Macrophage Migration Inhibitory Factor is subjected to glucose modification and oxidation in Alzheimer's Disease

Kassaar O, Pereira Morais M, Xu S, Adam EL, Chamberlain RC, Jenkins B, James T, Francis PT, Ward S, Williams RJ, van den Elsen J (2017) Send to Sci Rep. 7: 42874. doi: 10.1038/srep42874

Web URL: Read this and related abstracts on PubMed here

Abstract:

Glucose and glucose metabolites are able to adversely modify proteins through a non-enzymatic reaction called glycation, which is associated with the pathology of Alzheimer's Disease (AD) and is a characteristic of the hyperglycaemia induced by diabetes.

However, the precise protein glycation profile that characterises AD is poorly defined and the molecular link between hyperglycaemia and AD is unknown.

In this study, we define an early glycation profile of human brain using fluorescent phenylboronate gel electrophoresis and identify early glycation and oxidation of macrophage migration inhibitory factor (MIF) in AD brain. This modification inhibits MIF enzyme activity and ability to stimulate glial cells. MIF is involved in immune response and insulin regulation, hyperglycaemia, oxidative stress and glycation are all implicated in AD.

Our study indicates that glucose modified and oxidised MIF could be a molecular link between hyperglycaemia and the dysregulation of the innate immune system in AD.

FAB RESEARCH COMMENT:

Read the associated news story:

Alzheimer's could be caused by excess sugar: new study finds 'molecular link'

< 23 February 2017 - The Telegraph - Alzheimer's could be caused by excess sugar: new study finds 'molecular link'

Hwang et al 2017 - The human brain produces fructose from glucose >

Feeding Better Mood, Behaviour, Learning and Sleep - Evidence and Best Practice - BOOK HERE

Macrophage Migration Inhibitory Factor is subjected to glucose modification and oxidation in Alzheimer's Disease

Abstract:

FAB RESEARCH COMMENT:

Newsletter Signup

Useful Links

Contact Us

Important Notice