经前烦躁不安障碍/经前综合征的认识和治疗的最新进展

Faculty reviews Pub Date : 2022-04-28 DOI:10.12703/r/11-11
L. Tiranini, R. Nappi
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引用次数: 18

摘要

经前综合症(PMS)和经前烦躁不安障碍(PMDD)是月经周期黄体期常见的疾病,其特征是中度至重度身体、情感或行为症状,损害日常活动和生活质量。经前症候群和经前不悦症最近在研究界引起了极大的兴趣,因为它们在全球相当普遍。经前综合症/经前不悦症的病因是复杂的。卵巢生殖类固醇(雌二醇和黄体酮)被认为是致病效应物,但关键特征似乎是gaba能中枢抑制系统对异孕酮的敏感性改变,异孕酮是排卵后产生的黄体酮衍生的神经类固醇。此外,血清素的减少似乎也与此有关。新的见解指出了激素和神经递质通路的遗传和表观遗传修饰的作用,炎症是外周和神经系统对压力源的综合反应之间的潜在联系。因此,新的治疗PMS/PMDD的方法包括抑制大脑中的孕酮受体(即,用醋酸乌普利司妥),用杜他雄胺减少孕酮向其代谢物异孕酮的转化,以及用舍普诺酮可能调节异孕酮对脑gaba能系统的作用。需要进一步的研究来更好地了解外周炎症分子(细胞因子、白细胞介素、c反应蛋白和活性氧)与经前症候群/经前不悦症女性脑神经递质系统之间的相互作用。如果得到证实,神经炎症可能会导致开发靶向抗炎疗法,并确定PMS/PMDD相关慢性炎症风险的预防策略。最后,观察到的经前紊乱和心理疾病之间的联系可以指导及时和充分的干预措施,以实现更好的生活质量。
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Recent advances in understanding/management of premenstrual dysphoric disorder/premenstrual syndrome
Premenstrual syndrome (PMS) and premenstrual dysphoric disorder (PMDD) are common disorders of the luteal phase of the menstrual cycle and are characterized by moderate to severe physical, affective, or behavioral symptoms that impair daily activities and quality of life. PMS and PMDD have recently raised great interest in the research community for their considerable global prevalence. The etiology of PMS/PMDD is complex. Ovarian reproductive steroids (estradiol and progesterone) are considered pathogenetic effectors, but the key feature seems to be an altered sensitivity of the GABAergic central inhibitory system to allopregnanolone, a neurosteroid derived from progesterone produced after ovulation. Also, a reduced availability of serotonin seems to be involved. New insights point to a role for genetic and epigenetic modifications of hormonal and neurotransmitter pathways, and inflammation is the potential link between peripheral and neurological integrated responses to stressors. Thus, new therapeutic approaches to PMS/PMDD include inhibition of progesterone receptors in the brain (i.e., with ulipristal acetate), reduced conversion of progesterone to its metabolite allopregnanolone with dutasteride, and possible modulation of the action of allopregnanolone on the brain GABAergic system with sepranolone. Further research is needed to better understand the interaction between peripheral inflammatory molecules (cytokines, interleukins, C-reactive protein, and reactive oxygen species) and the brain neurotransmitter systems in women with PMS/PMDD. If confirmed, neuroinflammation could lead both to develop targeted anti-inflammatory therapies and to define prevention strategies for the associated chronic inflammatory risk in PMS/PMDD. Finally, the observed association between premenstrual disorders and psychological diseases may guide prompt and adequate interventions to achieve a better quality of life.
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