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Literature DB >> 1676700

Exclusion of linkage to the pericentromeric region of chromosome 21 in the Canadian pedigree with familial Alzheimer disease.

S M Pulst¹, P Fain, V Cohn, L E Nee, R J Polinsky, J R Korenberg.

Abstract

Alzheimer disease (AD) is a devastating neurodegenerative disease leading to global dementia. The familial form (FAD) has been linked to markers on chromosome 21 in some families, most tightly to the loci D21S16 and D21S13 located close to the centromere of the long arm. In other families the FAD mutation has been excluded from the more telomeric D21S1/S11 region, but not from the centromeric region of chromosome 21. We identified two new restriction fragment length polymorphisms (RFLPs) for the locus D21S13 and have used these RFLPs for the analysis of one of the largest known early-onset FAD pedigrees. We calculated pairwise and multipoint lod scores for the loci D21S13, D21S110, and D21S11. Linkage to this region of chromosome 21 was excluded with maximum negative lod scores of -6.4 at D21S13 and D21S110. Thus, it is unlikely that the FAD mutation in this family is located in the region that has shown linkage in other FAD pedigrees. This result provides evidence for genetic heterogeneity of early-onset FAD or a location of FAD centromeric to D21S13.

Entities: Disease Gene

Mesh：

Substances：

Year: 1991 PMID： 1676700 DOI： 10.1007/bf00204173

Source DB: PubMed Journal: Hum Genet ISSN： 0340-6717 Impact factor: 4.132

15 in total

1. A genetic linkage map of 17 markers on human chromosome 21.

Authors: A C Warren; S A Slaugenhaupt; J G Lewis; A Chakravarti; S E Antonarakis
Journal: Genomics Date: 1989-05 Impact factor: 5.736

2. Predisposing locus for Alzheimer's disease on chromosome 21.

Authors: A M Goate; A R Haynes; M J Owen; M Farrall; L A James; L Y Lai; M J Mullan; P Roques; M N Rossor; R Williamson
Journal: Lancet Date: 1989-02-18 Impact factor: 79.321

Review 3. Alzheimer's disease.

Authors: R Katzman
Journal: N Engl J Med Date: 1986-04-10 Impact factor: 91.245

4. Genetic linkage studies suggest that Alzheimer's disease is not a single homogeneous disorder.

Authors: P H St George-Hyslop; J L Haines; L A Farrer; R Polinsky; C Van Broeckhoven; A Goate; D R McLachlan; H Orr; A C Bruni; S Sorbi; I Rainero; J F Foncin; D Pollen; J M Cantu; R Tupler; N Voskresenskaya; R Mayeux; J Growden; V A Fried; R H Myers; L Nee; H Backhovens; J J Martin; M Rossor; M J Owen; M Mullan; M E Percy; H Karlinsky; S Rich; L Heston; M Montesi; M Mortilla; N Nacmias; J F Gusella; J A Hardy
Journal: Nature Date: 1990-09-13 Impact factor: 49.962

Exclusion of linkage to the pericentromeric region of chromosome 21 in the Canadian pedigree with familial Alzheimer disease.

1. A genetic linkage map of 17 markers on human chromosome 21.

2. Predisposing locus for Alzheimer's disease on chromosome 21.

Review 3. Alzheimer's disease.

4. Genetic linkage studies suggest that Alzheimer's disease is not a single homogeneous disorder.

5. A family with histologically confirmed Alzheimer's disease.

6. The achondroplasia gene is not linked to the locus for neurofibromatosis 1 on chromosome 17.

7. The genetic defect causing familial Alzheimer's disease maps on chromosome 21.

8. Absence of linkage of chromosome 21q21 markers to familial Alzheimer's disease.

9. A new EcoRI polymorphism at the D21S13 locus.

10. A new HaeIII polymorphism at the D21S13 locus.

1. Potassium channel dysfunction in fibroblasts identifies patients with Alzheimer disease.