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Neuropsychobiological Correlates of Sex-steroid Hormone Manipulation in Healthy Women: a Risk Model for Depression (GnRHa)

Primary Purpose

Postpartum Depression, Major Depressive Disorder, Postpartum Psychosis

Status
Completed
Phase
Not Applicable
Locations
Denmark
Study Type
Interventional
Intervention
Goserelin 3.6 mg implant
Placebo
Sponsored by
Gitte Moos Knudsen
About
Eligibility
Locations
Arms
Outcomes
Full info

About this trial

This is an interventional basic science trial for Postpartum Depression focused on measuring Mental health, Brain Imaging, Steroid hormones, Serotonin, PET, MRI, fMRI, human, gender, risk model

Eligibility Criteria

18 Years - 40 Years (Adult)FemaleAccepts Healthy Volunteers

Inclusion Criteria:

  • Healthy women
  • Regular menstrual cycles (23 -35 days cycle length)
  • No systemic or intrauterine steroid hormone use

Exclusion Criteria:

  • Psychiatric disorder (DSM IV Axis I or WHO ICD-10 diagnostic classification).
  • Prior or present neurological or other severe medical condition including substance abuse.
  • No drug intake suspected to influence results
  • Conditions that may increase risk by participating in the study program including ovarian cysts
  • Pregnancy during the last year
  • Delivery during the last 2 years
  • Presently wishing to obtain pregnancy
  • Breast feeding
  • Not fluent in Danish or severe visual or hearing impairments
  • Earlier or present learning disabilities
  • Claustrophobia (due to MRI scans)
  • Metal implants (excludes MRI)

Sites / Locations

  • Neurobiology Research Unit, Rigshospitalet

Arms of the Study

Arm 1

Arm 2

Arm Type

Active Comparator

Placebo Comparator

Arm Label

GnRHa

Placebo

Arm Description

Goserelin 3.6 mg implant

Injection of saline

Outcomes

Primary Outcome Measures

Changes from baseline in symptoms of depression
Hamilton 17 item score
Changes from baseline in serotonin transporter binding in volumes of interest (VOIs)
PET scan assessed serotonin transporter binding changes
Changes from baseline in fMRI response to emotional faces
fMRI response changes to emotional faces in emotion processing network including amygdala reactivity
Changes from baseline in fMRI response to gambling paradigm
fMRI response changes to reward (monetary win) paradigm in reward processing network
Changes from baseline in rsfMRI changes in functional connectivity
rsfMRI changes in functional connectivity in response to intervention
Changes from baseline in affective cognition (VAMT-24 test)
Neuropsychological (VAMT-24 test) outcomes on affective cognition
Changes from baseline in reaction time
Changes in reaction time
Serial mood fluctuations (SD of total mood disturbance (TMD) score of daily POMS across intervention period)
Mood fluctuations measured by serial collection of daily POMS
Changes from baseline in hippocampal volume
Hippocampal volumes from structural MRI
Changes in pre-pulse-inhibition (PPI) from baseline
Change in amplitude of the startle response to pulse after pre-pulse warning as measured by EMG in the orbicularis oculi muscle (subtraction of averages across a series of 10 repititions at baseline and at follow-up 16±3 days).
Changes in a set of markers of immunoactivity across study period
Cytokines, hsCRP and gene transcript profile markers of
Changes in epigenetic markers of estrogen sensitivity
Epigenetic (methylation) markers
Changes in HPA-axis dynamics (the cortisol awakening response)
The cortical awakening response
Changes in sensorimotor gating (P50 suppression) from baseline
Changes in sensorimotor gating (P50 suppression) from baseline
Changes from baseline in hippocampal microstructure
Hippocampal microstructure from MRI

Secondary Outcome Measures

Changes from baseline in fMRI responses to emotional memory paradigm
Changes in brain activation to fMRI emotional memory paradigm - delayed recall forgetting of word prior to emotional disturbance
Changes from baseline in Cohens perceived stress score
Changes Cohens perceived stress score
Changes in Pittsburg Sleep Quality Inventory (PSQI)
Sleep quality self reported weekly across intervention period
Side effects scores (project specific 15 items questionnaire)
Total side effect score across and after intervention period
Changes in SCL-R (Symptom check-list revised)
Changes in symptoms of psychopathology across intervention period
Major Depression Inventory (MDI)
Changes in self-reported symptoms of depression across intervention period
Changes in profile of mood states (POMS TMD score)
Changes in self-reported symptoms of mental distress across intervention period

Full Information

First Posted
January 13, 2016
Last Updated
January 19, 2016
Sponsor
Gitte Moos Knudsen
Collaborators
Center for Integrated Molecular Brain Imaging, Copenhagen, Denmak, Fertility Clinic Rigshospitalet, CNSR, Glostrup Psychiatric Center, Danish Multiple Sclerosis Center Rigshospitalet, Dept. of Clinical Immunology, Rigshospitalet
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1. Study Identification

Unique Protocol Identification Number
NCT02661789
Brief Title
Neuropsychobiological Correlates of Sex-steroid Hormone Manipulation in Healthy Women: a Risk Model for Depression
Acronym
GnRHa
Official Title
Neuropsychobiological Correlates of Sex-steroid Hormone Manipulation in Healthy Women: a Risk Model for Depression
Study Type
Interventional

2. Study Status

Record Verification Date
January 2016
Overall Recruitment Status
Completed
Study Start Date
January 2011 (undefined)
Primary Completion Date
December 2012 (Actual)
Study Completion Date
December 2012 (Actual)

3. Sponsor/Collaborators

Responsible Party, by Official Title
Sponsor-Investigator
Name of the Sponsor
Gitte Moos Knudsen
Collaborators
Center for Integrated Molecular Brain Imaging, Copenhagen, Denmak, Fertility Clinic Rigshospitalet, CNSR, Glostrup Psychiatric Center, Danish Multiple Sclerosis Center Rigshospitalet, Dept. of Clinical Immunology, Rigshospitalet

4. Oversight

Data Monitoring Committee
Yes

5. Study Description

Brief Summary
The project aimed at identifying neuropsychobiological signatures of pharmacological sex-steroid hormone manipulations in healthy women as a risk model for depression. The study is a double-blind, randomized, placebo-controlled study. Investigators included 63 healthy female volunteers with regular menstrual cycles between 23 and 35 days. Participants were randomized to active Gonadotrophin-Releasing-Hormone agonist (GnRHa) (goserelin 3.6 mg implant) or placebo (saline injection) intervention, which was initiated in the mid follicular phase (i.e. cycle day 22.6 ±2.5). Sixty women completed follow-up and entered the analyses, except for a few drop outs on some domains. The following domains were addressed at baseline and at follow-up (16±3 days post intervention), (which corresponded to the early ovarian suppression phase of the biphasic hormone response to GnRHa): 1) serotonin transporter binding as imaged by 11CDASB Positron Emission Tomography (PET), 2) functional Magnetic Resonance Imaging (fMRI) emotional processing, 3) fMRI reward processing, 3) rating state fMRI (rsfMRI), 4) structural MRI, 5) Neuropsychology, 6) Psychophysiology, 7) Hypothalamus-Pituitary-Adrenal cortex (HPA)-axis dynamics, 8) Peripheral markers of immunoactive cell responses, 9) Epigenetic factors. Psychometrics in terms of self reported mental distress and interview based ratings were monitored across the intervention period to monitor potential symptoms of mental distress and psychopathology. Also ovarian hormone responses, peripheral blood markers, and side effects scores were collected across the intervention period.
Detailed Description
Aims and hypotheses: Gender matters in normal brain function as well as in neuropsychiatric disorders. E.g. the vulnerability to mood and anxiety disorders is considerably greater in women. Among other factors, this possibly reflects gender differences in central serotonergic function since dysfunction of serotonergic neurotransmission is critically involved in the pathophysiology of mood and anxiety disorders, schizophrenia, and Alzheimer's disease. In particular, women going through phases in life where sex hormones decline rapidly from high levels or fluctuate, have a higher frequency of severe mood state changes and are more vulnerable to psychiatric disorders, e.g. across the pre to postpartum and menopausal transition. Interestingly, this risk is associated with increased variability of the plasma levels of the sex-hormone estradiol. Therefore, sex-hormone manipulation with a pharmacologically induced biphasic ovarian hormone response serve as a unique opportunity to study how sex-hormone fluctuations provoke mood state changes and increase vulnerability to neuropsychiatric disorders. In this project investigators aimed at investigating whether sex-hormone manipulation affects: 1. Molecular imaging markers of serotonergic neurotransmission in vivo, 2. Brain structure, architecture and functional connectivity, 3. Stress and inflammatory responses, and 4. Cognitive functions, emotional processing, and information filtering, of importance in the pathophysiology of neuropsychiatric disorders. Mentally healthy female volunteers were assessed at baseline (i.e cycle day 6.6 ±2.2) and at follow-up (i.e 16.2 ±2.6 days post intervention) in the early ovarian suppression phase af a Gonadotrophin-Releasing-Hormone agonist response in a placebo-controlled, double-blinded design (cohort size aim: N=30x2). Research in neurobiological correlates of vulnerability related to sex-hormone changes is pivotal to improve the etiological understanding of brain disorders with gender differences in their incidence and/or nature. Such research may contribute to ameliorate fertility treatment, to improve treatment of mood disorders and schizophrenia, and, ideally, shed light on possible preventive strategies in vulnerable phases of women's lives such as the pre- to post-partum and menopausal transition period. Hypotheses: Investigators hypothesised that sex-hormone manipulation is associated with the following: 1. Compromised serotonergic neurotransmission, 2. Changes in functional and structural connectivity and lower hippocampal brain volumes and/or markers of decreased neurogenesis, 3. Increased stress reactivity and inflammatory responses, and 4. Changes in neurocognitive functioning and negative bias in emotional processing and information filtering. Investigators further hypothesised that these changes occur in a manner dependent on the magnitude of the estradiol drop from baseline and dependent on symptoms of depressed and anxious mood. General study design: The study is a prospective, double-blinded, placebo-controlled, combined within-subject and between-group design of neuropsychobiological changes in response to hormonal down-regulation. The investigation program will be performed at baseline in the mid-follicular phase, at day 5-8 of the menstrual cycle, and in the down-regulated state, 14-19 days after GnRHa intervention. Participants. Investigators aimed at including 60 healthy female volunteers, in the age range 18-40 years. Group 1 (N=30) will receive sex-hormone manipulation with GnRHa, and group 2 (N=30) will receive placebo (saline injection). The inclusion will be stratified according to a polymorphism in the serotonin transporter promoter region (5-HTLPR). The investigation program includes functional brain imaging of the serotonin transporter with [11C]DASB PET (6) and fMRI, structural brain imaging, blood measurements of sex-hormone levels, inflammatory and epigenetic biomarkers, characterization of the cortisol awakening response, and psychophysiological measures of information processing, and monitoring of symptoms of mental distress and psychopathology across the intervention period. An initial screening program will secure inclusion of healthy controls only and determine trait parameters such as genotypes, IQ and personality measures. The study was registered at and approved by the Danish Ethical Committee before participant inclusion under the protocol identification number: H-2-2010-108. All participants gave written informed consent.

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study
Postpartum Depression, Major Depressive Disorder, Postpartum Psychosis, Menopause, Neurodegeneration, Schizophrenia
Keywords
Mental health, Brain Imaging, Steroid hormones, Serotonin, PET, MRI, fMRI, human, gender, risk model

7. Study Design

Primary Purpose
Basic Science
Study Phase
Not Applicable
Interventional Study Model
Parallel Assignment
Masking
ParticipantCare ProviderInvestigatorOutcomes Assessor
Allocation
Randomized
Enrollment
63 (Actual)

8. Arms, Groups, and Interventions

Arm Title
GnRHa
Arm Type
Active Comparator
Arm Description
Goserelin 3.6 mg implant
Arm Title
Placebo
Arm Type
Placebo Comparator
Arm Description
Injection of saline
Intervention Type
Drug
Intervention Name(s)
Goserelin 3.6 mg implant
Other Intervention Name(s)
Zoladex
Intervention Description
Pharmacologically induced biphasic sex-steroid hormone fluctuation
Intervention Type
Drug
Intervention Name(s)
Placebo
Other Intervention Name(s)
Saline
Intervention Description
Injection of saline
Primary Outcome Measure Information:
Title
Changes from baseline in symptoms of depression
Description
Hamilton 17 item score
Time Frame
Baseline to follow-up 16±3 days after intervention
Title
Changes from baseline in serotonin transporter binding in volumes of interest (VOIs)
Description
PET scan assessed serotonin transporter binding changes
Time Frame
Baseline to follow-up 16±3 days after intervention
Title
Changes from baseline in fMRI response to emotional faces
Description
fMRI response changes to emotional faces in emotion processing network including amygdala reactivity
Time Frame
Baseline to follow-up 16±3 days after intervention
Title
Changes from baseline in fMRI response to gambling paradigm
Description
fMRI response changes to reward (monetary win) paradigm in reward processing network
Time Frame
Baseline to follow-up 16±3 days after intervention
Title
Changes from baseline in rsfMRI changes in functional connectivity
Description
rsfMRI changes in functional connectivity in response to intervention
Time Frame
Baseline to follow-up 16±3 days after intervention
Title
Changes from baseline in affective cognition (VAMT-24 test)
Description
Neuropsychological (VAMT-24 test) outcomes on affective cognition
Time Frame
Baseline to follow-up 16±3 days after intervention
Title
Changes from baseline in reaction time
Description
Changes in reaction time
Time Frame
Baseline to follow-up 16±3 days after intervention
Title
Serial mood fluctuations (SD of total mood disturbance (TMD) score of daily POMS across intervention period)
Description
Mood fluctuations measured by serial collection of daily POMS
Time Frame
Intervention start to follow-up 16±3 days after intervention
Title
Changes from baseline in hippocampal volume
Description
Hippocampal volumes from structural MRI
Time Frame
Baseline to follow-up 16±3 days after intervention
Title
Changes in pre-pulse-inhibition (PPI) from baseline
Description
Change in amplitude of the startle response to pulse after pre-pulse warning as measured by EMG in the orbicularis oculi muscle (subtraction of averages across a series of 10 repititions at baseline and at follow-up 16±3 days).
Time Frame
Baseline to follow-up 16±3 days after intervention
Title
Changes in a set of markers of immunoactivity across study period
Description
Cytokines, hsCRP and gene transcript profile markers of
Time Frame
Baseline, intervention time, flare-up phase and follow-up
Title
Changes in epigenetic markers of estrogen sensitivity
Description
Epigenetic (methylation) markers
Time Frame
Baseline to follow-up 16±3 days after intervention
Title
Changes in HPA-axis dynamics (the cortisol awakening response)
Description
The cortical awakening response
Time Frame
Baseline to follow-up 16±3 days after intervention
Title
Changes in sensorimotor gating (P50 suppression) from baseline
Description
Changes in sensorimotor gating (P50 suppression) from baseline
Time Frame
Baseline to follow-up 16±3 days after intervention
Title
Changes from baseline in hippocampal microstructure
Description
Hippocampal microstructure from MRI
Time Frame
Baseline to follow-up 16±3 days after intervention
Secondary Outcome Measure Information:
Title
Changes from baseline in fMRI responses to emotional memory paradigm
Description
Changes in brain activation to fMRI emotional memory paradigm - delayed recall forgetting of word prior to emotional disturbance
Time Frame
Baseline to follow-up 16±3 days after intervention
Title
Changes from baseline in Cohens perceived stress score
Description
Changes Cohens perceived stress score
Time Frame
Baseline to follow-up 16±3 days after intervention
Title
Changes in Pittsburg Sleep Quality Inventory (PSQI)
Description
Sleep quality self reported weekly across intervention period
Time Frame
Baseline and 1 time per week until follow-up at 16 ±3 days
Title
Side effects scores (project specific 15 items questionnaire)
Description
Total side effect score across and after intervention period
Time Frame
7, 12 and 30 days post intervention
Title
Changes in SCL-R (Symptom check-list revised)
Description
Changes in symptoms of psychopathology across intervention period
Time Frame
Baseline and 1 time per week from intervention to follow up at 16±3 days post intervention
Title
Major Depression Inventory (MDI)
Description
Changes in self-reported symptoms of depression across intervention period
Time Frame
Baseline and 1 time per week from intervention to follow up at 16±3 days post intervention
Title
Changes in profile of mood states (POMS TMD score)
Description
Changes in self-reported symptoms of mental distress across intervention period
Time Frame
Baseline and 1 time per week from intervention to follow up at 16±3 days post intervention
Other Pre-specified Outcome Measures:
Title
Ovarian hormone responses to intervention
Description
Ovarian hormone responses to intervention, i.e. concentrations of estradiol, progesterone and testosterone in peripheral blood)
Time Frame
Baseline (i.e, cycle day 5-8), intervention time (i.e cycle day 21-23), flare-up phase (i.e, 3-4 days post intervention) and follow-up (i.e.,16±3 days post intervention)

10. Eligibility

Sex
Female
Minimum Age & Unit of Time
18 Years
Maximum Age & Unit of Time
40 Years
Accepts Healthy Volunteers
Accepts Healthy Volunteers
Eligibility Criteria
Inclusion Criteria: Healthy women Regular menstrual cycles (23 -35 days cycle length) No systemic or intrauterine steroid hormone use Exclusion Criteria: Psychiatric disorder (DSM IV Axis I or WHO ICD-10 diagnostic classification). Prior or present neurological or other severe medical condition including substance abuse. No drug intake suspected to influence results Conditions that may increase risk by participating in the study program including ovarian cysts Pregnancy during the last year Delivery during the last 2 years Presently wishing to obtain pregnancy Breast feeding Not fluent in Danish or severe visual or hearing impairments Earlier or present learning disabilities Claustrophobia (due to MRI scans) Metal implants (excludes MRI)
Overall Study Officials:
First Name & Middle Initial & Last Name & Degree
Vibe G Frokjaer, MD, Phd
Organizational Affiliation
Neurobiology Research Unit
Official's Role
Principal Investigator
Facility Information:
Facility Name
Neurobiology Research Unit, Rigshospitalet
City
Copenhagen
ZIP/Postal Code
2100
Country
Denmark

12. IPD Sharing Statement

Plan to Share IPD
Yes
IPD Sharing Plan Description
Via database of Center for Integrated Molecular Brain Imaging (Knudsen et al 2016, NeuroImage) data will be available for neuroscience research community contingent on approval by scientific board
Citations:
PubMed Identifier
31099405
Citation
Mehta D, Rex-Haffner M, Sondergaard HB, Pinborg A, Binder EB, Frokjaer VG. Genome-wide gene expression in a pharmacological hormonal transition model and its relation to depressive symptoms. Acta Psychiatr Scand. 2019 Jul;140(1):77-84. doi: 10.1111/acps.13038. Epub 2019 May 24.
Results Reference
derived
PubMed Identifier
27649641
Citation
Fisher PM, Larsen CB, Beliveau V, Henningsson S, Pinborg A, Holst KK, Jensen PS, Svarer C, Siebner HR, Knudsen GM, Frokjaer VG. Pharmacologically Induced Sex Hormone Fluctuation Effects on Resting-State Functional Connectivity in a Risk Model for Depression: A Randomized Trial. Neuropsychopharmacology. 2017 Jan;42(2):446-453. doi: 10.1038/npp.2016.208. Epub 2016 Sep 21.
Results Reference
derived

Learn more about this trial

Neuropsychobiological Correlates of Sex-steroid Hormone Manipulation in Healthy Women: a Risk Model for Depression

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