Identification of the minimal active soluble TREM2 sequence for modulating microglial phenotypes and amyloid pathology.

Xuan ShengYunling YaoRuizhi HuangYing XuYifei ZhuLinting ChenLianshuai ZhangWanbing WangRengong ZhuoDan CanChe-Feng ChangYun-Wu ZhangHuaxi XuGuojun BuLi ZhongXiao-Fen Chen

Published in: Journal of neuroinflammation (2021)

Our results indicate that the interaction of sTREM2 truncated variants with Aβ is essential for enhancing microglial recruitment to the vicinity of an amyloid plaque and reducing the plaque load. Importantly, we identified a 41-amino acid sequence of sTREM2 that is sufficient for modulating microglial functions and more potent than the full-length sTREM2 in reducing the plaque load and the plaque-associated neurotoxicity. Taken together, our data provide more insights into the mechanisms underlying sTREM2 function and the minimal active sTREM2 sequence represents a promising candidate for AD therapy.

Keyphrases

amino acid
coronary artery disease
inflammatory response
lipopolysaccharide induced
lps induced
neuropathic pain
signaling pathway
gene expression
copy number
spinal cord injury
big data
electronic health record
bone marrow
spinal cord
mesenchymal stem cells
genome wide