Examining the Effects of Estradiol on Neural and Molecular Response to Rewards in Perimenopausal-Onset Anhedonia and Psychosis
Overview
- Phase
- Phase 4
- Intervention
- Micronized Progesterone
- Conditions
- Depression
- Sponsor
- University of North Carolina, Chapel Hill
- Enrollment
- 103
- Locations
- 2
- Primary Endpoint
- Changes in Striatal Activation Between Groups during the MID task
- Status
- Recruiting
- Last Updated
- 3 days ago
Overview
Brief Summary
This proposal will examine the effects of estradiol administration on perimenopausal-onset (PO) anhedonia and psychosis symptoms as well as on brain function using simultaneous positron emission tomography and functional magnetic resonance imaging (PET-MR).
Detailed Description
The transition to menopause (the "perimenopause") is characterized by increased risk for new onset of depression and psychosis. Our work and that of others has demonstrated that a prominent symptom of perimenopausal-onset (PO) depression is anhedonia, contributing significantly to distress and functional impairment. Additionally, the incidence of psychosis in women may increase during this period. Declining or low levels of estradiol, particularly in the late perimenopause, may play a role in the pathogenesis of PO anhedonia and PO psychosis via effects on mesolimbic brain reward circuitry and dopamine (DA) neurotransmission. Preclinical evidence has established that estradiol modulates dopamine systems and reward-related behaviors and estradiol withdrawal evokes loss of dopaminergic functions. Whereas estrogen therapy has shown benefits in reducing mood and psychotic symptoms in perimenopausal women, no study has examined the neural mechanisms underlying such effects in a transdiagnostic sample. This project will examine the effects of estradiol administration on perimenopausal-onset (PO) anhedonia and psychosis using simultaneous positron emission tomography and functional magnetic resonance imaging (PET-MR). Preliminary data presented here demonstrate that anhedonia is associated with decreased striatal DA release to rewards using PET with the D2/D3 DA receptor antagonist \[11C\]raclopride; anhedonia and psychosis are characterized by altered striatal activation to rewards using fMRI; estradiol impacts neural responses to rewards in PO anhedonia and PO psychosis; and estradiol improves PO anhedonia and PO psychosis. This project proposes to extend these lines of research by using simultaneous PET-MR to investigate the effects of transdermal estradiol, administered as a mechanistic probe, on PO anhedonia and PO psychosis in a transdiagnostic sample of women using a double-blind between-groups placebo-controlled design. This sample will be enriched for anhedonia (i.e., at least mild anhedonia). Although anhedonia and psychosis will be analyzed dimensionally, our recruitment and stratification strategy will ensure that a range of symptom severities (mild-to-moderate or high PO anhedonia; absent-to-mild or moderate PO psychosis) are equally balanced and randomized to each experimental group (estradiol or placebo). Our central hypotheses are that the mesolimbic DA system is impaired in PO anhedonia and psychosis, that estradiol administration will normalize neural responses to rewards (measured by fMRI) and striatal DA functioning (measured by PET), and that the degree of change in striatal functioning will be associated with the degree of change in PO anhedonia and PO psychosis. Specific Aim 1 (baseline associations between PO anhedonia, PO psychosis, and PET-MR): Characterize, at baseline, associations between PO anhedonia and PO psychosis symptom severity and reward-related striatal activation measured by fMRI, and tonic and phasic striatal DA activity measured by \[11C\]raclopride PET. Specific Aim 2 (estradiol effects on PO anhedonia and PET-MR): Determine the effects of estradiol (vs. placebo) on PO anhedonia and changes in PET-MR metrics related to reward processing. Specific Aim 3 (estradiol effects on PO psychosis and PET-MR): Determine the effects of estradiol (vs. placebo) on PO psychosis and changes in PET-MR metrics related to reward processing. This project will improve our understanding of PO anhedonia and psychosis and the mechanisms of action of the effect of estradiol on PO anhedonia and psychosis. This research will provide new mechanistic endpoints to evaluate novel PO anhedonia and psychosis treatments that target the mesolimbic DA system.
Investigators
Eligibility Criteria
Inclusion Criteria
- •Provision of signed and dated informed consent form
- •Stated willingness to comply with all study procedures, lifestyle considerations, and availability for the duration of the study
- •44-55 years old unmedicated perimenopausal women who have ≥ 2 skipped menstrual cycles, amenorrhea ≥ 60 days, corresponding to the late menopause transition (Stages of Reproductive Aging Workshop (STRAW stage -1).
- •Anhedonia or psychosis symptoms that began during the period of menstrual irregularity.
- •Clinician's Global Impression Scale-Severity score (CGI-S) \> 3 to confirm a clinically impaired sample.
- •Anhedonia severity inclusion criteria and stratification: All participants will have Snaith-Hamilton Pleasure Scale (SHAPS) scores \> 20 consistent with the NIMH Fast-Fail Trial for Mood and Anxiety Disorders, corresponding to clinically impairing anhedonia.
- •Psychosis severity inclusion criteria and stratification: Participants will be stratified according to scores on the psychotic subscale of the Brief Psychiatric Rating Scale (BPRS)
- •Willingness to adhere to the estradiol regimen
Exclusion Criteria
- •Pregnancy; allergies to any active or inactive ingredients in the Climara® patch or Prometrium®.
- •BMI \< 18 or \> 35 kg/m\^2
- •A history of chronic menstrual cycle irregularity, meaning \> 1 year without menses
- •MR contraindications: Metal in the body, dental work other than fillings or gold, tattoos, metal injury, any other implant unless they are 100% plastic.
- •PET contradictions: participation in \>1 research study in the past 12 months that included ionizing radiation exceeding 3 rem to the whole body (e.g., PET, CT). Standard of care imaging is not exclusionary.
- •The use of psychotropics or hormonal preparations.
- •History of psychiatric illness during the 2 years before the onset of perimenopause.
- •History of chronic, recurrent mood or psychotic disorders (i.e., more than one non-reproductive-related mood episode prior to the perimenopausal index episode).
- •A history of mood episodes requiring hospitalization.
- •Current mania;
Arms & Interventions
Perimenopausal women with mild-to-moderate anhedonia + absent-to-mild psychosis, active group
Participants will be randomly assigned to take 100 μg/day of transdermal estradiol for 3 weeks followed by 1 week of combined 100 μg/day of transdermal estradiol and 200 mg/day progesterone.
Intervention: Micronized Progesterone
Perimenopausal women with mild-to-moderate anhedonia + moderate psychosis, active group
Participants will be randomly assigned to take 100 μg/day of transdermal estradiol for 3 weeks followed by 1 week of combined 100 μg/day of transdermal estradiol and 200 mg/day progesterone.
Intervention: Transdermal Estradiol
Perimenopausal women with mild-to-moderate anhedonia + moderate psychosis, active group
Participants will be randomly assigned to take 100 μg/day of transdermal estradiol for 3 weeks followed by 1 week of combined 100 μg/day of transdermal estradiol and 200 mg/day progesterone.
Intervention: Micronized Progesterone
Perimenopausal women with mild-to-moderate anhedonia + moderate psychosis, placebo group
Participants will be randomly assigned to receive a matching placebo patch for 3 weeks.
Intervention: Matching Placebo Patch
Perimenopausal women with high anhedonia + absent-to-mild psychosis, placebo group
Participants will be randomly assigned to receive a matching placebo patch for 3 weeks.
Intervention: Matching Placebo Patch
Perimenopausal women with high anhedonia + moderate psychosis, active group
Participants will be randomly assigned to take 100 μg/day of transdermal estradiol for 3 weeks followed by 1 week of combined 100 μg/day of transdermal estradiol and 200 mg/day progesterone.
Intervention: Transdermal Estradiol
Perimenopausal women with high anhedonia + moderate psychosis, placebo group
Participants will be randomly assigned to receive a matching placebo patch for 3 weeks.
Intervention: Matching Placebo Patch
Perimenopausal women with mild-to-moderate anhedonia + absent-to-mild psychosis, active group
Participants will be randomly assigned to take 100 μg/day of transdermal estradiol for 3 weeks followed by 1 week of combined 100 μg/day of transdermal estradiol and 200 mg/day progesterone.
Intervention: Transdermal Estradiol
Perimenopausal women with mild-to-moderate anhedonia + absent-to-mild psychosis, active group
Participants will be randomly assigned to take 100 μg/day of transdermal estradiol for 3 weeks followed by 1 week of combined 100 μg/day of transdermal estradiol and 200 mg/day progesterone.
Intervention: Raclopride C11
Perimenopausal women with mild-to-moderate anhedonia + absent-to-mild psychosis, placebo group
Participants will be randomly assigned to receive a matching placebo patch for 3 weeks.
Intervention: Raclopride C11
Perimenopausal women with mild-to-moderate anhedonia + moderate psychosis, active group
Participants will be randomly assigned to take 100 μg/day of transdermal estradiol for 3 weeks followed by 1 week of combined 100 μg/day of transdermal estradiol and 200 mg/day progesterone.
Intervention: Raclopride C11
Perimenopausal women with mild-to-moderate anhedonia + moderate psychosis, placebo group
Participants will be randomly assigned to receive a matching placebo patch for 3 weeks.
Intervention: Raclopride C11
Perimenopausal women with high anhedonia + absent-to-mild psychosis, active group
Participants will be randomly assigned to take 100 μg/day of transdermal estradiol for 3 weeks followed by 1 week of combined 100 μg/day of transdermal estradiol and 200 mg/day progesterone.
Intervention: Raclopride C11
Perimenopausal women with high anhedonia + absent-to-mild psychosis, placebo group
Participants will be randomly assigned to receive a matching placebo patch for 3 weeks.
Intervention: Raclopride C11
Perimenopausal women with high anhedonia + moderate psychosis, active group
Participants will be randomly assigned to take 100 μg/day of transdermal estradiol for 3 weeks followed by 1 week of combined 100 μg/day of transdermal estradiol and 200 mg/day progesterone.
Intervention: Raclopride C11
Perimenopausal women with high anhedonia + moderate psychosis, placebo group
Participants will be randomly assigned to receive a matching placebo patch for 3 weeks.
Intervention: Raclopride C11
Perimenopausal women with mild-to-moderate anhedonia + absent-to-mild psychosis, placebo group
Participants will be randomly assigned to receive a matching placebo patch for 3 weeks.
Intervention: Matching Placebo Patch
Perimenopausal women with high anhedonia + absent-to-mild psychosis, active group
Participants will be randomly assigned to take 100 μg/day of transdermal estradiol for 3 weeks followed by 1 week of combined 100 μg/day of transdermal estradiol and 200 mg/day progesterone.
Intervention: Transdermal Estradiol
Perimenopausal women with high anhedonia + absent-to-mild psychosis, active group
Participants will be randomly assigned to take 100 μg/day of transdermal estradiol for 3 weeks followed by 1 week of combined 100 μg/day of transdermal estradiol and 200 mg/day progesterone.
Intervention: Micronized Progesterone
Perimenopausal women with high anhedonia + moderate psychosis, active group
Participants will be randomly assigned to take 100 μg/day of transdermal estradiol for 3 weeks followed by 1 week of combined 100 μg/day of transdermal estradiol and 200 mg/day progesterone.
Intervention: Micronized Progesterone
Outcomes
Primary Outcomes
Changes in Striatal Activation Between Groups during the MID task
Time Frame: Baseline (week 3) to Endpoint (week 7)
Characterize reward-related striatal activation measured by fMRI using the Monetary Incentive Delay (MID) task to elicit blood-oxygen-level dependent (BOLD) responses. During MID the task, participants respond to "win" trials by pressing a button on a button box in the MRI as quickly as possible when the see a target. Reactivity is measured by examining participant's change in blood-oxygen-level dependent (BOLD) response to win trials versus non-win trials. Reactivity is then compared between the two groups.
Secondary Outcomes
- Changes in PO Psychosis Symptoms following Estradiol Administration Using the BPRS(Baseline (week 3) to Endpoint (week 7))
- Changes in PO Anhedonia Following Estradiol Administration Using the SHAPS(Baseline (week 3) to Endpoint (week 7))
- Change in striatal phasic DA release and background DA tone to rewards measured by [11C]raclopride PET using the Monetary Incentive Delay (MID) task.(Baseline (week 3) to Endpoint (week 7))