Caspase-6-cleaved Tau is Relevant in Alzheimer's Disease and Marginal in Four-repeat Tauopathies: Diagnostic and Therapeutic Implications

Overview

Journal Neuropathol Appl Neurobiol

Specialty Neurology

Date 2022 May 4

PMID 35508761

Authors

Panos Theofilas

Antonia M H Piergies

Ian Oh

Yoo Bin Lee

Song Hua Li

Felipe L Pereira

Cathrine Petersen

Alexander J Ehrenberg

Rana A Eser

Andrew J Ambrose

Brian Chin

Teddy Yang

Shireen Khan

Raymond Ng

Salvatore Spina

Willian W Seeley

Bruce L Miller

Michelle R Arkin

Lea T Grinberg

Affiliations

Soon will be listed here.

Abstract

Aim: Tau truncation (tr-tau) by active caspase-6 (aCasp-6) generates tau fragments that may be toxic. Yet the relationship between aCasp-6, different forms of tr-tau and hyperphosphorylated tau (p-tau) accumulation in human brains with Alzheimer's disease (AD) and other tauopathies remains unclear.

Methods: We generated two neoepitope monoclonal antibodies against tr-tau sites (D402 and D13) targeted by aCasp-6. Then, we used five-plex immunofluorescence to quantify the neuronal and astroglial burden of aCasp-6, tr-tau, p-tau and their co-occurrence in healthy controls, AD and primary tauopathies.

Results: Casp-6 activation was strongest in AD and Pick's disease (PiD) but almost absent in 4-repeat (4R) tauopathies. In neurons, the tr-tau burden was much more abundant in AD and PiD than in 4R tauopathies and disproportionally higher when normalising by p-tau pathology. Tr-tau astrogliopathy was detected in low numbers in 4R tauopathies. Unexpectedly, about half of tr-tau positive neurons in AD and PiD lacked p-tau aggregates, a finding we confirmed using several p-tau antibodies.

Conclusions: Early modulation of aCasp-6 to reduce tr-tau pathology is a promising therapeutic strategy for AD and PiD but is unlikely to benefit 4R tauopathies. The large percentage of tr-tau-positive neurons lacking p-tau suggests that many vulnerable neurons to tau pathology go undetected when using conventional p-tau antibodies. Therapeutic strategies against tr-tau pathology could be necessary to modulate the extent of tau abnormalities in AD. The disproportionally higher burden of tr-tau in AD and PiD supports the development of biofluid biomarkers against tr-tau to detect AD and PiD and differentiate them from 4R tauopathies at a patient level.

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