LINKAGE AND MUTATIONAL ANALYSIS OF FAMILIAL ALZHEIMER-DISEASE KINDREDS FOR THE APP GENE REGION

被引：2

作者：

KAMINO, K

ORR, HT

PAYAMI, H

WIJSMAN, EM

ALONSO, ME

PULST, SM

ANDERSON, L

ODAHL, S

NEMENS, E

WHITE, JA

SADOVNICK, AD

BALL, MJ

KAYE, J

WARREN, A

MCINNIS, M

ANTONARAKIS, SE

KORENBERG, JR

SHARMA, V

KUKULL, W

LARSON, E

HESTON, LL

MARTIN, GM

BIRD, TD

SCHELLENBERG, GD

机构：

[1] UNIV WASHINGTON,DIV NEUROL,SEATTLE,WA 98195

[2] UNIV WASHINGTON,DIV MED GENET,SEATTLE,WA 98195

[3] UNIV WASHINGTON,DEPT PATHOL,SEATTLE,WA 98195

[4] UNIV WASHINGTON,DEPT EPIDEMIOL,SEATTLE,WA 98195

[5] UNIV WASHINGTON,DEPT MED,SEATTLE,WA 98195

[6] VET ADM MED CTR,DIV NEUROL,SEATTLE,WA 98108

[7] WASHINGTON INST MENT ILLNESS RES & TRAINING,STEILACOOM,WA

[8] UNIV MINNESOTA,DEPT LAB MED & PATHOL,MINNEAPOLIS,MN 55455

[9] UNIV MINNESOTA,INST HUMAN GENET,MINNEAPOLIS,MN 55455

[10] UNIV MINNESOTA,DEPT PSYCHIAT,MINNEAPOLIS,MN 55455

[11] OREGON HLTH SCI UNIV,DEPT MOLEC & MED GENET,PORTLAND,OR 97201

[12] OREGON HLTH SCI UNIV,DEPT NEUROL,PORTLAND,OR 97201

[13] OREGON HLTH SCI UNIV,DIV NEUROPATHOL,PORTLAND,OR 97201

[14] NATL INST NEUROL & NEUROSURG,MEXICO CITY,MEXICO

[15] UNIV CALIF LOS ANGELES,CEDARS SINAI MED CTR,DIV NEUROL,LOS ANGELES,CA 90048

[16] UNIV BRITISH COLUMBIA,DEPT MED GENET,VANCOUVER V6T 1W5,BC,CANADA

[17] JOHNS HOPKINS UNIV,SCH MED,DEPT PSYCHIAT,BALTIMORE,MD 21205

来源：

AMERICAN JOURNAL OF HUMAN GENETICS | 1992年 / 51卷 / 05期

关键词：

D O I：

暂无

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

A large number of familial Alzheimer disease (FAD) kindreds were examined to determine whether mutations in the amyloid precursor protein (APP) gene could be responsible for the disease. Previous studies have identified three mutations at APP codon 717 which are pathogenic for Alzheimer disease (AD). Samples from affected subjects were examined for mutations in exons 16 and 17 of the APP gene. A combination of direct sequencing and single-strand conformational polymorphism analysis was used. Sporadic AD and normal controls were also examined by the same methods. Five sequence variants were identified. One variant at APP codon 693 resulted in a Glu-->Gly change. This is the same codon as the hereditary cerebral hemorrhage with amyloidosis-Dutch type Glu-->Gln mutation. Another single-base change at APP codon 708 did not alter the amino acid encoded at this site. Two point mutations and a 6-bp deletion were identified in the intronic sequences surrounding exon 17. None of the variants could be unambiguously determined to be responsible for FAD. The larger families were also analyzed by testing for linkage of FAD to a highly polymorphic short tandem repeat marker (D21S210) that is tightly linked to APP. Highly negative LOD scores were obtained for the family groups tested, and linkage was formally excluded beyond theta = .10 for the Volga German kindreds, theta = .20 for early-onset non-Volga Germans, and theta = .10 for late-onset families. LOD scores for linkage of FAD to markers centromeric to APP (D21S1/S11, D21S13, and D21S215) were also negative in the three family groups. These studies show that APP mutations account for AD in only a small fraction of FAD kindreds.

引用

页码：998 / 1014

页数：17

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