Schizophrenia Clinical Trial
Official title:
Selective Estrogen Receptor Modulators - A Potential Treatment for Psychotic Symptoms of Schizophrenia?
The aim of the project is to investigate the use of Raloxifene (a new form of estrogen) in
the treatment of women with schizophrenia and schizoaffective disorder. Raloxifene is a
Selective Estrogen Receptor Modulator (SERM), which means that it can affect the central
nervous system (CNS) effects of estrogen (eg. improving emotional symptoms, memory,
information processing and concentration), without adversely affecting reproductive
tissue/organs such as breast, uterus and ovaries. The investigators are conducting a
double-blind, placebo controlled, three month study comparing the psychotic symptom response
of women with schizophrenia in both groups. One group will receive standard antipsychotic
medication plus 120mg Raloxifene, while the second group will receive standard antipsychotic
medication plus oral placebo.
Hypothesis 1: That the women receiving adjunctive Raloxifene would have a quicker recovery
from psychotic symptoms, as measured on the rating scales, compared with the women receiving
adjunctive placebo.
Hypothesis 2: That the Raloxifene group would have better cognitive improvement than the
placebo group.
Estrogen is hypothesised to be protective for women against early onset of severe symptoms
of schizophrenia (Hafner, 1991; Seeman, 1992). This 'estrogen hypothesis' was derived from
epidemiological, clinical and animal studies. Following the results of such studies, the
investigators conducted a study (Kulkarni et al 1996) in which a group of premenopausal
women with schizophrenia were given 0.02mg oral estradiol as an adjunct to antipsychotic
drug treatment for eight weeks, and compared their progress with a similar group who
received antipsychotic drugs only. The group receiving estrogen made a significantly more
rapid recovery from acute psychotic symptoms and also reported improvement in their general
health status. Subsequently, the investigators conducted a four week double-blind,
placebo-controlled study, using 100mcg estradiol skin patches. The investigators found that
the 12 premenopausal women who received the estradiol adjunct had a significantly lower
total PANSS and BPRS score than 12 women who received placebo patches plus antipsychotic
medication.
The major potential risks in using estrogen as a longer term adjunctive treatment in
premenopausal women with schizophrenia appear to be the potential harmful effects of
estrogen itself in its action on breast and uterine tissue. Our studies were brief for this
reason, in that the investigators used estrogen without progesterone over an eight week or
four week period.
With the recent advent of Selective Estrogen Receptor Modulators, in particular Raloxifene
Hydrochloride, there is the potential to harness the positive estrogenic effect on CNS
neurotransmitter systems without affecting breast or uterine tissue. While the CNS effects
of Raloxifene have not been fully studied, its actions are mediated through binding to
estrogen receptors and can thereby regulate gene expression that is ligand, tissue or gene
specific. By inference then, Raloxifene would be expected to impact on dopamine and
serotonin pathways in a similar fashion to conjugated estrogen. A study (Nickleisen et al
1999) on the effect of Raloxifene on cognition in healthy, postmenopausal women found a
slight increase in verbal memory performance after one month of high dose treatment, while
no other differences were found after 12 months of treatment. There are no studies in women
with cognitive impairment where a treatment effect would be more likely to be apparent.
Similarly, there are no clinical studies to date investigating the effect of Raloxifene on
psychotic symptoms. To this end, the investigators are putting forward an investigator
initiated clinical trial proposal to investigate the effect of adjunctive Raloxifene on
psychotic symptoms in women with schizophrenia. This is, therefore, a study to follow our
Pilot Study in the same area, but with an increase of Raloxifene from 60mg to 120mg daily.
The aim of this project is to study the effect of Raloxifene as an adjunct to antipsychotic
medication in women with schizophrenia as a means to developing a novel, safe adjunctive
treatment for women with schizophrenia to improve their quality of life.
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Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Investigator), Primary Purpose: Treatment
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