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Literature DB >> 31974166

A synthetic heparinoid blocks Tau aggregate cell uptake and amplification.

Barbara E Stopschinski¹, Talitha L Thomas², Sourena Nadji³, Eric Darvish³, Linfeng Fan⁴, Brandon B Holmes⁵, Anuja R Modi², Jordan G Finnell², Omar M Kashmer², Sandi Estill-Terpack², Hilda Mirbaha², Hung S Luu⁶, Marc I Diamond⁷.

Abstract

Tau aggregation underlies neurodegeneration in Alzheimer's disease and related tauopathies. We and others have proposed that transcellular propagation of pathology is mediated by Tau prions, which are ordered protein assemblies that faithfully replicate in vivo and cause specific biological effects. The prion model predicts the release of aggregates from a first-order cell and subsequent uptake into a second-order cell. The assemblies then serve as templates for their own replication, a process termed "seeding." We have previously observed that heparan sulfate proteoglycans on the cell surface mediate the cellular uptake of Tau aggregates. This interaction is blocked by heparin, a sulfated glycosaminoglycan. Indeed, heparin-like molecules, or heparinoids, have previously been proposed as a treatment for PrP prion disorders. However, heparin is not ideal for managing chronic neurodegeneration, because it is difficult to synthesize in defined sizes, may have poor brain penetration because of its negative charge, and is a powerful anticoagulant. Therefore, we sought to generate an oligosaccharide that would bind Tau and block its cellular uptake and seeding, without exhibiting anticoagulation activity. We created a compound, SN7-13, from pentasaccharide units and tested it in a range of assays that measured direct binding of Tau to glycosaminoglycans and inhibition of Tau uptake and seeding in cells. SN7-13 does not inhibit coagulation, binds Tau with low nanomolar affinity, and inhibits cellular Tau aggregate propagation similarly to standard porcine heparin. This synthetic heparinoid could facilitate the development of agents to treat tauopathy.

Entities: Chemical Disease Species

Keywords: Alzheimer disease; Tau protein (Tau); glycosaminoglycan; heparan sulfate; heparin; heparin-binding protein; neurodegeneration; neurodegenerative disease; tauopathy

Mesh：

Substances：

Year: 2020 PMID： 31974166 PMCID： PMC7062170 DOI： 10.1074/jbc.RA119.010353

Source DB: PubMed Journal: J Biol Chem ISSN： 0021-9258 Impact factor: 5.157

51 in total

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4. Tau Prion Strains Dictate Patterns of Cell Pathology, Progression Rate, and Regional Vulnerability In Vivo.

Authors: Sarah K Kaufman; David W Sanders; Talitha L Thomas; Allison J Ruchinskas; Jaime Vaquer-Alicea; Apurwa M Sharma; Timothy M Miller; Marc I Diamond
Journal: Neuron Date: 2016-10-27 Impact factor: 17.173

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Authors: E Ersdal-Badju; A Lu; Y Zuo; V Picard; S C Bock
Journal: J Biol Chem Date: 1997-08-01 Impact factor: 5.157

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7. Tau Trimers Are the Minimal Propagation Unit Spontaneously Internalized to Seed Intracellular Aggregation.

Authors: Hilda Mirbaha; Brandon B Holmes; David W Sanders; Jan Bieschke; Marc I Diamond
Journal: J Biol Chem Date: 2015-04-17 Impact factor: 5.157

8. Propagation of tau misfolding from the outside to the inside of a cell.

Authors: Bess Frost; Rachel L Jacks; Marc I Diamond
Journal: J Biol Chem Date: 2009-03-11 Impact factor: 5.157

9. Treatment of transmissible spongiform encephalopathy by intraventricular drug infusion in animal models.

Authors: Katsumi Doh-ura; Kensuke Ishikawa; Ikuko Murakami-Kubo; Kensuke Sasaki; Shirou Mohri; Richard Race; Toru Iwaki
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Review 10. Prions and Protein Assemblies that Convey Biological Information in Health and Disease.

Authors: David W Sanders; Sarah K Kaufman; Brandon B Holmes; Marc I Diamond
Journal: Neuron Date: 2016-02-03 Impact factor: 17.173

8 in total

Review 1. The Role of Extracellular Matrix Components in the Spreading of Pathological Protein Aggregates.

Authors: Edoardo Moretto; Skye Stuart; Sunaina Surana; Jose Norberto S Vargas; Giampietro Schiavo
Journal: Front Cell Neurosci Date: 2022-04-29 Impact factor: 6.147

2. Mutations in the COPI coatomer subunit α-COP induce release of Aβ-42 and amyloid precursor protein intracellular domain and increase tau oligomerization and release.

Authors: Jacob W Astroski; Leonora K Akporyoe; Elliot J Androphy; Sara K Custer
Journal: Neurobiol Aging Date: 2021-01-13 Impact factor: 4.673

A synthetic heparinoid blocks Tau aggregate cell uptake and amplification.

1. Prophylactic potential of pentosan polysulphate in transmissible spongiform encephalopathies.

2. A new synthetic pentasaccharide with increased anti-factor Xa activity: possible role for anionic clusters in the interaction of heparin and antithrombin III.

3. Proteopathic tau seeding predicts tauopathy in vivo.

4. Tau Prion Strains Dictate Patterns of Cell Pathology, Progression Rate, and Regional Vulnerability In Vivo.

5. Identification of the antithrombin III heparin binding site.

6. Heparin oligosaccharides that pass the blood-brain barrier inhibit beta-amyloid precursor protein secretion and heparin binding to beta-amyloid peptide.

7. Tau Trimers Are the Minimal Propagation Unit Spontaneously Internalized to Seed Intracellular Aggregation.

8. Propagation of tau misfolding from the outside to the inside of a cell.

9. Treatment of transmissible spongiform encephalopathy by intraventricular drug infusion in animal models.

Review 10. Prions and Protein Assemblies that Convey Biological Information in Health and Disease.

Review 1. The Role of Extracellular Matrix Components in the Spreading of Pathological Protein Aggregates.

2. Mutations in the COPI coatomer subunit α-COP induce release of Aβ-42 and amyloid precursor protein intracellular domain and increase tau oligomerization and release.

3. PIKfyve activity is required for lysosomal trafficking of tau aggregates and tau seeding.

4. Tau Protein Modulates Perineuronal Extracellular Matrix Expression in the TauP301L-acan Mouse Model.

5. Inhibition Of Tau Protein Aggregation By a Chaperone-like β-Boswellic Acid Conjugated To Gold Nanoparticles.

Review 6. Cell-to-Cell Transmission of Tau and α-Synuclein.

Review 7. The Sulfation Code of Tauopathies: Heparan Sulfate Proteoglycans in the Prion Like Spread of Tau Pathology.

Review 8. Fibrotic Scar in Neurodegenerative Diseases.