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• W4200406161 endingPage "1990" @default.
• W4200406161 startingPage "1990" @default.
• W4200406161 abstract "The presence of complement activation products at sites of pathology in post-mortem Alzheimer's disease (AD) brains is well known. Recent evidence from genome-wide association studies (GWAS), combined with the demonstration that complement activation is pivotal in synapse loss in AD, strongly implicates complement in disease aetiology. Genetic variations in complement genes are widespread. While most variants individually have only minor effects on complement homeostasis, the combined effects of variants in multiple complement genes, referred to as the complotype, can have major effects. In some diseases, the complotype highlights specific parts of the complement pathway involved in disease, thereby pointing towards a mechanism; however, this is not the case with AD. Here we review the complement GWAS hits; CR1 encoding complement receptor 1 (CR1), CLU encoding clusterin, and a suggestive association of C1S encoding the enzyme C1s, and discuss difficulties in attributing the AD association in these genes to complement function. A better understanding of complement genetics in AD might facilitate predictive genetic screening tests and enable the development of simple diagnostic tools and guide the future use of anti-complement drugs, of which several are currently in development for central nervous system disorders." @default.
• W4200406161 created "2021-12-31" @default.
• W4200406161 creator A5025054683 @default.
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• W4200406161 creator A5090102833 @default.
• W4200406161 date "2021-12-15" @default.
• W4200406161 modified "2023-10-12" @default.
• W4200406161 title "Genetic Insights into the Impact of Complement in Alzheimer’s Disease" @default.
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