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SNPs associated with cerebrospinal fluid Phospho-tau levels influence rate of decline in alzheimer's disease
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نویسنده
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cruchaga c. ,kauwe j.s.k. ,mayo k. ,spiegel n. ,bertelsen s. ,nowotny p. ,shah a.r. ,abraham r. ,hollingworth p. ,harold d. ,owen m.m. ,williams j. ,lovestone s. ,peskind e.r. ,li g. ,leverenz j.b. ,galasko d. ,morris j.c. ,fagan a.m. ,holtzman d.m. ,goate a.m.
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منبع
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plos genetics - 2010 - دوره : 6 - شماره : 9
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چکیده
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Alzheimer's disease (ad) is a complex and multifactorial disease. while large genome-wide association studies have had some success in identifying novel genetic risk factors for ad,case-control studies are less likely to uncover genetic factors that influence progression of disease. an alternative approach to identifying genetic risk for ad is the use of quantitative traits or endophenotypes. the use of endophenotypes has proven to be an effective strategy,implicating genetic risk factors in several diseases,including anemia,osteoporosis and heart disease. in this study we identify a genetic factor associated with the rate of decline in ad patients and present a methodology for identification of other such factors. we have used an established biomarker for ad,cerebrospinal fluid (csf) tau phosphorylated at threonine 181 (ptau181) levels as an endophenotype for ad,identifying a snp,rs1868402,in the gene encoding the regulatory sub-unit of protein phosphatase b,associated with csf ptau181 levels in two independent csf series (pcombined=1.17×10-05). we show no association of rs1868402 with risk for ad or age at onset,but detected a very significant association with rate of progression of disease that is consistent in two independent series(pcombined=1.71×10-05). our analyses suggest that genetic variants associated with csf ptau181 levels may have a greater impact on rate of progression,while genetic variants such as apoe4,that are associated with csf aβ42 levels influence risk and onset but not the rate of progression. our results also suggest that drugs that inhibit or decrease tau phosphorylation may slow cognitive decline in individuals with very mild dementia or delay the appearance of memory problems in elderly individuals with low csf aβ42 levels. finally,we believe genome-wide association studies of csf tau/ptau181 levels should identify novel genetic variants which will likely influence rate of progression of ad. © 2010 cruchaga et al.
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آدرس
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department of psychiatry,washington university school of medicine,st. louis,mo,united states,th e hope center program on protein aggregation and neurodegeneration (hpan),washington university school of medicine,st. louis,mo, United States, department of biology,brigham young univ ersity,provo,ut, United States, department of psychiatry,washington university school of medicine,st. louis,mo,united states,th e hope center program on protein aggregation and neurodegeneration (hpan),washington university school of medicine,st. louis,mo, United States, department of psychiatry,washington university school of medicine,st. louis,mo,united states,th e hope center program on protein aggregation and neurodegeneration (hpan),washington university school of medicine,st. louis,mo, United States, department of psychiatry,washington university school of medicine,st. louis,mo, United States, department of psychiatry,washington university school of medicine,st. louis,mo,united states,th e hope center program on protein aggregation and neurodegeneration (hpan),washington university school of medicine,st. louis,mo, United States, th e hope center program on protein aggregation and neurodegeneration (hpan),washington university school of medicine,st. louis,mo,united states,department of neurology,washington university school of medicine,st. louis,mo, United States, department of neurology,university of washington school of medicine,seattle,wa, United States, de partment of psychological medicine,medical research council (mrc) centre for neuropsychiatric genetics and genomics,school of medicine,cardiff university,cardiff, United Kingdom, de partment of psychological medicine,medical research council (mrc) centre for neuropsychiatric genetics and genomics,school of medicine,cardiff university,cardiff, United Kingdom, de partment of psychological medicine,medical research council (mrc) centre for neuropsychiatric genetics and genomics,school of medicine,cardiff university,cardiff, United Kingdom, de partment of psychological medicine,medical research council (mrc) centre for neuropsychiatric genetics and genomics,school of medicine,cardiff university,cardiff, United Kingdom, kings college,london, United Kingdom, departments of psychiatry and behavioral sciences,university of washington school of medicine,seattle,wa,united states,veterans affairs northwest network mental illness research,education,and clinical center,seattle,wa, United States, departments of psychiatry and behavioral sciences,university of washington school of medicine,seattle,wa,united states,veterans affairs northwest network mental illness research,education,and clinical center,seattle,wa, United States, departments of psychiatry and behavioral sciences,university of washington school of medicine,seattle,wa,united states,veterans affairs northwest network mental illness research,education,and clinical center,seattle,wa,united states,department of neurology,university of washington school of medicine,seattle,wa, United States, department of neurosciences,university of california san diego,la jolla,ca, United States, department of neurology,washington university school of medicine,st. louis,mo,united states,kings college,london,united kingdom,department of pathology and immunology,washington university school of medicine,st. louis,mo, United States, th e hope center program on protein aggregation and neurodegeneration (hpan),washington university school of medicine,st. louis,mo,united states,department of neurology,washington university school of medicine,st. louis,mo,united states,alzheimer's disease research center,washington university school of medicine,st. louis,mo, United States, th e hope center program on protein aggregation and neurodegeneration (hpan),washington university school of medicine,st. louis,mo,united states,department of neurology,washington university school of medicine,st. louis,mo,united states,department of developmental biology,washington university school of medicine,st. louis,mo,united states,alzheimer's disease research center,washington university school of medicine,st. louis,mo, United States, department of psychiatry,washington university school of medicine,st. louis,mo,united states,th e hope center program on protein aggregation and neurodegeneration (hpan),washington university school of medicine,st. louis,mo,united states,department of neurology,washington university school of medicine,st. louis,mo,united states,alzheimer's disease research center,washington university school of medicine,st. louis,mo, United States
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Authors
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