Skip to main content
OSTI.GOVU.S. Department of Energy Office of Scientific and Technical Information
U.S. Department of Energy
Office of Scientific and Technical Information
 

Genetic heterogeneity and Alzheimer`s disease

Journal Article · · American Journal of Human Genetics
OSTI ID:134722
;  [1];  [2]
  1. Univ. of Washington, Seattle (United States)
  2. Veteran`s Affairs Medical Center, Seattle, WA (United States)
+ Show Author Affiliations
In some early-onset Alzheimer`s disease (AD) families, inheritance is autosomal dominant. (Early-onset AD is arbitarily defined as onset at {le} 60 years.) Two loci have been identified which are causative for early-onset familial AD (FAD). One is the amyloid precursor protein gene in which specific mutation have been identified. The second is a locus at 14q24.3 (AD3) which has been localized by linkage analysis; the gene and specific mutations have not been identified. Linkage studies place this locus between D14S61 and D14S63. These 2 loci, however, do not account for all early-onset FAD. The Volga German (VG) kindreds are descendants of families which emigrated from Germany to the Volga river region of Russia and subsequently to the US; AD in these families is hypothesized to be the result of a common genetic founder. The average age-at-onset in these families is 57 years. Linkage analysis for this group has been negative for the APP gene and for chromosome 14 markers. Thus, there is at least 1 other early-onset FAD locus. Recently, the {epsilon}4 allele of apolipoprotein E (ApoE) was identified as a risk-factor for late-onset AD. In a series of 53 late-onset kindreds, a strong genetic association was observed between the ApoE {epsilon}4 allele and AD. However, when linkage analysis was performed using a highly polymorphic locus at the ApoCII gene, which is within 30 kb of ApoE, significant evidence for co-segregation was not observed. This and other data suggests that while ApoE is an age-at-onset modifying locus, another gene(s), located elsewhere, contribute(s) to late-onset AD. Thus, there is probably at least 1 other late-onset locus. Once the VG locus is identified, it will be possible to determine whether an allelic variant of this locus is responsible for late-onset FAD.
OSTI ID:
134722
Report Number(s):
CONF-941009--
Journal Information:
American Journal of Human Genetics, Journal Name: American Journal of Human Genetics Journal Issue: Suppl.3 Vol. 55; ISSN AJHGAG; ISSN 0002-9297
Country of Publication:
United States
Language:
English

Similar Records

Exclusion mapping of familial Alzheimer disease (FAD) in the Volga Germans
Journal Article · Thu Sep 01 00:00:00 EDT 1994 · American Journal of Human Genetics · OSTI ID:134703
The apolipoprotein E/CI/CII gene cluster and late-onset Alzheimer disease
Journal Article · Thu Mar 31 23:00:00 EST 1994 · American Journal of Human Genetics; (United States) · OSTI ID:7105259
Chromosome 14 and late-onset familial alzheimer disease (FAD)
Journal Article · Wed Sep 01 00:00:00 EDT 1993 · American Journal of Human Genetics; (United States) · OSTI ID:5016810

Related Subjects

55 BIOLOGY AND MEDICINE
BASIC STUDIES
AGE DEPENDENCE
APOLIPOPROTEINS
DOMINANT MUTATIONS
FEDERAL REPUBLIC OF GERMANY
GENE MUTATIONS
GENES
GENETIC MAPPING
GENETICS
HEREDITARY DISEASES
HUMAN CHROMOSOME 14
MENTAL DISORDERS
NERVOUS SYSTEM DISEASES
PATIENTS