作者
PH St George-Hyslop, JL Haines, LA Farrer, R Polinsky, C Van Broeckhoven, A Goate, DR Crapper McLachlan, H Orr, AC Bruni, Sandro Sorbi, Innocenzo Rainero, J-F Foncin, D Pollen, JM Cantu, R Tupler, N Voskresenskaya, R Mayeux, J Growdon, VA Fried, RH Myers, L Nee, H Backhovens, JJ Martin, M Rossor, Michael John Owen, M Mullan, ME Percy, H Karlinsky, S Rich, L Heston, M Montesi, M Mortilla, N Nacmias, JF Gusella, JA Hardy
发表日期
1990/9/13
期刊
Nature
卷号
347
期号
6289
页码范围
194-197
出版商
Nature Publishing Group UK
简介
ALZHEIMER'S disease, a fatal neurodegenerative disorder of unknown aetiology, is usually considered to be a single disorder because of tbe general uniformity of the disease phenotype1,2. Two recent genetic linkage studies revealed co-segregation of familial Alzheimer disease with the D21S1/S11 and D21S16 loci on chromosome 21 (refs 3,4). But two other studies, one of pre-dominantly multiplex kindreds with a late age-of-onset5, the other of a cadre of kindreds with a unique Volga German ethnic origin6, found absence of linkage at least to D21S1/S11. So far it has not been possible to discern whether these conflicting reports reflect aetiological heterogeneity, differences in methods of pedigree selection, effects of confounding variables in the analysis (for example, diagnostic errors, assortative matings), or true non-replication. To resolve this issue, we have now examined the inheritance of five polymorphic …
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PH St George-Hyslop, JL Haines, LA Farrer, R Polinsky… - Nature, 1990