Hitoshi Shinotoh scite author profile

Summary Deposition of intracellular tau fibrils has been the focus of research on the mechanisms of neurodegeneration in Alzheimer’s disease (AD) and related tauopathies. Here, we developed a new class of tau ligands, phenyl/pyridinyl-butadienyl-benzothiazoles/benzothiazoliums (PBBs), for visualizing diverse tau inclusions in brains of living patients with AD or non-AD tauopathies and animal models of these disorders. In vivo optical and positron emission tomographic (PET) imaging of a transgenic mouse model demonstrated sensitive detection of tau inclusions by PBBs. A pyridinated PBB, [11C]PBB3 was next applied in a clinical PET study, and its robust signal in the AD hippocampus wherein tau pathology is enriched contrasted strikingly with that of a senile plaque radioligand, [11C]Pittsburgh Compound-B ([11C]PIB). [11C]PBB3-PET data were also consistent with the spreading of tau pathology with AD progression. Furthermore, increased [11C]PBB3 signals were found in a corticobasal syndrome patient negative for [11C]PIB-PET.

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Questionnaire-based assessment of pelvic organ dysfunction in Parkinson's disease

Sakakibara

Shinotoh

Uchiyama

et al. 2001

Autonomic Neuroscience

322

245

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High-Contrast In Vivo Imaging of Tau Pathologies in Alzheimer’s and Non-Alzheimer’s Disease Tauopathies

Tagai

Ono

Kubota

et al. 2021

Neuron

192

198

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Mapping of brain acetylcholinesterase alterations in Lewy body disease by PET

Shimada¹,

Hirano²,

Shinotoh³

et al. 2009

Neurology

329

175

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