以心脏为目标：阿尔茨海默病预防的新轴心。

Journal of dementia and alzheimer's disease Pub Date : 2025-06-01 Epub Date: 2025-05-01 DOI:10.3390/jdad2020010

Lawrence I Heller, Allison S Lowe, Thaís Del Rosario Hernández, Sayali V Gore, Mallika Chatterjee, Robbert Creton

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摘要

背景/目的：环孢素A和其他钙调磷酸酶抑制剂已被确定为预防阿尔茨海默病的前瞻性治疗方法。我们之前发现，钙调磷酸酶抑制剂在斑马鱼幼虫中引发了一种独特的行为特征，其特征是活动增加、声音超兴奋性和视觉引导行为减少。使用Z-LaP Tracker筛选fda批准的大量化合物发现，一些心脏药物产生类似的行为特征，表明这些药物可能发挥钙调磷酸酶抑制剂样作用，与预防或改善阿尔茨海默病有关。方法：使用神经网络模型Z-LaP Tracker筛选fda批准的大型药物库，发现65种药物具有类似环孢素a的行为特征。其中14种是心脏药物，包括血管紧张素受体阻滞剂、受体阻滞剂、肾上腺素受体拮抗剂和他汀类药物。结果：在Z-LaP跟踪器中，心脏药物与环孢素A的双重给药显示出协同效应：每种低剂量的心脏药物可以与低剂量的环孢素A一起给药，以引起类似或更大的行为效应，而不是单独使用每种高剂量的药物。其他研究表明，许多这些心脏药物直接或间接抑制钙调磷酸酶- nfat途径，如环孢素A，提供了一种潜在的机制。结论：低剂量环孢素a与选定的心脏药物联合使用可能是一种潜在的有效治疗策略，可以预防阿尔茨海默病的发生，同时治疗心血管功能障碍，同时减轻高剂量环孢素a的副作用。鉴于许多患者在阿尔茨海默病之前患有心脏病，医生可能能够创建一种治疗方案，同时解决这两种情况。我们的研究结果表明，钙调磷酸酶抑制剂联合辛伐他汀、厄贝沙坦、西洛他唑、多沙唑嗪或奈比洛尔是未来探索最有希望的候选药物。

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Target the Heart: A New Axis of Alzheimer's Disease Prevention.

Background/objective: Cyclosporine A and other calcineurin inhibitors have been identified as prospective treatments for preventing Alzheimer's disease. We previously found that calcineurin inhibitors elicit a unique behavioral profile in zebrafish larvae, characterized by increased activity, acoustic hyperexcitability, and reduced visually guided behaviors. Screening a large library of FDA-approved compounds using Z-LaP Tracker revealed that some heart medications produce a similar behavioral profile, suggesting these drugs may exert calcineurin-inhibitor-like effects relevant to prevent-ing or ameliorating Alzheimer's disease.

Methods: Screening a large library of FDA-approved drugs using Z-LaP Tracker, a neural network model, revealed a cluster of 65 drugs demonstrating a cyclosporine A-like behavioral profile. Fourteen of these drugs were heart medications, including angiotensin receptor blockers, beta blockers, al-pha-adrenergic receptor antagonists, and a statin.

Results: Dual administration of the heart medications with cyclosporine A in Z-LaP Tracker revealed synergistic effects: lower doses of each heart medication could be delivered in conjunction with a lower dose of cyclosporine A to evoke a similar or larger behavioral effect than higher doses of each drug independently. Other studies have shown that many of these heart medica-tions drugs directly or indirectly inhibit the calcineurin-NFAT pathway, like cyclo-sporine A, providing a potential mechanism.

Conclusions: Co-administering a low dose of cyclosporine A with select cardiac drugs could be a potentially effective treatment strategy for preventing Alzheimer's disease occurrence and simultaneously treating cardiovascular dysfunction, while mitigating the side effects associated with higher doses of cyclosporine A. Given that heart disease precedes Alzheimer's disease in many patients, physicians may be able to create a treatment regimen that addresses both con-ditions. Our results suggest that a calcineurin inhibitor combined with simvastatin, irbesartan, cilostazol, doxazosin, or nebivolol is the most promising candidate for future exploration.

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Journal of dementia and alzheimer's disease

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