidence: 92%

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confidence: 99%

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Ultra High Risk Status and Transition to Psychosis in 22q11.2 Deletion Syndrome

et al. 2017

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“…Stigma was also experienced in relation to psychiatric illness, as 22q11DS patients are at higher risk for developing psychiatric illnesses, such as mood disorders, psychosis, or schizophrenia (Tang et al, 2014). The studies report that stigma experienced in relation to mental health, did not only appear to affect societal perceptions but also the possibility of parents unconsciously treating their child differently.…”

Section: Resultsmentioning

confidence: 99%

The psychosocial impact of 22q11 deletion syndrome on patients and families: A systematic review

McNeill

Vogt

2018

American J of Med Genetics Pt A

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The 22q11 deletion syndrome (22q11DS) is one of the most common genomic disorders in humans, affecting around 1:2,000 to 1: 4,000 people. 22q11DS affects multiple body systems and is associated with multiple physical problems. Given the high rate of physical morbidity associated with the 22q11DS, it was hypothesized that it would exert a high psychosocial impact on patients and their relatives. To investigate this, a systematic review of the literature and narrative synthesis was performed. Three major themes emerged. First, the complex and conflicting emotions experienced by family members resulting from the diagnosis. Second, the pervasive educational and health‐care challenges associated with the diagnosis and third that people affect by 22q11DS strived for individualism. The results of this review help to inform clinical management of families with 22q11DS.

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“…Its behavioural phenotype, including the psychopathological features and endocrine dysfunctions, especially hypoparathyroidism, was originally described by the speech therapist Robert Shprintzen [50]. Over subsequent years it became apparent that 22q11DS is highly associated with symptoms from the schizophrenia, bipolar, anxiety and autistic spectrum [51,52]. With respect to the neuropsychological phenotype, it has been shown that deficits in problem solving and planning as well as in abstract and social thinking are most prominent [53].…”

Section: Psychopathological Phenotypes: Some Examples 22q112 Microdementioning

confidence: 99%

Aetiology Based Diagnosis and Treatment Selection in Intellectually Disabled People with Challenging Behaviours

Verhoeven¹,

Egger

2014

J. Intellect. Disabl. Diagn. Treat.

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Since both intellectual disability and challenging behaviour are entities encompassing heterogeneous clinical conditions and current taxonomies are of limited use in this field of psychiatry, diagnosing psychiatric symptoms in intellectually disabled patients is still very complex. In the diagnostic process of psychiatric symptoms and behavioural abnormalities, the first step should be genome profiling using the latest techniques in order to detect pathogenic CNVs or single gene mutations that are causative for the developmental delay. Their importance can be derived from the scientific observation that several genetic syndromes are associated with a specific behavioural, psychiatric, neuropsychological or neurological symptom profile, relevant for both choice of treatment and prognosis. Second, it has to be stressed that psychiatric disorders, especially from the depression and anxiety spectrum, frequently manifest with atypical symptoms that may hamper adequate pharmacological treatment. With respect to challenging behaviours in general, it should be emphasized that these are essentially dependent on contextual variables for which no rational pharmacological treatment is available and behavioural interventions are primarily warranted. Prescription of psychotropics has been demonstrated to be marginally effective only and to induce regularly unwanted side effects or even an increase of abnormal behaviours. It is therefore recommended to measure always the plasma concentration of psychotropics and antiepileptics and to perform, preferably prior to the start of treatment, genotyping of relevant cytochrome isoenzymes.In is concluded that, apart from the a priori genetic analysis, careful investigation of the here described data sources is needed to formulate a diagnostic hypothesis and treatment proposal.

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Psychiatric disorders in 22q11.2 deletion syndrome are prevalent but undertreated

Cited by 136 publications

References 32 publications

Ultra High Risk Status and Transition to Psychosis in 22q11.2 Deletion Syndrome

Ultra High Risk Status and Transition to Psychosis in 22q11.2 Deletion Syndrome

The psychosocial impact of 22q11 deletion syndrome on patients and families: A systematic review

Aetiology Based Diagnosis and Treatment Selection in Intellectually Disabled People with Challenging Behaviours

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