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Behavioural, genomics and proteomic approach to examine Alzheimer's disease in zebrafish

斑马鱼 神经科学 疾病 阿尔茨海默病 痴呆 生物 病态的 医学 生物信息学 心理学 病理 基因 遗传学
作者
Aisha Siddiqui,Syafiq Asnawi Zainal Abidin,Zahoor Ahmad,Iekhsan Othman,Yatinesh Kumari
出处
期刊:Comparative Biochemistry and Physiology C-toxicology & Pharmacology [Elsevier BV]
卷期号:271: 109636-109636 被引量:4
标识
DOI:10.1016/j.cbpc.2023.109636
摘要

Globally around 24 million elderly population are dealing with dementia, and this pathological characteristic is commonly seen in people suffering from Alzheimer's disease (AD). Despite having multiple treatment options that can mitigate AD symptoms, there is an imperative call to advance our understanding of the disease pathogenesis to unfold disease-modifying treatments/therapies. To explore the driving mechanisms of AD development, we stretch out further to study time-dependant changes after Okadaic acid (OKA)-induced AD-like conditions in zebrafish. We evaluated the pharmacodynamics of OKA at two-time points, i.e., after 4-days and 10-days exposure to zebrafish. T-Maze was utilized to observe the learning and cognitive behaviour, and inflammatory gene expressions such as 5-Lox, Gfap, Actin, APP, and Mapt were performed in zebrafish brains. To scoop everything out from the brain tissue, protein profiling was performed using LCMS/MS. Both time course OKA-induced AD models have shown significant memory impairment, as evident from T-Maze. Gene expression studies of both groups have reported an overexpression of 5-Lox, GFAP, Actin, APP, and OKA 10D group has shown remarkable upregulation of Mapt in zebrafish brains. In the case of protein expression, the heatmap suggested an important role of some common proteins identified in both groups, which can be explored further to investigate their mechanism in OKA-induced AD pathology. Presently, the preclinical models available to understand AD-like conditions are not completely understood. Hence, utilizing OKA in the zebrafish model can be of great importance in understanding the pathology of AD progression and as a screening tool for drug discovery.
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