The Efficacy and Safety of a Selective Estrogen Receptor Beta Agonist (LY500307) for Negative Symptoms and Cognitive Impairment Associated With Schizophrenia
NCT ID: NCT01874756
Last Updated: 2019-07-02
Study Results
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View full resultsBasic Information
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TERMINATED
PHASE2
95 participants
INTERVENTIONAL
2013-06-30
2017-12-31
Brief Summary
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Stage 1 was conducted in year 1 and Stage 2 will be conducted in years 2 and 3. The goal of Stage 1 was to identify and advance the highest dose that did not demonstrate a safety signal and had target selectivity as determined by lack of TT suppression. This criteria was fulfilled at both doses, the larger of the two (75 mg/day dose) was advanced to Stage 2. Furthermore, there was no suggestion of ERα receptor activation (i.e., no pattern of TT decreases or feminization AEs) at either dose (25 mg/day and 75 mg/day). A third arm of 150 mg/day was added to Stage 2 for evaluation. Stage 2 results in the following three arms: placebo, 75 mg/day and 150 mg/day. The goals of Stage 2 are to further assess LY500307 doses for safety and target selectivity, confirm cortical target engagement and assess efficacy.
Primary Aim 1: To determine if LY500307 demonstrates cortical target engagement as assessed by fMRI/N-back in frontal-parietal regions. Secondary measures of target engagement are fMRI episodic memory, Pseudo-Continuous Arterial Spin Labeling, Mismatch Negativity/evoked response potentials, Auditory Steady State Response, Auditory P300 and Quantitative EEG (QEEG).
Primary Aim 2: To determine if LY500307 is superior to placebo for one or more of the primary efficacy endpoints: negative symptoms (Negative Symptom Assessment Scale - 16-item total score), working memory (the composite score for the Letter Number Sequencing and Spatial Span tests) and verbal memory (Hopkins Verbal Learning Test).
Primary Aim 3: To determine if LY500307 reduces total testosterone (TT) plasma concentrations, which is indicative of loss of selectivity for ERβ and engagement of ERα, using the following criteria: Decrease in TT plasma concentrations of 50% from baseline in 50% of subjects per arm treated for two consecutive post-randomization values with LY500307 in Stage 1 and Stage 2 of the trial.
Primary Aim 4: To assess the safety of LY500307 by determining if there are SAEs, AEs "probably related to study drug," QTc prolongation, TT suppression (50% reduction from baseline) and to evaluate for other safety signals.
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Detailed Description
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Conditions
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Study Design
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RANDOMIZED
PARALLEL
TREATMENT
TRIPLE
Study Groups
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LY500307 150mg
LY500307 150mg
LY500307 150mg
LY500307 150mg daily dose (6 capsules of 25mg) for 8 weeks
placebo
placebo 6 pills of inactive drug
Placebo
6 placebo capsules daily for 8 weeks
LY500307 75mg
LY500307 75mg
LY500307 75mg
LY500307 75mg daily dose (3 capsules of 25mg and 3 capsules of placebo) for 8 weeks
LY500307 25mg
LY500307 25mg
LY500307 25mg
LY500307 25mg daily dose (1 capsules of 25mg and 5 capsules of placebo) for 8 weeks
Interventions
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LY500307 150mg
LY500307 150mg daily dose (6 capsules of 25mg) for 8 weeks
LY500307 75mg
LY500307 75mg daily dose (3 capsules of 25mg and 3 capsules of placebo) for 8 weeks
Placebo
6 placebo capsules daily for 8 weeks
LY500307 25mg
LY500307 25mg daily dose (1 capsules of 25mg and 5 capsules of placebo) for 8 weeks
Eligibility Criteria
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Inclusion Criteria
* Male
* DSM IV-TR diagnosis of schizophrenia as confirmed by Structured Clinical Interview for DSM-IV-TR (SCID)
* Outpatient or inpatient status
* Mild to moderate overall disease severity as defined by a CGI-S score of less than or equal to 4 (moderately ill) at randomization
* Moderate levels of negative symptoms as defined by a PANSS negative symptom sub-score greater than or equal to 11.
* Clinical stability as defined by:
1. No exacerbation of illness leading to an intensification of treatment in the opinion of the investigator within four weeks prior to randomization, and
2. No change in antipsychotic medication for at least four weeks prior to randomization
Exclusion Criteria
* Known or suspected history of prostate cancer, breast cancer, or other clinically significant neoplastic disease (other than squamous cell or basal cell carcinoma of skin)
* Known or suspected history of deep venous thrombosis, stroke, venous thromboembolism, pulmonary embolism, paresis or paralysis that may be thrombogenic in origin
* Subjects currently receiving testosterone replacement therapy or drugs that influence the hypothalamus-pituitary-gonadal axis.
* Subjects who have clinically significant extrapyramidal signs (EPS) as defined by a score of \>20 on the Simpson-Angus Scale (SAS)
* Clinically significant electrocardiogram (ECG) abnormality, including, but not limited to, a corrected QT interval (Bazett's; QTcB) \>450 msec. Repeat ECGs may be conducted at the discretion of the principal investigator.
* Subjects with known medical history of Human Immunodeficiency Virus positive (HIV+) status
* Subjects with an active seizure disorder
* Subjects with implanted pacemaker, medication pump, vagal stimulator, deep brain stimulator, TENS unit, ventriculoperitoneal shunt, or other contraindication to undergoing an MRI scan
* Known IQ less than 70 based on medical history
* Current DSM IV-TR diagnosis of substance dependence (excluding caffeine and nicotine)
* Subjects who test positive for (1) Hepatitis C virus antibody or (2) Hepatitis B surface antigen (HBsAg) with or without positive Hepatitis B core total antibody
* Subjects with moderate to severe renal impairment as defined by creatinine clearance (CrCl) \< 60 ml/min (measured by the Cockcroft-Gault equation) at screening. Repeat evaluation may be conducted at the discretion of the Principal Investigator.
* Subjects with hepatic impairment as defined by liver transaminases or total bilirubin \> 3 × upper limit of normal (ULN). Repeat evaluation may be conducted at the discretion of the Principal Investigator.
* Subjects considered a high risk for suicidal acts - active suicidal ideation as determined by clinical interview OR any suicide attempt in 30 days prior to screening
* Subjects who have participated in a clinical trial with any pharmacological treatment intervention for which they received study-related medication in the four weeks prior to randomization OR subjects currently receiving treatment (within 1 dosing interval plus four weeks) with an investigational depot formulation of an antipsychotic medication
* Subjects who demonstrate overtly aggressive behavior or who are deemed to pose a substantial risk of danger in the Investigator's opinion
18 Years
65 Years
MALE
No
Sponsors
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Eli Lilly and Company
INDUSTRY
Indiana University
OTHER
Responsible Party
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Alan Breier
Psychiatrist
Principal Investigators
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Alan Breier, MD
Role: PRINCIPAL_INVESTIGATOR
Indiana University
Locations
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Indiana University Center for NeuroImaging
Indianapolis, Indiana, United States
IU Biostatistics
Indianapolis, Indiana, United States
Prevention and Recovery Center for Early Psychosis
Indianapolis, Indiana, United States
Larue D Carter Memorial Hospital
Indianapolis, Indiana, United States
Countries
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Provided Documents
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Document Type: Study Protocol and Statistical Analysis Plan
Other Identifiers
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1303010802
Identifier Type: -
Identifier Source: org_study_id
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