Clusterin in Alzheimer's disease: a player in the biological behavior of amyloid-beta

Alzheimer's disease (AD) remains a major killer, and although its pathogenesis varies, one dominant feature is an increase in the expression, formation, and sedimentation of senile plaques of amyloid-beta (A beta) peptides in the brain. The chaperone protein clusterin has, since its first discovery at the end of the 20(th) century, been labeled as a cytoprotector. However, epigenetic studies showing that clusterin is associated with the severity and risk of AD, especially in the hippocampus, triggered studies to clarify its role in the pathogenesis of AD. It is true that clusterin can inhibit the aggregation of A beta and therefore prevent further formation of senile plaques in the AD brain, yet it induces the formation of soluble forms of A beta which are toxic to neurons. Another problematic finding is that clusterin is involved in a pathway through which A beta has neurodegenerative effects intracellularly. Although the role of clusterin in the pathogenesis of AD is still not clear, this review specifically discusses the interactions between clusterin and A beta, to open up the possibility of a potential therapeutic approach for treating AD.