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手术后绝经后用高度选择性孕激素治疗后的记忆、焦虑和生长因子 IGF-1R 的评估。

Evaluations of memory, anxiety, and the growth factor IGF-1R after post-surgical menopause treatment with a highly selective progestin.

机构信息

Department of Psychology, Arizona State University, 950 S. McAllister Ave., Tempe, AZ 85287, USA; Arizona Alzheimer's Consortium, 4745 N 7th St, Phoenix, AZ 85014, USA.

Department of Psychology, Arizona State University, 950 S. McAllister Ave., Tempe, AZ 85287, USA; Arizona Alzheimer's Consortium, 4745 N 7th St, Phoenix, AZ 85014, USA; TGen Institute, 445 N 5th St, Phoenix, AZ 85004, USA.

出版信息

Behav Brain Res. 2023 Jun 25;448:114442. doi: 10.1016/j.bbr.2023.114442. Epub 2023 Apr 20.

Abstract

Progestogens are a key component of menopausal hormone therapies. While some progestogens can be detrimental to cognition, there is preclinical evidence that progestogens with a strong progesterone-receptor affinity benefit some molecular mechanisms believed to underlie cognitive function. Thus, a progestin that maximizes progesterone-receptor affinity and minimizes affinities to other receptors may be cognitively beneficial. We evaluated segesterone-acetate (SGA), a 19-norprogesterone derivative with a strong progesterone-receptor affinity and no androgenic or estrogenic-receptor activity, hypothesizing that it would enhance cognition. Middle-aged rats underwent Sham or Ovariectomy (Ovx) surgery followed by administration of medroxyprogesterone-acetate (MPA; used as a positive control as we have previously shown MPA-induced cognitive deficits), SGA (low or high dose), or vehicle (one Sham and one Ovx group). Spatial working and reference memory, delayed retention, and anxiety-like behavior were assessed, as were memory- and hormone- related protein assays within the frontal cortex, dorsal hippocampus, and entorhinal cortex. Low-dose SGA impaired spatial working memory, while high-dose SGA had a more extensive detrimental impact, negatively affecting spatial reference memory and delayed retention. Replicating previous findings, MPA impaired spatial reference memory and delayed retention. SGA, but not MPA, alleviated Ovx-induced anxiety-like behaviors. On two working memory measures, IGF-1R expression correlated with better working memory only in rats without hormone manipulation; any hormone manipulation or combination of hormone manipulations used herein altered this relationship. These findings suggest that SGA impairs spatial cognition after surgical menopause, and that surgical menopause with or without progestin administration disrupts relationships between a growth factor critical to neuroplasticity.

摘要

孕激素是绝经激素治疗的一个关键组成部分。虽然一些孕激素可能对认知有害,但有临床前证据表明,与其他受体亲和力强的孕激素有益于一些被认为是认知功能基础的分子机制。因此,一种最大限度地提高孕激素受体亲和力并最大限度地降低与其他受体亲和力的孕激素可能对认知有益。我们评估了塞孕酯(SGA),这是一种具有强孕激素受体亲和力且无雄激素或雌激素受体活性的 19-去甲孕酮衍生物,假设它会增强认知。中年大鼠接受假手术(Sham)或卵巢切除术(Ovx)手术,然后给予醋酸甲羟孕酮(MPA;用作阳性对照,因为我们之前已经表明 MPA 引起认知缺陷)、SGA(低或高剂量)或载体(Sham 和 Ovx 各一组)。评估空间工作和参考记忆、延迟保留以及焦虑样行为,同时评估额叶皮质、背海马和内嗅皮质中的记忆和激素相关蛋白。SGA 低剂量组损害空间工作记忆,而 SGA 高剂量组则产生更广泛的不利影响,对空间参考记忆和延迟保留产生负面影响。与之前的发现一致,MPA 损害空间参考记忆和延迟保留。SGA 但不是 MPA 减轻了 Ovx 诱导的焦虑样行为。在两项工作记忆测量中,IGF-1R 表达与未经激素处理的大鼠的工作记忆更好相关;任何激素处理或本文中使用的激素处理组合都会改变这种关系。这些发现表明,SGA 会在手术绝经后损害空间认知,并且手术绝经加上孕激素的使用或不使用都会破坏对神经可塑性至关重要的生长因子之间的关系。

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