Bipolar Disorder Clinical Trial
Official title:
Comparison of Combination Olanzapine and Lithium and Combination Chlorpromazine and Lithium in the Treatment of a First Manic Episode With Psychotic Features.
Verified date | November 2015 |
Source | Melbourne Health |
Contact | n/a |
Is FDA regulated | No |
Health authority | |
Study type | Interventional |
Aim: In a population of first episode manic patients with psychotic features, we want to
compare the side effect profile, the degree of adherence and the subjective well being, as
well as the efficacy of two treatments: The standard treatment currently applied (lithium +
chlorpromazine) and an alternative treatment more recently introduced (lithium + olanzapine).
In addition, we want to study retrospectively the development of bipolar disorder and study
prospectively the 6 and 12-month outcome of a cohort of patients presenting a first manic
episode with psychotic features.
Research Background: While the efficacy of lithium in the treatment of acute mania has been
established by numerous studies, it is also known that up to 50% of the patients fail to
respond when it is prescribed alone. It is therefore common practice to complement the
treatment, most commonly with antipsychotics and benzodiazepines. It has been suggested that
antipsychotic agents are faster acting and are superior in controlling hyperactivity compared
to lithium, whereas mood stabilisation is better achieved by lithium, Typical antipsychotics,
such as chlorpromazine, may therefore be useful as adjunctive medication to mood stabilisers,
especially within the first few weeks of treatment of acute mania, and for patients
exhibiting psychotic symptoms or hyperactivity. They however can induce side effects
(somnolence, dizziness, dry mouth, extrapyramidal side effects such as rigidity of the
muscles, and possibly tardive dyskinesia (involuntary movements or contraction of muscles),
as well as akathysia (sense of restlessness). They finally have been suspected to contribute
to the occurrence of post-manic depression. Recent publications in chronic populations have
shown that atypical antipsychotics, such as olanzapine, are also an effective adjunctive
treatment. Olanzapine has the important advantage to induce a very low incidence of
extrapyramidal side effects, including tardive dyskinesia. It can however induce somnolence,
dizziness, dry mouth, and rather commonly weight gain. Moreover, some authors have reported
that olanzapine might induce mania. Both treatments appear then to have positive effects as
well as undesirable side effects. Our project is to compare them. The literature concerning
first episode mania is sparse, particularly in the domain of pharmacotherapy. One
retrospective study showed that 77% of the patients received antipsychotics at discharge and
25% at 6 months follow-up. No comparison has however been made between typical and atypical
antipsychotics, and there are no specific treatment guidelines of first episode mania with
psychotic features.
Project Summary: The hypothesis is that olanzapine and chlorpromazine will have a comparable
efficacy as adjunctive treatment of the acute manic episode with psychotic features. We
however think olanzapine will induce less side effects and will be better accepted by the
patients, and therefore that the adherence to the treatment will be better than with
chlorpromazine. We finally think the subjective sense of well being will be greater with
olanzapine than with chlorpromazine.We will recruit 75 patients at the time of their first
admission for mania with psychotic features at EPPIC. After signature of the informed
consent, we will perform a baseline assessment first to confirm the diagnosis, and second to
evaluate the level of psychopathology. The patients will then be randomly selected to receive
either a treatment of lithium and olanzapine or a treatment of lithium and chlorpromazine. By
the end of the study there will be 37 patients in each group.The patients will go through a
baseline assessment including physical examination and usual laboratory investigation to
exclude any physical illness. They will also go through a one-hour assessment of
psychopathology. Between day 2 and 3 they will go through 2 hours of interview to reassess
diagnosis and personal history. They will thereafter be assessed weekly for eight weeks on
various dimensions: evolution of the intensity of the symptoms, appearance of depressive
symptoms, occurrence of side effects and degree of adherence to the treatment, in an 1-hour
interview. Subjective well being and quality of life will re evaluated at week 4 and 8,
adding 45 minutes to the duration of the interview. This is a flexible dose, open trial,
which means the doctor in charge of the patient will know which medication is being
prescribed, and that he will be allowed to adapt the dosage according to what he feels
necessary. This research project will allow us to organise a more specialised clinic for the
care of first episode manic patients. We will take this opportunity to study carefully the
months preceding the appearance of the first episode in order to try to reconstruct the
prodrome of bipolar disorders. We will also, in an extension phase of the study, look at the
long term outcome (at 6 and 12 months) of a first episode of mania.
Status | Completed |
Enrollment | 83 |
Est. completion date | November 1, 2015 |
Est. primary completion date | November 1, 2015 |
Accepts healthy volunteers | No |
Gender | All |
Age group | 15 Years to 29 Years |
Eligibility |
Inclusion Criteria: - Male and female patients aged 15 to 29. - Experiencing a first episode psychosis. - Meet DSM-IV criteria for bipolar either manic or mixed episode, or schizoaffective disorder manic episode. - Minimum score of 20 on the YMRS - Written informed consent to participation. Exclusion Criteria: - Patients at immediate risk of committing harm to self or others - Use of neuroleptics or mood-stabilisers in the two months preceding admission to EPPIC - Organic mental disease, including mental retardation - History of clinically significant illness (liver or renal insufficiency, significant cardiac, vascular, pulmonary, gastrointestinal, endocrine, neurological or metabolic disturbances). - Clinically relevant biochemical or hematological abnormalities. - Pregnant or lactating woman - History of epilepsy - History of severe drug allergy or hypersensitivity - Non fluency in English. |
Country | Name | City | State |
---|---|---|---|
Australia | ORYGEN Youth Health | Parkville | Victoria |
Lead Sponsor | Collaborator |
---|---|
Melbourne Health |
Australia,
Type | Measure | Description | Time frame | Safety issue |
---|---|---|---|---|
Primary | Intensity of side effects | Intensity of side effects | 8 weeks | |
Primary | ¨The frequency of treatment-emergent adverse events (events that first appear or worsen during the study period) will be compared between both groups. | 8 weeks | ||
Primary | ¨The frequency of side effects as rated with the UKU scale will be compared between both groups. | 8 weeks | ||
Primary | ¨Weight gain will be compared between both groups. | 8 weeks | ||
Primary | ¨Frequency of changes in vital signs and laboratory findings will be compared between both groups. | 8 weeks | ||
Primary | Subjective well being | 8 weeks | ||
Primary | ¨Total scores on the DAI and the SWN will be compared between both groups. | 8 weeks | ||
Secondary | Adherence | 8 weeks | ||
Secondary | ¨Degree of adherence to the treatment as scored on the MARS will be compared between both groups. | 8 weeks | ||
Secondary | Response to treatment | 8 weeks | ||
Secondary | ¨End point analysis: Mean change in various scales from baseline to week 4 and week 8 will be used to compare the efficacy of the two treatments: | 8 weeks | ||
Secondary | ¨Primary efficacy analysis will be assessed by comparing the mean change in theYMRS total score. | 8 weeks | ||
Secondary | ¨Secondary efficacy analysis will be assessed by comparing the mean change in CGI-BP total score and in BPRS total score. | 8 weeks | ||
Secondary | ¨Response analysis: Response is defined as at least a 50% drop in the total YMRS total score from base line to the 8-weeks end point. Euthymia is defined as a total score on the YMRS of no greater than 12 at end point. The number of patients reaching bot | 8 weeks | ||
Secondary | Incidence of depressive episodes | 8 weeks | ||
Secondary | ¨A worsening in the HAMD-21 score of at least 3 points will be used as a definition of a clinically detectable worsening in depressive symptoms. | 8 weeks | ||
Secondary | Six and 12 months outcome | 12 months | ||
Secondary | Definition of recovery: | 12 months | ||
Secondary | ¨Syndromic recovery: Eight contiguous weeks [50] during which the patient no longer meets criteria for a manic, mixed, or depressive syndrome. Recovery from each of these syndromes is based on DSM-IV criteria and is operationalised as follows: manic synd | 12 months | ||
Secondary | ¨Symptomatic recovery: Eight contiguous weeks [50] during which the patient experiences minimal to no psychiatric symptoms, operationalized as follows: Young Mania Rating Scale total score of 5 or less, Hamilton depression scale total score of 10 or les | 12 months | ||
Secondary | ¨Relapse: Relapse is defined as the return of symptoms after a remission of less than 8 weeks. | 12 months | ||
Secondary | ¨Recurrence: Recurrence is defined as return of symptoms after recovery. | 12 months | ||
Secondary | ¨Functional recovery: Return to premorbid levels of function for at least 8 contiguous weeks [50]. To assess functional recovery, seven of the nine general items from the Premorbid Adjustment Scale are evaluated at the 6 and 12-month follow-up visit for | 12 months |
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