AUTHOR=Al-Hilaly Youssra K. , Hurt Connor , Rickard Janet E. , Harrington Charles R. , Storey John M. D. , Wischik Claude M. , Serpell Louise C. , Siemer Ansgar B. 

TITLE=Solid-state NMR of paired helical filaments formed by the core tau fragment tau(297-391)

JOURNAL=Frontiers in Neuroscience

VOLUME=16

YEAR=2022

URL=https://www.frontiersin.org/journals/neuroscience/articles/10.3389/fnins.2022.988074

DOI=10.3389/fnins.2022.988074

ISSN=1662-453X

ABSTRACT=<p>Aggregation of the tau protein into fibrillar cross-β aggregates is a hallmark of Alzheimer’s diseases (AD) and many other neurodegenerative tauopathies. Recently, several core structures of patient-derived tau paired helical filaments (PHFs) have been solved revealing a structural variability that often correlates with a specific tauopathy. To further characterize the dynamics of these fibril cores, to screen for strain-specific small molecules as potential biomarkers and therapeutics, and to develop strain-specific antibodies, recombinant in-vitro models of tau filaments are needed. We recently showed that a 95-residue fragment of tau (from residue 297 to 391), termed dGAE, forms filaments <italic>in vitro</italic> in the absence of polyanionic co-factors often used for <italic>in vitro</italic> aggregation of full-length tau. Tau(297-391) was identified as the proteolytic resistant core of tau PHFs and overlaps with the structures characterized by cryo-electron microscopy in <italic>ex vivo</italic> PHFs, making it a promising model for the study of AD tau filaments <italic>in vitro</italic>. In the present study, we used solid-state NMR to characterize tau(297-391) filaments and show that such filaments assembled under non-reducing conditions are more dynamic and less ordered than those made in the presence of the reducing agent DTT. We further report the resonance assignment of tau(297-391)+DTT filaments and compare it to existing core structures of tau.</p>