Hiring in life sciences? Share your open positions with our professional community. Read more Close

Your cookie settings

This site uses cookies. Some cookies are essential to make the site work and others help us to improve our services. Read more about cookies in our Privacy policy.

Choose your cookie preferences:

Advertisement

An Engineered Multifunctional Fusion Protein Targeting Aβ Oligomers, Microglia and Autophagy Ameliorates Cognitive Deficits and Amyloid Pathology in Alzheimer's Disease Mice.

Created on 24 Jun 2026

Authors

Jie Zhu, Ya-Ru Huang, Fei Chen, Mei-Qi Wang, Xiao-Lin Yu, Gui-Feng Zhang, Rui-Tian Liu

Published in

Cellular and molecular neurobiology. Jun 24, 2026. Epub Jun 24, 2026.

Abstract

In Alzheimer's disease (AD), Amyloid-β (Aβ) oligomers function as key neurotoxic agents that underpin the disease's progression. A diverse array of therapeutic entities, including peptides, single-chain variable fragments (scFvs), and small molecules, have demonstrated the ability to interact with Aβ oligomers, thereby suppressing their aggregation and associated neurotoxicity. Despite these advances, such agents frequently struggle to promote the phagocytosis and subsequent breakdown of aggregated Aβ by microglia. Moreover, the dense accumulation of Aβ oligomers may resist enzymatic hydrolysis within the acidic lysosomal lumen, contributing to lysosomal stress and dysfunction. To overcome these problems, we engineered a multifunctional fusion protein, p62-LIR-W20-Tuftsin (W20-LT), consisting of an oligomer-specific scFv, a microglia-targeting Tuftsin peptide, and a p62-LIR peptide to activate autophagy. In vitro assays demonstrated that W20-LT significantly outperformed the parental W20 by promoting the rapid microglial uptake of Aβ oligomers and enhancing their intracellular clearance through an autophagy-associated pathway. In APPswe/PS1dE9 (APP/PS1) mice, a low-dose regimen (0.5 µg, every 3 days) of W20-LT, but not W20, significantly ameliorated cognitive deficits and reduced amyloid pathology. Mechanistically, W20-LT was associated with enhanced autophagy-lysosomal pathway activity, as indicated by increased LC3B-II and reduced p62 levels, together with downregulated CatD and LAMP1 levels, thereby mitigating neuroinflammation. In summary, our findings suggest that W20-LT represents a promising proof-of-concept therapeutic strategy that combines scFv-based Aβ oligomer recognition with enhanced autophagy-associated clearance, thereby mitigating AD pathology.

PMID:
42340476
Bibliographic data and abstract were imported from PubMed on 24 Jun 2026.

Read full publication at:
Please sign in to see all details.

Advertisement

Stats

  • Community rating n/a 0 votes
  • Reviewers' rating n/a 0 votes
  • Sign in to post a review. Add review
  • Your rating

1-terrible, 9-excellent. How would you rate this publication? Sign in in to submit your rating.

  • Recommendations n/a n/a positive of 0 vote(s)
  • Views 2
  • Comments 0

Recommended by

  • No recommendations yet.

Do you recommend this? Please sign in. Yes No

Recommended

Post a comment

You need to be signed in to post comments. You can sign in here.

Comments

There are no comments yet.

Advertisement