Possible Clues for Brain Energy Translation via Endolysosomal Trafficking of APP‐CTFs in Alzheimer’s Disease

疾病 翻译(生物学) 神经科学 化学 生物 医学 病理 生物化学 基因 信使核糖核酸
作者
Senthilkumar Sivanesan,Ravi Mundugaru,Jayakumar Rajadas
出处
期刊:Oxidative Medicine and Cellular Longevity [Hindawi Publishing Corporation]
卷期号:2018 (1) 被引量:8
标识
DOI:10.1155/2018/2764831
摘要

Vascular dysfunctions, hypometabolism, and insulin resistance are high and early risk factors for Alzheimer’s disease (AD), a leading neurological disease associated with memory decline and cognitive dysfunctions. Early defects in glucose transporters and glycolysis occur during the course of AD progression. Hypometabolism begins well before the onset of early AD symptoms; this timing implicates the vulnerability of hypometabolic brain regions to beta‐secretase 1 (BACE‐1) upregulation, oxidative stress, inflammation, synaptic failure, and cell death. Despite the fact that ketone bodies, astrocyte‐neuron lactate shuttle, pentose phosphate pathway (PPP), and glycogenolysis compensate to provide energy to the starving AD brain, a considerable energy crisis still persists and increases during disease progression. Studies that track brain energy metabolism in humans, animal models of AD, and in vitro studies reveal striking upregulation of beta‐amyloid precursor protein ( β ‐APP) and carboxy‐terminal fragments (CTFs). Currently, the precise role of CTFs is unclear, but evidence supports increased endosomal‐lysosomal trafficking of β ‐APP and CTFs through autophagy through a vague mechanism. While intracellular accumulation of A β is attributed as both the cause and consequence of a defective endolysosomal‐autophagic system, much remains to be explored about the other β ‐APP cleavage products. Many recent works report altered amino acid catabolism and expression of several urea cycle enzymes in AD brains, but the precise cause for this dysregulation is not fully explained. In this paper, we try to connect the role of CTFs in the energy translation process in AD brain based on recent findings.
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