The clinical phenotype of two missense mutations in the presenilin I gene in Japanese patients

被引:50
作者
Ikeda, M
Sharma, V
Sumi, M
Rogaeva, EA
Poorkaj, P
Sherrington, R
Nee, L
Tsuda, T
Oda, N
Watanabe, M
Aoki, M
Shoji, M
Abe, K
Itoyama, Y
Hirai, S
Schellenberg, GD
Bird, TD
StGeorgeHyslop, PH
机构
[1] TORONTO HOSP,DEPT MED,TORONTO,ON M5T 2S8,CANADA
[2] UNIV WASHINGTON,SCH MED,DEPT MED,SEATTLE,WA 98195
[3] UNIV WASHINGTON,SCH MED,DEPT NEUROL,SEATTLE,WA 98195
[4] VET AFFAIRS PUGET SOUND HLTH CARE SYST,CTR GERIATR RES EDUC & CLIN,SEATTLE,WA
[5] VET AFFAIRS PUGET SOUND HLTH CARE SYST,NEUROL SECT,SEATTLE,WA
[6] NINCDS,CLIN NEUROPHARMACOL SECT,BETHESDA,MD 20892
[7] TOHOKU UNIV,SCH MED,DEPT NEUROL,MAEBASHI,GUMMA,JAPAN
[8] TOHOKU UNIV,SCH MED,DEPT NEUROL,SENDAI,MIYAGI 980,JAPAN
[9] ISHII HOSP NEUROSURG & OPHTHALMOL,DIV NEUROL & NEUROSURG,IWAKI,FUKUSHIMA,JAPAN
来源
ANNALS OF NEUROLOGY | 1996年 / 40卷 / 06期
关键词
D O I
10.1002/ana.410400614
中图分类号
R74 [神经病学与精神病学];
学科分类号
摘要
We report the clinical and neuropathologic phenotypes associated with two different missense mutations in the presenilin I (PS-I) gene in Japanese patients with early-onset familial Alzheimer's disease (FAD). In the AM/JPN1 pedigree a missense mutation (C-->T) was found at nucleotide 1102, which is predicted to cause an alanine-to-valine missense substitution at codon 260. In this family, the disease had a mean age of onset of 40.3 rears and an indolent course (range, 8-19 years). Neuropathologic studies in 3 members of this pedigree showed widespread senile plaques, neuro-fibrillary tangles, and neuronal loss, as well as abundant perivascular subpial amyloid deposits in the Virchow-Robin spaces and the presence of Pick-like intraneuronal inclusions in the dentate gyrus. In the second pedigree, transmitting a C-->T nucleotide substitution at position 1027, leading to the missense mutation of alanine to valine at codon 285, the disease had a later onset (mean, 51 years) but a more rapid course. Comparison of the disease phenotypes associated with other missense mutations in exon 9 of PS-I reveals no clinical or pathological phenotype, which uniquely distinguishes Alzheimer's disease associated with PS-I mutations from other forms of early-onset PAD, implying that direct mutation screening is required to identify these cases.
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页码:912 / 917
页数:6
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