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Literature DB >> 33716717

Passive Immunization With a Novel Monoclonal Anti-PrP Antibody TW1 in an Alzheimer's Mouse Model With Tau Pathology.

Allal Boutajangout^1,2,3,4, Wei Zhang⁵, Justin Kim^1,2, Wed Ali Abdali^1,2, Frances Prelli^1,2, Thomas Wisniewski^1,2,3,6.

Abstract

Neurofibrillary tangles (NFTs) are a major pathologic hallmark of Alzheimer's disease (AD). Several studies have shown that amyloid β oligomers (Aβo) and tau oligomers mediate their toxicity, in part, via binding to cellular prion protein (PrPC) and that some anti-PrP antibodies can block this interaction. We have generated a novel monoclonal anti-PrP antibody (TW1) and assessed the efficacy of passive immunization with it in a mouse model of AD with extensive tau pathology: hTau/PS1 transgenic (Tg) mice. These mice were injected intraperitoneally once a week with TW1 starting at 5 months of age. Behavior was assessed at 8 months of age and brain tissue was subsequently harvested for analysis of treatment efficacy at 9 months. Mice treated with TW1 did not show any significant difference in sensorimotor testing including traverse beam, rotarod, and locomotor activity compared to controls. Significant cognitive benefits were observed with the novel object recognition test (ORT) in the immunized mice (two-tailed, t-test p = 0.0019). Immunized mice also showed cognitive benefits on the closed field symmetrical maze (day 1 two-tailed t-test p = 0.0001; day 2 two-tailed t-test p = 0.0015; day 3 two-tailed t-test p = 0.0002). Reduction of tau pathology was observed with PHF-1 immunohistochemistry in the piriform cortex by 60% (two-tailed t-test p = 0.01) and in the dentate gyrus by 50% (two-tailed t-test p = 0.02) in animals treated with TW1 compared to controls. There were no significant differences in astrogliosis or microgliosis observed between treated and control mice. As assessed by Western blots using PHF-1, the TW1 therapy reduced phosphorylated tau pathology (two-tailed t-test p = 0.03) and improved the ratio of pathological soluble tau to tubulin (PHF1/tubulin; two-tailed t-test p = 0.0006). Reduction of tau pathology also was observed using the CP13 antibody (two-tailed t-test p = 0.0007). These results indicate that passive immunization with the TW1 antibody can significantly decrease tau pathology as assessed by immunohistochemical and biochemical methods, resulting in improved cognitive function in a tau transgenic mouse model of AD.

Entities: Chemical

Keywords: Alzheimer’s disease; immunotherapy; passive immunization; prion; tau related pathology; transgenic mice

Year: 2021 PMID： 33716717 PMCID： PMC7947695 DOI： 10.3389/fnagi.2021.640677

Source DB: PubMed Journal: Front Aging Neurosci ISSN： 1663-4365 Impact factor: 5.750

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Passive Immunization With a Novel Monoclonal Anti-PrP Antibody TW1 in an Alzheimer's Mouse Model With Tau Pathology.

1. Automated identification of complementarity determining regions (CDRs) reveals peculiar characteristics of CDRs and B cell epitopes.

2. Immunological comparison of scrapie-associated fibrils isolated from animals infected with four different scrapie strains.

3. Clearance and prevention of prion infection in cell culture by anti-PrP antibodies.

4. The toxicity of antiprion antibodies is mediated by the flexible tail of the prion protein.

5. Experimental Models of Tauopathy - From Mechanisms to Therapies.

6. Cross-linking cellular prion protein triggers neuronal apoptosis in vivo.

Review 7. Recent advancements toward therapeutic vaccines against Alzheimer's disease.

8. Immunotherapy to improve cognition and reduce pathological species in an Alzheimer's disease mouse model.

Review 9. New Insights Into Drug Discovery Targeting Tau Protein.

Review 10. Passive immunotherapies targeting Aβ and tau in Alzheimer's disease.

Review 1. Oligomeropathies, inflammation and prion protein binding.