@article{oai:repo.qst.go.jp:00080854,
 author = {Shimada, Hiroyuki and Minatani, Shinobu and Takeuchi, Jun and Takeda, Akitoshi and Joji Kawabe and Wada, Yasuhiro and Mawatari, Aya and Yasuyoshi Watanabe and Shimada, Hitoshi and Higuchi, Makoto and Suhara, Tetsuya and Tomiyama, Takami and Itoh, Yoshiaki and Hitoshi, Shimada and Makoto, Higuchi and Tetsuya, Suhara},
 issue = {12},
 journal = {International Journal of Molecular Sciences},
 month = {Jun},
 note = {We previously identified a novel mutation in amyloid precursor protein from a Japanese pedigree of familial Alzheimer's disease, FAD (Osaka). Our previous positron emission tomography (PET) study revealed that amyloid β (Aβ) accumulation was negligible in two sister cases of this pedigree, indicating a possibility that this mutation induces dementia without forming senile plaques. To further explore the relationship between Aβ, tau and neurodegeneration, we performed tau and Aβ PET imaging in the proband of FAD (Osaka) and in patients with sporadic Alzheimer's disease (SAD) and healthy controls (HCs). The FAD (Osaka) patient showed higher uptake of tau PET tracer in the frontal, lateral temporal, and parietal cortices, posterior cingulate gyrus and precuneus than the HCs (>2.5 SD) and in the lateral temporal and parietal cortices than the SAD patients (>2 SD). Most noticeably, heavy tau tracer accumulation in the cerebellum was found only in the FAD (Osaka) patient. Scatter plot analysis of the two tracers revealed that FAD (Osaka) exhibits a distinguishing pattern with a heavy tau burden and subtle Aβ accumulation in the cerebral cortex and cerebellum. These observations support our hypothesis that Aβ can induce tau accumulation and neuronal degeneration without forming senile plaques.},
 title = {Heavy Tau Burden with Subtle Amyloid β Accumulation in the Cerebral Cortex and Cerebellum in a Case of Familial Alzheimer’s Disease with APP Osaka Mutation},
 volume = {21},
 year = {2020}
}