Schizophrenia Clinical Trial
Official title:
Double Blind Study of Estradiol Plus Neuroleptic Versus Placebo Plus Neuroleptic in the Treatment of Psychotic Symptoms in Women With Schizophrenia
To investigate the 'estrogen-protection' hypothesis by comparing changes in psychotic
symptoms between one group of patients receiving standard antipsychotic drug treatment plus
placebo and a second matched group receiving standard antipsychotic drug treatment plus
100microgram estradiol patch in a double blind controlled trial.
Hypothesis : That the women receiving adjunctive estradiol will demonstrate a more rapid and
more substantial decrease in psychotic symptoms over the course of the study than the women
receiving adjunctive placebo.
BACKGROUND:
Schizophrenia is a severe mental disorder that affects up to two percent of the adult
population. Patients present with a variety of symptoms including hallucinations, delusions
and bizarre behaviour while some develop additional "negative" symptoms such as
amotivational states and poverty of thought. Schizophrenia is generally thought to be an
organic brain disorder with psychosocial determinants for course and outcome. The illness
appears to be heterogenous with groups of patients presenting with distinct and differing
patterns of psychopathology and illness course. Part of this heterogeneity includes distinct
male and female subtypes of schizophrenia.
In recent times, gender differences in schizophrenia have received some attention, in
particular from an epidemiological and psychopathological perspective. Hormonal studies have
been utilised to investigate underlying neuroendocrine disturbances in schizophrenia, but
information from these studies has not been used in the development of new gender specific
treatment strategies. Overall the treatment of schizophrenia has remained gender-blind. The
main gender differences observed in schizophrenia that have international consensus include
the later age of onset in women, better response to neuroleptics in women, and more
treatment resistant negative symptoms in men. Women have also demonstrated vulnerability to
psychotic episodes during menopause, the post-partum period and at low estrogen phases of
the menstrual cycle.
From these clinical observations, Seeman and Lang hypothesised that estrogen may provide
"protection" against early onset of severe schizophrenia in women, thereby accounting for
increased vulnerability during both lifetime and monthly low estrogen phases. Findings from
both basic and clinical research warrant further investigation of the hypothesis that
estrogen has a protective effect in women not only over the female life cycle, but also over
the menstrual cycle.
We have been conducting clinical trials in patients with schizophrenia using estrogen as a
treatment for many years, and have an international reputation for work in this area.
Initially, we conducted an open clinical trial with acutely ill schizophrenic women and
added 0.02mg of oral estradiol to the antipsychotic drug treatment of 11 women. Their
response was compared to seven women who received antipsychotic drugs alone. The estrogen
adjunct group showed dramatic earlier improvement, with significant reduction in positive
psychotic symptoms by day 3 of treatment. This suggests that estradiol may act as a catalyst
for treatment and could prove to be an important adjunctive treatment in the therapy of
schizophrenia. Subsequent to this early pilot study, we conducted a double blind placebo
controlled 3-arm study of 100mcg, 50mcg estradiol and placebo transdermal adjunctive
patches. Published in Schizophrenia Research(2001), our results showed that the 100mcg
estradiol adjunct afforded the best outcomes.
RESEARCH OBJECTIVES:
To investigate the usefulness of estradiol as an adjunctive treatment in schizophrenia ,by
comparing changes in psychopathology between one group of patients receiving standard
antipsychotic drug treatment plus a placebo skin patch and a second matched group receiving
standard antipsychotic drug treatment plus a 100mcg estradiol patch in a double blind, 28
day, controlled trial.
ETHICS REVIEW AND INFORMED CONSENT:
The protocol for this study has been approved by the Alfred Ethics Committee.
Only patients who are able to give informed consent, i.e. able to demonstrate an
understanding of the objectives of the study and the implications of their role in it, will
be recruited into the study. Patients who are extremely psychotic or disturbed will not be
approached to enter the study. Involuntary patients who are able to give informed consent
will be able to participate and where possible a guardian or relative will be contacted and
notified of the patients' involvement. Patients will be advised that their participation is
voluntary and that they are free to withdraw from the study at any stage.
CONFIDENTIALITY:
Patients' identity will remain anonymous at all times. Once a patient agrees to participate
in the study, she will be assigned a code number to ensure anonymity. Information about the
subject will be restricted to the researchers directly involved, unless there are clear
management issues, in which case the information will be shared with the treatment team.
Patients' files will be stored in locked filing cabinets with access available to
researchers only. All test results will be shared with the patient and family / guardian.
STUDY POPULATION:
A target number of 100 patients will be recruited over a three-year period with equal
numbers being allocated to each group. Patients will be recruited from both inpatient and
outpatient settings and patients may be recruited from other centres providing that approval
has been gained from the appropriate controlling bodies.
INCLUSION CRITERIA:
Female patients who have a current DSM 4 diagnosis of Schizophrenia, Schizoaffective or
Schizophreniform Disorder.
EXCLUSION CRITERIA:
- Female patients who are pregnant or lactating.
- Female patients with postpartum psychosis or related disorder
- Female patients with known abnormalities in the hypothalamo-pituitary gonadal-axis,
thyroid dysfunction, central nervous system tumours.
- Female patients taking estrogen preparations such as the oral contraceptive pill.
- Female patients whose psychotic illness is directly due to illicit drugs or who have a
history of substance abuse or dependence during the last 6 months.
Females with any significant unstable medical illness such as cardiovascular disease, renal
disease, Addisons disease, thromboembolic disorders, epilepsy, diabetes etc.
- Post-menopausal or pre-menarche female patients.
WITHDRAWAL CRITERIA:
Patients are free to withdraw from the study at any stage without offering an explanation.
Patients experiencing any adverse effects which, in the opinion of the investigator, are
serious (i.e. life threatening, requiring hospitalisation or medical treatment) will be
withdrawn from the study immediately. All patients withdrawn will be followed up until the
adverse event has resolved.
STUDY TREATMENTS CONCOMITANT TREATMENTS:
All patients will participate in standard in-patient and outpatient psychosocial therapies
and activities as advised by their treatment team. All patients will receive psychotropic
and non-psychotropic medications as per their treatment teams orders. All medications
received during the study will be recorded to be included in the analysis.
STUDY MEDICATION:
The study involves the addition of transdermal 100mcg estradiol (or transdermal placebo-
inactive substance) to standard antipsychotic treatment for 4 weeks. The length of the trial
is 1 menstrual cycle, which is a short period of estrogen use. Most side effects commonly
associated with estrogen use are related to long term administration and are thus not
applicable in this study.
STUDY MEASUREMENTS:
The PANSS (Kay et al. 1987) will be performed at screening/baseline and at each evaluation
visit. The PANSS consists of a Positive Scale (7 positive symptom constructs), a Negative
Scale (7 negative symptom constructs) and a General Psychopathology Scale (16 symptom
constructs). This scale will be the primary outcome measure of the trial.
In addition to the PANSS, the Adverse Symptom Checklist, Abnormal Involuntary Movement
Scale, Simpson Angus Scale and serum hormone measurements will be completed at each visit.
Cognitive testing will be performed monthly. Participants will be assessed at baseline, day
7, day 14, day 21 and day 28.
DATA MANAGEMENT:
All data gathered will be entered in the patients file under the patients code number. Files
will be stored in the research unit in locked filing cabinets. Data entered on computer will
be done so using the patients code number for identification. A separate booklet will be
used to record data collected at screening, baseline, and evaluation visits. All files will
be retained by the hospital for a period of 15 years after completion or discontinuation of
the trial.
;
Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double-Blind, Primary Purpose: Treatment
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