A small-molecule TLR4 antagonist reduced neuroinflammation in female E4FAD mice

Deebika Balu; Ana C Valencia-Olvera; Austin Nguyen; Mehul Patnam; Jason York; Francesco Peri; Frank Neumann; Mary Jo LaDu; Leon M Tai

doi:10.1186/s13195-023-01330-6

A small-molecule TLR4 antagonist reduced neuroinflammation in female E4FAD mice

Alzheimers Res Ther. 2023 Oct 19;15(1):181. doi: 10.1186/s13195-023-01330-6.

Authors

Deebika Balu¹, Ana C Valencia-Olvera¹, Austin Nguyen¹, Mehul Patnam¹, Jason York¹, Francesco Peri², Frank Neumann³, Mary Jo LaDu¹, Leon M Tai⁴

Affiliations

¹ Department of Anatomy and Cell Biology, University of Illinois at Chicago, Chicago, IL, 60612, USA.
² Department of Biotechnology and Biosciences, University of Milano-Bicocca, Milan, Italy.
³ Innaxon Biosciences, Tewkesbury, UK.
⁴ Department of Anatomy and Cell Biology, University of Illinois at Chicago, Chicago, IL, 60612, USA. leontai@uic.edu.

Abstract

Background: APOE genotype is the greatest genetic risk factor for sporadic Alzheimer's disease (AD). APOE4 increases AD risk up to 12-fold compared to APOE3, an effect that is greater in females. Evidence suggests that one-way APOE could modulate AD risk and progression through neuroinflammation. Indeed, APOE4 is associated with higher glial activation and cytokine levels in AD patients and mice. Therefore, identifying pathways that contribute to APOE4-associated neuroinflammation is an important approach for understanding and treating AD. Human and in vivo evidence suggests that TLR4, one of the key receptors involved in the innate immune system, could be involved in APOE-modulated neuroinflammation. Consistent with that idea, we previously demonstrated that the TLR4 antagonist IAXO-101 can reduce LPS- and Aβ-induced cytokine secretion in APOE4 glial cultures. Therefore, the goal of this study was to advance these findings and determine whether IAXO-101 can modulate neuroinflammation, Aβ pathology, and behavior in mice that express APOE4.

Methods: We used mice that express five familial AD mutations and human APOE3 (E3FAD) or APOE4 (E4FAD). Female and male E4FAD mice and female E3FAD mice were treated with vehicle or IAXO-101 in two treatment paradigms: prevention from 4 to 6 months of age or reversal from 6 to 7 months of age. Learning and memory were assessed by modified Morris water maze. Aβ deposition, fibrillar amyloid deposition, astrogliosis, and microgliosis were assessed by immunohistochemistry. Soluble levels of Aβ and apoE, insoluble levels of apoE and Aβ, and IL-1β were measured by ELISA.

Results: IAXO-101 treatment resulted in lower Iba-1 coverage, lower number of reactive microglia, and improved memory in female E4FAD mice in both prevention and reversal paradigms. IAXO-101-treated male E4FAD mice also had lower Iba-1 coverage and reactivity in the RVS paradigm, but there was no effect on behavior. There was also no effect of IAXO-101 treatment on neuroinflammation and behavior in female E3FAD mice.

Conclusion: Our data supports that TLR4 is a potential mechanistic therapeutic target for modulating neuroinflammation and cognition in APOE4 females.

Keywords: Alzheimer’s disease; Apolipoprotein E; EFAD; Female sex; IAXO-101; Neuroinflammation; TLR4; Treatment paradigms.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Alzheimer Disease* / genetics
Amyloid beta-Peptides / metabolism
Animals
Apolipoprotein E3 / genetics
Apolipoprotein E4* / genetics
Apolipoprotein E4* / metabolism
Apolipoproteins E / genetics
Cytokines
Female
Male
Mice
Mice, Transgenic
Neuroinflammatory Diseases
Toll-Like Receptor 4 / therapeutic use

Substances

Amyloid beta-Peptides
Apolipoprotein E3
Apolipoprotein E4
Apolipoproteins E
Cytokines
Toll-Like Receptor 4

Abstract

Publication types

MeSH terms

Substances

Grants and funding