Therapeutic Potential of Ferulic Acid in Alzheimer's Disease

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Date

2022

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Volume Title

Publisher

Bentham Science Publ Ltd

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Abstract

Alzheimer's Disease (AD) is one of the most important neurodegenerative diseases, accounting for 60% of all dementia cases. AD is a progressive neurodegenerative disease that occurs due to the production of beta-amyloid (A beta) protein and accumulation of hyper-phosphorylated tau protein; it causes breakage in the synaptic bonds and neuronal deaths to a large extent. Millions of people worldwide suffer from AD because there is no definitive drug for disease prevention, treatment, or slowing down its progression. Over the last decade, multiple target applications have been developed for AD treatments. These targets include A beta accumulations, hyper-phosphorylated tau proteins, mitochondrial dysfunction, and oxidative stress, resulting in toxicity. Various natural or semisynthetic antioxidant formulations have been shown to protect brain cells from A beta-induced toxicity and provide promising potentials for AD treatment. Ferulic acid (FA), a high-capacity antioxidant molecule, is naturally synthesized from certain plants. FA has been shown to have different substantial biological properties, such as anticancer, antidiabetic, antimicrobial, anti-inflammatory, hepatoprotective, and cardioprotective actions, etc. Furthermore, FA exerts neuroprotection via preventing A beta-fibril formation, acting as an anti-inflammatory agent, and inhibiting free radical generation and acetylcholinesterase (AChE) enzyme activity. In this review, we present key biological roles of FA and several FA derivatives in preventing A beta-induced neurotoxicity, protecting against free radical attacks, and exhibiting enzyme inhibitions and evaluate them as possible therapeutic agents for the treatment of AD.

Description

Arslan, Mehmet Enes/0000-0002-1600-2305; Pergentino De Sousa, Damião/0000-0002-7180-4896; Yuce Kahraman, Cigdem/0000-0003-1957-9596

Keywords

Ferulic Acid, Anti-Alzheimer, Alzheimer's Disease, Experimental Alzheimer's Model, Amyloid-Beta, Drug Candidate, Neurotoxicity, Neuroprotection

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WoS Q

Q2

Scopus Q

Q2

Source

Current Drug Delivery

Volume

19

Issue

8

Start Page

860

End Page

873
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