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N368-Tau fragments generated by legumain are detected only in trace amount in the insoluble Tau aggregates isolated from AD brain

Acta Neuropathol Commun. 2019; 
Schlegel K, Awwad K, Heym RG, Holzinger D, Doell A, Barghorn S, Jahn TR, Klein C, Mordashova Y, Schulz M, Gasparini L
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Peptide Synthesis Therefore, the quantification method used for human brain assesses fragments arising from all Tau isoforms. The sequence is also conserved between mouse and human, enabling the determination of endogenous mouse Tau as well. Calibration curves were obtained using the peptides Tau354–369 and Tau354–368 for total brain homogenates or full-length 2N4R Tau and Tau1–368 for PS1 and P3 extracts ranging from 5 to 20,000 ng/g. All human Tau peptides used for calibration curves (N369 and N368) were synthesized (GenScript Biotech, Leiden, Netherlands). Get A Quote

摘要

Intraneuronal insoluble inclusions made of Tau protein are neuropathological hallmarks of Alzheimer Disease (AD). Cleavage of Tau by legumain (LGMN) has been proposed to be crucial for aggregation of Tau into fibrils. However, it remains unclear if LGMN-cleaved Tau fragments accumulate in AD Tau inclusions.Using an in vitro enzymatic assay and non-targeted mass spectrometry, we identified four putative LGMN cleavage sites at Tau residues N167-, N255-, N296- and N368. Cleavage at N368 generates variously sized N368-Tau fragments that are aggregation prone in the Thioflavin T assay in vitro. N368-cleaved Tau is not detected in the brain of legumain knockout mice, indicating that LGMN is required for Tau cleavage ... More

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