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HIV-1 Tat 促进了雌性小鼠与年龄相关的认知、焦虑样和抗伤害感受损伤,这种损伤可被衰老和内分泌状态所调节。

HIV-1 Tat promotes age-related cognitive, anxiety-like, and antinociceptive impairments in female mice that are moderated by aging and endocrine status.

机构信息

Department of BioMolecular Sciences, School of Pharmacy, University of Mississippi, 315 Faser Hall, P.O. Box 1848, University, MS, 38677-1848, USA.

Department of Psychiatry, McLean Imaging Center, McLean Hospital/Harvard Medical School, Belmont, MA, 02478, USA.

出版信息

Geroscience. 2021 Feb;43(1):309-327. doi: 10.1007/s11357-020-00268-z. Epub 2020 Sep 17.

Abstract

Hypogonadism is a common comorbidity associated with HIV-1 that is more prevalent among infected individuals over the age of 45. The underlying mechanisms are unknown, but both combined antiretroviral therapeutics and HIV-1 proteins, such as trans-activator of transcription protein (Tat), dysregulate steroid-synthetic mechanisms including lipid storage/synthesis and mitochondrial function. Thus, Tat expression may accelerate age-related comorbidities partly by impairing endocrine function. Few studies exist of Tat-mediated behavioral deficits in aged animals and effects of endocrine status have not been investigated. Accordingly, we tested whether conditional Tat expression in aged (~ 1.5 years old), female, Tat-transgenic [Tat(+)] mice increases anxiety-like behavior, impairs cognition, and augments mechanical allodynia, when compared to age-matched controls that do not express Tat protein [Tat(-)]. We further tested whether aged mice that maintained their endocrine status (pre-estropausal) were more resilient to Tat/age-related comorbidities than peri- or post-estropausal mice. Tat and endocrine aging status exerted separate and interacting effects that influenced anxiety-like and cognitive behaviors. Peri- and post-estropausal mice exhibited greater anxiety-like behavior in the elevated plus-maze and impaired learning in the radial arm water maze compared to pre-estropausal mice. Irrespective of estropause status, Tat(+) mice demonstrated impaired learning, reduced grip strength, and mechanical allodynia compared to Tat(-) mice. Tat exposure reduced circulating estradiol in post-estropausal mice and increased the estradiol-to-testosterone ratio in pre-estropausal mice. Changes in circulating estradiol, testosterone, and progesterone correlated with grip strength. Thus, endocrine status is an important factor in age-related anxiety, cognition, neuromuscular function, and allodynia that can be accelerated by HIV-1 Tat protein.

摘要

性腺功能减退症是一种与 HIV-1 相关的常见合并症,在 45 岁以上的感染者中更为普遍。其潜在机制尚不清楚,但联合抗逆转录病毒疗法和 HIV-1 蛋白,如转录激活蛋白(Tat),会使类固醇合成机制失调,包括脂质储存/合成和线粒体功能。因此,Tat 的表达可能通过损害内分泌功能加速与年龄相关的合并症。目前很少有关于老年动物中 Tat 介导的行为缺陷的研究,也没有研究过内分泌状态的影响。因此,我们测试了在老年(~1.5 岁)、雌性、Tat 转基因(Tat(+))小鼠中条件性表达 Tat 是否会增加焦虑样行为、损害认知,并增强机械性痛觉过敏,与不表达 Tat 蛋白的年龄匹配对照(Tat(-))相比。我们进一步测试了维持内分泌状态(未绝经前)的老年小鼠是否比绝经前或绝经后小鼠更能抵抗 Tat/与年龄相关的合并症。Tat 和内分泌衰老状态产生了单独和相互作用的影响,影响了焦虑样和认知行为。绝经前、绝经前和绝经后小鼠在高架十字迷宫中表现出更高的焦虑样行为,在放射臂水迷宫中学习能力受损,与绝经前小鼠相比。与绝经前状态无关,Tat(+)小鼠与 Tat(-)小鼠相比,学习能力受损、握力下降和机械性痛觉过敏。Tat 暴露降低了绝经后小鼠的循环雌二醇水平,并增加了绝经前小鼠的雌二醇/睾酮比值。循环雌二醇、睾酮和孕酮的变化与握力相关。因此,内分泌状态是与年龄相关的焦虑、认知、神经肌肉功能和痛觉过敏的一个重要因素,可被 HIV-1 Tat 蛋白加速。

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