Association between coding variability in the LRP gene and the risk of late-onset Alzheimer’s disease

被引:0
|
作者
Fabienne Wavrant-DeVrièze
Jean-Charles Lambert
L. Stas
Richard Crook
Dominique Cottel
Florence Pasquier
Bernard Frigard
Martine Lambrechts
E. Thiry
Philippe Amouyel
J. Pérez-Tur
M. C. Chartier-Harlin
John Hardy
Fred Van Leuven
机构
[1] Mayo Clinic Jacksonville,
[2] 4500 San Pablo Rd.,undefined
[3] Jacksonville,undefined
[4] Fl 32224,undefined
[5] USA e-mail: hardy@mayo.edu,undefined
[6] Fax: +1904-953-7370,undefined
[7] CJF 95-05 INSERM 508,undefined
[8] Institut Pasteur de Lille,undefined
[9] 1 Rue du Pr Calmette BP 245,undefined
[10] F-59019 Lille Cedex,undefined
[11] France,undefined
[12] Experimental Genetics Group,undefined
[13] Center for Human Genetics,undefined
[14] Flanders Institute for Biotechnology,undefined
[15] K.U.Leuven – Campus Gasthuisberg ON 06,undefined
[16] B-3000 Leuven,undefined
[17] Belgium,undefined
[18] CHRU de Lille,undefined
[19] Clinique Neurologique,undefined
[20] Centre de la Mémoire,undefined
[21] Hôpital Roger Salengro,undefined
[22] F-59037 Lille Cédex,undefined
[23] France,undefined
[24] Centre de Gériatrie de Wasquehal Molinel,undefined
[25] Rue Salvador Allende,undefined
[26] BP165,undefined
[27] F-59444 Wesquehal,undefined
[28] France,undefined
来源
Human Genetics | 1999年 / 104卷
关键词
Genetic Variability; Regulatory Element; Genetic Data; Large Gene; Major Site;
D O I
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中图分类号
学科分类号
摘要
We have sequenced the entire (89 exons) open reading frame of the LRP gene in 12 cases of Alzheimer’s disease (AD) from Northern France. We have found no novel changes but confirm the occurrence of a polymorphism in exon 6 of the gene (A216V). This polymorphism is rare (2.8% of controls) and is in linkage equilibrium with previously reported polymorphisms. The V216 allele is negatively associated with the disease in a large case-controlled series. These data suggest that the LRP receptor may be involved in the pathobiology of AD, but the association that we report here cannot explain the previously reported genetic data implicating the LRP gene in AD. If the LRP gene is a major site of genetic variability leading to AD, there must be other biologically relevant variability in promoter or other regulatory elements of this large gene.
引用
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页码:432 / 434
页数:2
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