Tau proteins cross the blood-brain barrier

WA Banks, A Kovac, P Majerova… - Journal of …, 2017 - content.iospress.com
WA Banks, A Kovac, P Majerova, KM Bullock, M Shi, J Zhang
Journal of Alzheimer's Disease, 2017content.iospress.com
Tauopathies are a hallmark of many neurodegenerative diseases, including Alzheimer's
disease and traumatic brain injuries. It has been demonstrated that amyloid-beta peptides,
alpha-synuclein, and prion proteins cross the blood-brain barrier (BBB), contributing to their
abilities to induce disease. Very little is known about whether tau proteins can cross the
BBB. Here we systematically characterized several key forms of tau proteins to cross the
BBB, including Tau-441 (2N4R), Tau-410 (2N3R), truncated tau 151–391 (0N4R), and …
Abstract
Tauopathies are a hallmark of many neurodegenerative diseases, including Alzheimer’s disease and traumatic brain injuries. It has been demonstrated that amyloid-beta peptides, alpha-synuclein, and prion proteins cross the blood-brain barrier (BBB), contributing to their abilities to induce disease. Very little is known about whether tau proteins can cross the BBB. Here we systematically characterized several key forms of tau proteins to cross the BBB, including Tau-441 (2N4R), Tau-410 (2N3R), truncated tau 151–391 (0N4R), and truncated tau 121–227. All of these tau proteins crossed the BBB readily and bidirectonally; however, only Tau-410 had a saturable component to its influx. The tau proteins also entered the blood after their injection into the brain, with Tau 121–227 having the slowest exit from brain. The tau proteins varied in regards to their enzymatic stability in brain and blood and in their peripheral pharmacokinetics. These results show that blood-borne tau proteins could contribute to brain tauopathies. The result also suggest that the CNS can contribute to blood levels of tau, raising the possibility that, as suggested for other misfolded proteins, blood levels of tau proteins could be used as a biomarker of CNS disease.
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