Effects of multi-medication treatments including cardiovascular drugs in male and female APPNL-G-F knock in mice

IF 1.9 Q3 CLINICAL NEUROLOGY Cerebral circulation - cognition and behavior Pub Date : 2024-01-01 DOI:10.1016/j.cccb.2024.100309
Francesca Eroli, Christina Tsagkogianni, Stefania Zerial, Felix Andersson, Zeynep Acararicin, Maria Latorre-Leal, Jonas Wastesson, Angel Cedazo-Minguez, Kristina Johnell, Silvia Maioli
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引用次数: 0

Abstract

Objectives

Cardiovascular conditions like hypercholesterolemia and hypertension increase the risk for Alzheimer's Disease (AD). Thus, certain AD risk profiles may benefit from optimized multi- medication therapies including for example cholesterol-lowering and antihypertensive drugs. We previously showed that the drugs most frequently prescribed in older patients in Sweden are compounds from cardiovascular drug classes such as antithrombotic agents, lipid modifying agents, ACE inhibitors, selective calcium channel blockers and are used in combination. In this study we aim to investigate the effects of two multiple-drug regimens in the APPNL-G-F knock-in (APP KI) mouse model of AD and explore whether this could affect the disease progression at early stages.

Methods

APP KI mice were fed for 2 months with a control or multi-medication diet (including anti- hypertensive, lipid lowering and psychotropic drugs, in two different combinations) based on the most used medications by older adults in Sweden. In addition to the multi-medication regimens, mice were also tested for specific monotherapies from the compounds used in combination. Animals were assessed for locomotion, cognition, and anxiety-like behavior. Brain tissues were collected for molecular biology experiments, while blood was analyzed by GC/LC-MS to measure serum metabolomics.

Results

We found that multi-medication therapies in AD mice differentially affected essential functions such as locomotion, and distinct types of memory. APP KI male mice treated with combination#1 exhibited a rescue of cognitive deficits compared to controls, which we didn´t observe in females. These findings positively correlate with the significant reduction of cortical Aβ plaques observed in treated APP KI males. Conversely, combination#2 didn´t exert a positive effect on cognitive abilities. Monotherapy treatments induced different effects on functional and cognitive outcomes depending on sex, partially explaining the results observed in polypharmacy groups.

Discussion

We show that multi-medication therapies comprising cardiovascular drugs like statins and β-blockers or ACE inhibitors may impact the progression of AD pathophysiology depending on sex and multiple-drug combination, suggesting some synergic effects deriving from the multi- medication rather than the administration of single compounds. The outcomes from this study can provide knowledge for designing more individualized therapies in aging and AD, taking sex and gender into special consideration.

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多种药物治疗(包括心血管药物)对雌雄APPNL-G-F基因敲除小鼠的影响
目标高胆固醇血症和高血压等心血管疾病会增加阿尔茨海默病(AD)的患病风险。因此,某些阿尔茨海默病风险特征可能会受益于优化的多种药物疗法,例如降胆固醇和降血压药物。我们以前的研究表明,瑞典老年患者最常服用的药物是心血管类药物,如抗血栓药、调脂药、ACE 抑制剂、选择性钙通道阻滞剂,而且是联合使用。在这项研究中,我们旨在调查两种多种药物治疗方案对 APPNL-G-F 基因敲入(APP KI)小鼠 AD 模型的影响,并探讨这是否会在早期阶段影响疾病的进展。方法根据瑞典老年人最常用的药物,用对照或多种药物饮食(包括抗高血压药、降血脂药和精神药物,有两种不同的组合)喂养 APP KI 小鼠 2 个月。除了多种药物治疗方案外,小鼠还接受了联合使用的化合物中特定单一疗法的测试。对动物的运动、认知和焦虑行为进行了评估。结果我们发现,多种药物疗法对AD小鼠的运动等基本功能和不同类型的记忆产生了不同的影响。与对照组相比,接受组合药物#1治疗的APP KI雄性小鼠的认知障碍得到了缓解,但我们在雌性小鼠中却没有观察到这一点。这些发现与在接受治疗的 APP KI 雄性小鼠中观察到的皮质 Aβ 斑块显著减少呈正相关。相反,联合疗法#2对认知能力没有产生积极影响。讨论我们的研究表明,由他汀类药物、β-受体阻滞剂或 ACE 抑制剂等心血管药物组成的多种药物疗法可能会影响 AD 病理生理学的进展,这取决于性别和多种药物的组合,这表明多种药物疗法而非单一化合物的施用会产生一些协同效应。这项研究的结果可为设计更多针对衰老和AD的个体化疗法提供知识,同时特别考虑到性别和性别因素。
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来源期刊
Cerebral circulation - cognition and behavior
Cerebral circulation - cognition and behavior Neurology, Clinical Neurology
CiteScore
2.00
自引率
0.00%
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0
审稿时长
14 weeks
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