Schizophrenia Clinical Trial
Official title:
Is Premorbid Functioning a Predictor of Outcome in Patients With Early Onset Psychosis Treated With Risperdal Consta?
The purpose of this research study is to see how well patients in an early phase of their illness respond to treatment and whether this depends on how well they functioned socially, academically and vocationally before becoming ill. The study also examines whether patients with more insight into their illness have better outcomes.
Intervention with antipsychotic medications during the early stages of schizophrenia may
result in a better outcome for patients, with a higher number of patients achieving full
remission, a shorter time to remission and decreased risk of relapse. In addition, there is
evidence to suggest that a critical window of opportunity exists in the early period of
syndromal differentiation, when pharmacological intervention and intensive engagement of the
patient may impact favourably on symptoms in the longer term.
The long-acting injectable formulation of risperidone has shown improvements in measures of
disease severity over the oral formulation, and demonstrated an improved safety and
tolerability profile because of its lower peak-trough levels. A recent study has
demonstrated that patients in the early phase of their illness (0-3 years) benefit from
treatment with RLAI.
Although premorbid functioning is accepted to be a predictor of outcome and to affect
treatment adherence, prospective clinical data are scarce. RLAI addresses the problem of
adherence by eliminating the need for daily medication intake. In this study we investigate
whether patients with good premorbid functioning respond better to treatment with RLAI
compared to patients with poor premorbid functioning. Moreover, patients with schizophrenia
often fail to acknowledge their illness and need for treatment - so-called 'lack of
insight'. Previous studies investigating the relationship between acute psychopathology and
insight have produced conflicting results. Multiple administrations of a structured measure
of insight (SAI-E) and symptom measures will provide here a means to evaluate whether
insight is correlated with clinical change, whether insight changes over time and whether
changes in insight are related to changes in psychopathology.
A physical examination will be performed, including heart rate, blood pressure, and weight.
Interviews and assessments will be made to complete standard rating scales (Positive and
Negative Symptom Score (PANSS), Scale for Assessment of Insight-Expanded version (SAI-E),
Clinical Global Impression (CGI), Global Assessment of Functioning (GAF), and Extrapyramidal
Symptom Rating Scale (ESRS)). The Short-Form-36 questionnaire (SF-36) will be completed by
the patient. Any health problems and medicines of the patient will be recorded.
The primary hypothesis, that patients with "Stable-good" premorbid functioning will have
better outcomes than those with "Stable-poor" premorbid functioning will be examined by
dividing patients into a "Stable-good" and "Stable-poor" premorbid functioning groups based
on their total scores on the Premorbid Adjustment Scale (PAS). Statistically significant
differences between the "Stable-good" vs. "Stable-poor" pre-morbid groups on the combined
change measure at the 5% level will be interpreted as supporting the hypothesis.
Association of insight and outcomes will be examined using Scale for Assessment of
Insight-Expanded version (SAI-E )and insight item (G 12) from Positive and Negative Symptom
Score (PANSS). Effectiveness [Clinical Global Impression (CGI-S/C), PANSS, retention rate),
functioning [Short-Form-36 questionnaire (SF-36, rehospitalisation rates)] and safety and
tolerability will be assessed. The observation period is 6 months. RLAI is given as
intramuscular injections every 2 weeks. The starting dose of RLAI will be in accordance with
the product label (usually 25 mg). If necessary, the dosage of the injection may be
increased gradually. Treatment duration is 26 weeks. To ensure continued antipsychotic
coverage until the main release of risperidone from the microspheres, previous antipsychotic
therapy will be continued concomitantly during the first three weeks of the study.
;
Allocation: Non-Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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