Strategies for the prevention and treatment of late-onset Alzheimer's disease may be improved by the identification of a gene variant that seems to increase Alzheimer's disease, according to a report by Lars Bertram, M.D., of MassGeneral Institute for Neurodegenerative Diseases, Charlestown, Mass., and his associates.
Variants in the ubiquilin 1 (UBQLN1) gene, located on chromosome 9, may substantially increase the risk of late-onset Alzheimer's disease, which accounts for over 90% of the disease, other investigators have reported.
Dr. Bertram and his associates examined two groups of patients; the first consisted of 1,439 subjects from 437 families with Alzheimer's disease who participated in the National Institute of Mental Health multiplex family study between 1991 and 1997. Of that group, 994 patients had Alzheimer's, 411 were unaffected, and 34 had unknown phenotypes.
The mean age at disease onset was 72 years, the investigators said (N. Engl. J. Med. 2005;352:884–94).
Evaluation of 19 single-nucleotide polymorphisms in three genes within the chromosome 9q linkage region showed that Alzheimer's disease was significantly associated with two single-nucleotide polymorphisms in UBQLN1 and one in APBA1.
Haplotype block structure estimates showed that the single haplotype (H3), almost exclusively defined by the risk allele of UBQ-8i, was associated with a significantly increased rate of transmission to affected subjects. The testing of APBA1 polymorphisms did not indicate such transmission.
Ubiquilin 1 encodes the protein ubiquilin 1, regulates protein degradation, interacts with presenilin 1 and presenilin 2, and promotes the accumulation of presenilin in vitro, they said.
Findings from the second investigation, the Consortium on Alzheimer's Genetics study, showed that the rate of transmission of the H3 haplotype was increased among subjects with Alzheimer's disease. Investigators found no association with rs1411483 in APBA1.
Specimen collection began in 1999 and has been completed for 224 Alzheimer's patients and 265 unaffected siblings. Affected participants were at least 50 years old at disease onset; mean age at onset was 71 years.
Analyses by Dr. Bertram and colleagues on data merged from the two family groups showed the most pronounced single-local signals for UBQ-8i followed by rs2781002 and rs2780995.
Dr. Bertram's group also studied RNA extracts from neocortical brain tissue samples to see if the risk allele UBQ-8i affects the splicing of exon 8 in the UBQLN1 message. They found a relationship between the UBQ-8i allele and a UBQLN1 transcript lacking exon 8 in the 25 samples from patients with Alzheimer's disease.
In an accompanying editorial, Thomas D. Bird, M.D., called UBQLN1 “intriguing as a candidate gene because of its potential role in the proteasome degradation of proteins and its interaction with PS1 and PS2.”
“As always, this new association requires replication and confirmation in additional populations,” commented Dr. Bird, who is professor of neurology, medicine, and psychiatry at the University of Washington, Seattle, and a research neurologist at the Veterans Affairs Medical Center in Seattle (N. Engl. J. Med. 2005;352:862–4).
Dr. Bertram's group observed that “the rampant inconsistencies encountered in genetic analyses of putative candidate genes for Alzheimer's disease in the literature to date” may stem from the fact that most studies are done on groups too small to show moderate genetic effects like that of UBQLN1, instead of the more pronounced effects of APOE.