Allopregnanolone-based treatments for postpartum depression: Why/how do they work?

Walton, Najah; Maguire, Jamie

doi:10.1016/j.ynstr.2019.100198

Cited by 75 publications

(72 citation statements)

References 120 publications

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“…The novel medication brexanolone, a neurosteroid that acts as a positive neuromodulator at GABA‐A receptors 133,134 , has been developed for postpartum depression and approved by the US Food and Drug Administration for this condition in 2019 135 . Small RCTs (N=246) compared the efficacy and safety of a 60‐hr brexanolone infusion vs. placebo infusion, with the primary outcome being the mean Hamilton Depression Rating Scale (HAM‐D) score at the end of the infusion period.…”

Section: Interventionsmentioning

confidence: 99%

Perinatal mental health: a review of progress and challenges

2020

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Perinatal mental health has become a significant focus of interest in recent years, with investment in new specialist mental health services in some high‐income countries, and inpatient psychiatric mother and baby units in diverse settings. In this paper, we summarize and critically examine the epidemiology and impact of perinatal mental disorders, including emerging evidence of an increase of their prevalence in young pregnant women. Perinatal mental disorders are among the commonest morbidities of pregnancy, and make an important contribution to maternal mortality, as well as to adverse neonatal, infant and child outcomes. We then review the current evidence base on interventions, including individual level and public health ones, as well as service delivery models. Randomized controlled trials provide evidence on the effectiveness of psychological and psychosocial interventions at the individual level, though it is not yet clear which women with perinatal mental disorders also need additional support for parenting. The evidence base on psychotropic use in pregnancy is almost exclusively observational. There is little research on the full range of perinatal mental disorders, on how to improve access to treatment for women with psychosocial difficulties, and on the effectiveness of different service delivery models. We conclude with research and clinical implications, which, we argue, highlight the need for an extension of generic psychiatric services to include preconception care, and further investment into public health interventions, in addition to perinatal mental health services, potentially for women and men, to reduce maternal and child morbidity and mortality.

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Section: Interventionsmentioning

confidence: 99%

Perinatal mental health: a review of progress and challenges

2020

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“…During pregnancy, increased hormone production has been observed along with enhanced neurosteroid levels, such as allopregnanolone, and transient changes in allopregnanolone concentrations are implicated as a contributing factor to temporary changes in GABA-mediated inhibition, which can result in PPD-associated affective behaviors ( Frye et al, 2011 ; Schüle et al, 2014 ). The therapeutic utility of neurosteroids in other forms of depression, anxiety, and epilepsies are also currently being explored ( Lévesque et al, 2017 ; Czyk, 2019 ; Walton and Maguire, 2019 ; Zorumski et al, 2019 ; Belelli et al, 2020 ). We acknowledge that a variety of neurological and neuropsychiatric conditions involve GABA dysregulation ( Ramamoorthi and Lin, 2011 ; Mele et al, 2019 ), but we have chosen to focus on disorders where GABA A R pharmacology is currently and commonly used: benzodiazepines for epilepsy and anxiety, as well as neurosteroids for PPD.…”

Section: A Brief History On Gaba a Rs As Prolificmentioning

confidence: 99%

Looking for Novelty in an “Old” Receptor: Recent Advances Toward Our Understanding of GABAARs and Their Implications in Receptor Pharmacology

2021

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Diverse populations of GABAA receptors (GABAARs) throughout the brain mediate fast inhibitory transmission and are modulated by various endogenous ligands and therapeutic drugs. Deficits in GABAAR signaling underlie the pathophysiology behind neurological and neuropsychiatric disorders such as epilepsy, anxiety, and depression. Pharmacological intervention for these disorders relies on several drug classes that target GABAARs, such as benzodiazepines and more recently neurosteroids. It has been widely demonstrated that subunit composition and receptor stoichiometry impact the biophysical and pharmacological properties of GABAARs. However, current GABAAR-targeting drugs have limited subunit selectivity and produce their therapeutic effects concomitantly with undesired side effects. Therefore, there is still a need to develop more selective GABAAR pharmaceuticals, as well as evaluate the potential for developing next-generation drugs that can target accessory proteins associated with native GABAARs. In this review, we briefly discuss the effects of benzodiazepines and neurosteroids on GABAARs, their use as therapeutics, and some of the pitfalls associated with their adverse side effects. We also discuss recent advances toward understanding the structure, function, and pharmacology of GABAARs with a focus on benzodiazepines and neurosteroids, as well as newly identified transmembrane proteins that modulate GABAARs.

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“…However, progesterone's impact on dopaminergic transmission seems dependent on baseline estradiol levels as stimulating effects on dopamine release were found in rats which were pre-exposed with estradiol (Becker, 1990a(Becker, , 1990b. Allopregnanolone, a neuroactive steroid, which can be synthesized from steroid hormone precursors, such as progesterone, or synthesized de novo from cholesterol (Walton & Maguire, 2019) has been shown to modulate cognitive functions (Marx et al, 2009), likely due to modulatory effects on GABAergic neurotransmission (Majewska et al, 1986). Just like progesterone and its derivative, GABA levels increase from the follicular to the luteal phase (Epperson et al, 2002).…”

Section: Mechanisms Of Interaction Between Ovarian Hormones Brain Fumentioning

confidence: 99%

Influence of ovarian hormones on value-based decision-making systems: Contribution to sexual dimorphisms in mental disorders

Ambrase

Lewis

Barth

et al. 2021

Frontiers in Neuroendocrinology

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Women and men exhibit differences in behavior when making value-based decisions. Various hypotheses have been proposed to explain these findings, stressing differences in functional lateralization of the brain, functional activation, neurotransmitter involvement and more recently, sex hormones. While a significant interaction of neurotransmitter systems and sex hormones has been shown for both sexes, decision-making in women might be particularly affected by variations of ovarian hormones. In this review we have gathered information from animal and human studies on how ovarian hormones affect decision-making processes in females by interacting with neurotransmitter systems at functionally relevant brain locations and thus modify the computation of decision aspects. We also review previous findings on impaired decision-making in animals and clinical populations with substance use disorder and depression, emphasizing how little we know about the role of ovarian hormones in aberrant decision-making.

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Allopregnanolone-based treatments for postpartum depression: Why/how do they work?

Cited by 75 publications

References 120 publications

Perinatal mental health: a review of progress and challenges

Perinatal mental health: a review of progress and challenges

Looking for Novelty in an “Old” Receptor: Recent Advances Toward Our Understanding of GABAARs and Their Implications in Receptor Pharmacology

Influence of ovarian hormones on value-based decision-making systems: Contribution to sexual dimorphisms in mental disorders

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