An update on approved and emerging drugs for the treatment of postpartum depression.

IF 0.9 4区 医学 Q4 CLINICAL NEUROLOGY Ideggyogyaszati Szemle-Clinical Neuroscience Pub Date : 2024-07-30 DOI:10.18071/isz.77.0227
Elif Asena Çulcu, Şeniz Demiryürek, Abdullah Tuncay Demiryürek
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Abstract

Depression, anxiety and psychotic disorders are common perinatal mental health disorders in the postpartum period. Depressive symptoms that occur postpartum are also present in the prenatal period in 50% of patients. Risk factors for the development of postpartum depression include poor relationship with the partner, lack of social support, mother’s low socioeconomic status and multiparity. It has been determined that reproductive hormones change significantly during peripartum. Progesterone is one of these hormones and acts on the central nervous system starting from the fetal period; neurogenesis, neuromodulation, sedation are some of these effects. It has also been observed that progesterone has positive effects on learning, memory and mood. Progesterone exerts its effects on the central nervous system by converting into its metabolite allopregnanolone. Allopregnanolone is one of the neuroactive steroids, and found in similar amounts in the circulation of pregnant women and fetuses. It acts on synaptic and extrasynaptic γ-aminobutyric acid type A (GABAA) receptors and is a positive allosteric modulator of the GABAA receptor. Allopregnanolone increases both the receptor’s opening frequency and its open duration and improves GABAergic current. Low serum allopregnanolone levels in the second trimester are predictive of postpartum depression. Each 1 ng/mL increase in serum allopregnanolone level reduces the risk of development of postpartum depression by 63%. Brexanolone and zuranolone are synthetic allopregnanolone preparations approved by the FDA for use in female patients with postpartum depression. They act via positive allosteric modulation on the GABAA receptor. Brexanolone is administered via intravenous infusion at varying infusion rates in a healthcare facility over 60 hours. Its effect starts immediately after treatment and continues until the 30th day of follow-up, and depressive mood does not recur. Zuranolone was developed for oral use, and administered as a single dose of 50 mg after a fatty meal. Their effectiveness has been demonstrated in patients with treatment-resistant depression. The development of other novel agents that act on the GABAA receptor and other pathways for the treatment of postpartum depression is in progress.

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关于治疗产后抑郁症的已批准药物和新药的最新情况。
抑郁症、焦虑症和精神病是产后常见的围产期精神疾病。有 50%的患者在产前也会出现产后抑郁症状。产后抑郁症发病的风险因素包括与伴侣关系不佳、缺乏社会支持、母亲社会经济地位低下以及多胎妊娠。已经确定,生殖激素在围产期会发生显著变化。孕酮是这些激素中的一种,从胎儿期开始就作用于中枢神经系统;神经发生、神经调节和镇静是其中的一些作用。还观察到黄体酮对学习、记忆和情绪有积极影响。黄体酮通过转化为其代谢产物异孕酮而对中枢神经系统产生影响。异孕酮是神经活性类固醇之一,在孕妇和胎儿的血液循环中含量相似。它作用于突触和突触外的γ-氨基丁酸 A 型(GABAA)受体,是 GABAA 受体的正异构调节剂。别孕烯醇酮可增加受体的开放频率和开放持续时间,并改善 GABA 能电流。第二孕期血清中的异丙孕酮水平较低可预测产后抑郁症。血清异丙孕酮水平每增加 1 毫微克/毫升,产后抑郁症的发病风险就会降低 63%。Brexanolone 和 Zuranolone 是美国食品及药物管理局批准用于女性产后抑郁症患者的合成异孕酮制剂。它们通过对 GABAA 受体的正异位调节发挥作用。Brexanolone 通过静脉输注的方式在医疗机构中以不同的输注速度给药,持续 60 小时。其疗效在治疗后立即开始,并持续到随访的第 30 天,而且抑郁情绪不会复发。祖拉诺龙被开发为口服药物,单次剂量为 50 毫克,在进食脂肪餐后服用。其疗效已在耐药抑郁症患者中得到证实。用于治疗产后抑郁症的其他作用于 GABAA 受体和其他途径的新型药物的开发工作正在进行中。
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来源期刊
Ideggyogyaszati Szemle-Clinical Neuroscience
Ideggyogyaszati Szemle-Clinical Neuroscience CLINICAL NEUROLOGY-NEUROSCIENCES
CiteScore
1.30
自引率
0.00%
发文量
40
审稿时长
>12 weeks
期刊介绍: The aim of Clinical Neuroscience (Ideggyógyászati Szemle) is to provide a forum for the exchange of clinical and scientific information for a multidisciplinary community. The Clinical Neuroscience will be of primary interest to neurologists, neurosurgeons, psychiatrist and clinical specialized psycholigists, neuroradiologists and clinical neurophysiologists, but original works in basic or computer science, epidemiology, pharmacology, etc., relating to the clinical practice with involvement of the central nervous system are also welcome.
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