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缺乏促黄体生成素信号可挽救衰老雌性小鼠的焦虑表型。

Absent LH signaling rescues the anxiety phenotype in aging female mice.

作者信息

Sims Steven, Barak Orly, Ryu Vitaly, Miyashita Sari, Kannangara Hasni, Korkmaz Funda, Wizman Soleil, Macdonald Anne, Gumerova Anisa, Goosens Ki, Zaidi Mone, Yuen Tony, Lizneva Daria, Frolinger Tal

机构信息

Center for Translational Medicine and Pharmacology, Departments of Pharmacological Sciences and of Medicine, Icahn School of Medicine at Mount Sinai, New York, NY, 10029, USA.

出版信息

Mol Psychiatry. 2023 Aug;28(8):3324-3331. doi: 10.1038/s41380-023-02209-6. Epub 2023 Aug 10.

Abstract

Clinical studies and experimental data together support a role for pituitary gonadotropins, including luteinizing hormone (LH), otherwise considered solely as fertility hormones, in age-related cognitive decline. Furthermore, rising levels of LH in post-menopausal women have been implicated in the high prevalence of mood disorders. This study was designed to examine the effect of deficient LH signaling on both cognitive and emotional behavior in 12-month-old Lhcgr mice. For this, we established and validated a battery of five tests, including Dark-Light Box (DLB), Y-Maze Spontaneous Alternation, Novel Object Recognition (NOR), and contextual and cued Fear Conditioning (FCT) tests. We found that 12-month-old female wild type mice display a prominent anxiety phenotype on DLB and FCT. This phenotype was not seen in 12-month-old female Lhcgr mice, indicating full phenotypic rescue. Furthermore, there was no effect of LHCGR depletion on recognition memory or working spatial memory on NOR and Y-maze testing, respectively, in 12-month-old mice, notwithstanding the absence of a basal phenotype in wild type littermates. The latter data do not exclude an effect of LH on cognition documented in previous studies. Finally, 12-month-old male mice and 3-month-old male and female mice did not consistently display deficits on any test. The data collectively document, for the first time, that loss of LH signaling reverses age-related emotional disturbances, a prelude to future targeted therapies that block LH action.

摘要

临床研究和实验数据共同支持垂体促性腺激素(包括促黄体生成素,即LH,以往仅被视为生育激素)在与年龄相关的认知衰退中发挥作用。此外,绝经后女性LH水平升高与情绪障碍的高患病率有关。本研究旨在检测LH信号缺陷对12月龄Lhcgr小鼠认知和情绪行为的影响。为此,我们建立并验证了一组五项测试,包括明暗箱(DLB)、Y迷宫自发交替、新物体识别(NOR)以及情境和线索恐惧条件反射(FCT)测试。我们发现,12月龄雌性野生型小鼠在DLB和FCT测试中表现出显著的焦虑表型。而在12月龄雌性Lhcgr小鼠中未观察到这种表型,表明完全的表型拯救。此外,尽管野生型同窝小鼠不存在基础表型,但在12月龄小鼠中,LHCGR缺失对NOR和Y迷宫测试中的识别记忆或工作空间记忆均无影响。后一项数据并不排除LH对先前研究中所记录的认知有影响。最后,12月龄雄性小鼠以及3月龄雄性和雌性小鼠在任何测试中均未一致表现出缺陷。这些数据首次共同证明,LH信号缺失可逆转与年龄相关的情绪障碍,这是未来阻断LH作用的靶向治疗的前奏。

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