Journal Article Mutations in bassoon in individuals with familial and sporadic progressive supranuclear palsy-like syndrome

Yabe, Ichiro  ,  Yaguchi, Hiroaki  ,  Kato, Yasutaka  ,  Miki, Yasuo  ,  Takahashi, Hidehisa  ,  Tanikawa, Satoshi  ,  Shirai, Shinichi  ,  Takahashi, Ikuko  ,  Kimura, Mari  ,  Hama, Yuka  ,  Matsushima, Masaaki  ,  Fujioka, Shinsuke  ,  Kano, Takahiro  ,  Watanabe, Masashi  ,  Nakagawa, Shin  ,  Kunieda, Yasuyuki  ,  Ikeda, Yoshio  ,  Hasegawa, Masato  ,  Nishihara, Hiroshi  ,  Ohtsuka, Toshihisa  ,  Tanaka, Shinya  ,  Tsuboi, Yoshio  ,  Hatakeyama, Shigetsugu  ,  Wakabayashi, Koichi  ,  Sasaki, Hidenao

8p.819 , 2018-01-16 , Nature Publishing Group
Clinical diagnosis of progressive supranuclear palsy (PSP) is sometimes difficult because various phenotypes have been identified. Here, we report a mutation in the bassoon (BSN) gene in a family with PSP-like syndrome. Their clinical features resembled not only those of PSP patients but also those of individuals with multiple system atrophy and Alzheimer’s disease. The neuropathological findings showed a novel three + four repeat tauopathy with pallido-luysio-nigral degeneration and hippocampal sclerosis. Whole-exome analysis of this family identified a novel missense mutation in BSN. Within the pedigree, the detected BSN mutation was found only in affected individuals. Further genetic analyses were conducted in probands from four other pedigrees with PSP-like syndrome and in 41 sporadic cases. Three missense mutations in BSN that are very rarely listed in databases of healthy subjects were found in four sporadic cases. Western blot analysis of tau following the overexpression of wild-type or mutated BSN revealed the possibility that wild-type BSN reduced tau accumulation, while mutated BSN lost this function. An association between BSN and neurological diseases has not been previously reported. Our results revealed that the neurodegenerative disorder associated with the original proband’s pedigree is a novel tauopathy, differing from known dementia and parkinsonism syndromes, including PSP.

Number of accesses :  

Other information