17β-雌二醇水平改变雌性大鼠NMDAR功能和抗精神病样活性

IF 9.6 1区医学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY

Molecular Psychiatry Pub Date : 2025-04-04 DOI:10.1038/s41380-025-02996-0

Kimberly M. Holter, McKenna G. Klausner, Mary Hunter Hite, Carson T. Moriarty, Samuel H. Barth, Bethany E. Pierce, Alexandria N. Iannucci, Douglas J. Sheffler, Nicholas D. P. Cosford, Heather A. Bimonte-Nelson, Kimberly F. Raab-Graham, Robert W. Gould

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引用次数: 0

摘要

育龄女性的17β-雌二醇（E2）水平较低，且随着绝经期E2水平明显下降，导致精神分裂症症状严重程度加重（即认知功能障碍），对抗精神病药物的反应减弱。然而，其潜在机制尚不清楚。n -甲基- d -天冬氨酸受体（NMDAR）功能低下与精神分裂症的病理生理有关，但E2缺失对NMDAR功能的影响尚不清楚。定量脑电图（qEEG），特别是伽马功率，是一种公认的大脑皮层活动的功能读数，精神分裂症患者的大脑皮层活动升高，对NMDAR功能的改变很敏感。通过qEEG和触摸屏认知评估，本研究通过给去卵巢大鼠注射MK-801 （NMDAR拮抗剂）来研究E2对NMDAR功能的影响，这些大鼠分别植入或不植入E2 （Ovx+E和Ovx）。与Ovx+E大鼠相比，Ovx大鼠对mk -801诱导的伽马能量升高和注意力损伤更敏感。进一步的研究表明，这些作用是由突触GluN2A表达减少介导的。与临床报告一致，奥氮平（第二代抗精神病药）在缓解mk -801诱导的Ovx大鼠γ功率升高方面效果较差。最后，我们检测了II组代谢性谷氨酸受体（mGlu2/3）阳性变构调节剂（PAM） SBI-0646535的抗精神病样活性，作为e2剥夺条件下的一种新型治疗药物。SBI-0646535逆转了mk -801诱导的γ功率升高，无论E2状态如何。总的来说，这些研究建立了E2剥夺与NMDAR功能之间的关系，这种关系部分依赖于glun2a，支持E2剥夺增加NMDAR功能减退的易感性的观点。这强调了在考虑抗精神病反应和设计新的药物治疗时，需要检查年龄/激素特异性因素。

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17β-estradiol status alters NMDAR function and antipsychotic-like activity in female rats

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17β-estradiol status alters NMDAR function and antipsychotic-like activity in female rats

Low 17β-estradiol (E2) in females of reproductive age, and marked E2 decline with menopause, contributes to heightened symptom severity in schizophrenia (i.e. cognitive dysfunction) and diminished response to antipsychotic medications. However, the underlying mechanisms are unknown. N-methyl-D-aspartate receptor (NMDAR) hypofunction contributes to the pathophysiology of schizophrenia, yet impact of E2 depletion on NMDAR function is not well characterized. Quantitative electroencephalography (qEEG), specifically gamma power, is a well-established functional readout of cortical activity that is elevated in patients with schizophrenia and is sensitive to alterations in NMDAR function. Using qEEG and touchscreen cognitive assessments, present studies investigated the effects of E2 on NMDAR function by administering MK-801 (NMDAR antagonist) to ovariectomized rats with or without E2 implants (Ovx+E and Ovx, respectively). Ovx rats were more sensitive to MK-801-induced elevations in gamma power and attentional impairments compared to Ovx+E rats. Further investigation revealed these effects were mediated by reduced synaptic GluN2A expression. Consistent with clinical reports, olanzapine (second-generation antipsychotic) was less effective in mitigating MK-801-induced elevations in gamma power in Ovx rats. Lastly, we examined antipsychotic-like activity of a Group II metabotropic glutamate receptor (mGlu_2/3) positive allosteric modulator (PAM), SBI-0646535, as a novel therapeutic in E2-deprived conditions. SBI-0646535 reversed MK-801-induced elevations in gamma power regardless of E2 status. Collectively, these studies established a relationship between E2 deprivation and NMDAR function that is in part GluN2A-dependent, supporting the notion that E2 deprivation increases susceptibility to NMDAR hypofunction. This highlights the need to examine age/hormone-specific factors when considering antipsychotic response and designing novel pharmacotherapies.

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来源期刊

Molecular Psychiatry 医学-精神病学

CiteScore

20.50

自引率

4.50%

发文量

459

审稿时长

4-8 weeks

期刊介绍： Molecular Psychiatry focuses on publishing research that aims to uncover the biological mechanisms behind psychiatric disorders and their treatment. The journal emphasizes studies that bridge pre-clinical and clinical research, covering cellular, molecular, integrative, clinical, imaging, and psychopharmacology levels.