Identification of disulfide cross-linked tau dimer responsible for tau propagation

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作者
Dohee Kim
Sungsu Lim
Md. Mamunul Haque
Nayeon Ryoo
Hyun Seok Hong
Hyewhon Rhim
Dong-Eun Lee
Young-Tae Chang
Jun-Seok Lee
Eunji Cheong
Dong Jin Kim
Yun Kyung Kim
机构
[1] Brain Science Institute,Korea Institute of Science and Technology (KIST)
[2] Center for neuro-medicine,Department of Biotechnology
[3] Translational Research Center for Protein Function Control,Biological Chemistry
[4] College of Life Science and Biotechnology,Korea Institute of Science and Technology (KIST)
[5] Yonsei University,Department of Neuroscience
[6] University of Science and Technology (UST),Department of Chemistry & Med Chem Program
[7] Brain Science Institute,Singapore BioImaging Consortium
[8] Center for Neuroscience,Korea Institute of Science and Technology (KIST)
[9] Medifron-DBT Inc.,undefined
[10] University of Science and Technology (UST),undefined
[11] Advanced Radiation Technology Institute,undefined
[12] Korea Atomic Energy Research Institute,undefined
[13] National University of Singapore,undefined
[14] Agency for Science,undefined
[15] Technology and Research,undefined
[16] Molecular Recognition Research Center,undefined
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摘要
Recent evidence suggests that tau aggregates are not only neurotoxic, but also propagate in neurons acting as a seed for native tau aggregation. Prion-like tau transmission is now considered as an important pathogenic mechanism driving the progression of tau pathology in the brain. However, prion-like tau species have not been clearly characterized. To identify infectious tau conformers, here we prepared diverse tau aggregates and evaluated the effect on inducing intracellular tau-aggregation. Among tested, tau dimer containing P301L-mutation is identified as the most infectious form to induce tau pathology. Biochemical analysis reveals that P301L-tau dimer is covalently cross-linked with a disulfide bond. The relatively small and covalently cross-linked tau dimer induced tau pathology efficiently in primary neurons and also in tau-transgenic mice. So far, the importance of tau disulfide cross-linking has been overlooked in the study of tau pathology. Here our results suggested that tau disulfide cross-linking might play critical role in tau propagation by producing structurally stable and small tau conformers.
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