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April 22, 2014; 82 (16) Article

Late-onset Alzheimer disease genetic variants in posterior cortical atrophy and posterior AD

Minerva M. Carrasquillo, Qurat ul Ain Khan, Melissa E. Murray, Siddharth Krishnan, Jeremiah Aakre, V. Shane Pankratz, Thuy Nguyen, Li Ma, Gina Bisceglio, Ronald C. Petersen, Steven G. Younkin, Dennis W. Dickson, Bradley F. Boeve, Neill R. Graff-Radford, Nilüfer Ertekin-Taner
First published March 26, 2014, DOI: https://doi.org/10.1212/WNL.0000000000000335
Minerva M. Carrasquillo
From the Departments of Neuroscience (M.M.C., M.E.M., S.K., T.N., L.M., G.B., S.G.Y., D.W.D., N.E.-T.) and Neurology (Q.u.A.K., N.R.G.-R., N.E.-T.), Mayo Clinic Florida, Jacksonville; and Departments of Biostatistics (J.A., V.S.P.) and Neurology (R.C.P., B.F.B.), Mayo Clinic Minnesota, Rochester.
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Qurat ul Ain Khan
From the Departments of Neuroscience (M.M.C., M.E.M., S.K., T.N., L.M., G.B., S.G.Y., D.W.D., N.E.-T.) and Neurology (Q.u.A.K., N.R.G.-R., N.E.-T.), Mayo Clinic Florida, Jacksonville; and Departments of Biostatistics (J.A., V.S.P.) and Neurology (R.C.P., B.F.B.), Mayo Clinic Minnesota, Rochester.
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Melissa E. Murray
From the Departments of Neuroscience (M.M.C., M.E.M., S.K., T.N., L.M., G.B., S.G.Y., D.W.D., N.E.-T.) and Neurology (Q.u.A.K., N.R.G.-R., N.E.-T.), Mayo Clinic Florida, Jacksonville; and Departments of Biostatistics (J.A., V.S.P.) and Neurology (R.C.P., B.F.B.), Mayo Clinic Minnesota, Rochester.
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Siddharth Krishnan
From the Departments of Neuroscience (M.M.C., M.E.M., S.K., T.N., L.M., G.B., S.G.Y., D.W.D., N.E.-T.) and Neurology (Q.u.A.K., N.R.G.-R., N.E.-T.), Mayo Clinic Florida, Jacksonville; and Departments of Biostatistics (J.A., V.S.P.) and Neurology (R.C.P., B.F.B.), Mayo Clinic Minnesota, Rochester.
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Jeremiah Aakre
From the Departments of Neuroscience (M.M.C., M.E.M., S.K., T.N., L.M., G.B., S.G.Y., D.W.D., N.E.-T.) and Neurology (Q.u.A.K., N.R.G.-R., N.E.-T.), Mayo Clinic Florida, Jacksonville; and Departments of Biostatistics (J.A., V.S.P.) and Neurology (R.C.P., B.F.B.), Mayo Clinic Minnesota, Rochester.
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V. Shane Pankratz
From the Departments of Neuroscience (M.M.C., M.E.M., S.K., T.N., L.M., G.B., S.G.Y., D.W.D., N.E.-T.) and Neurology (Q.u.A.K., N.R.G.-R., N.E.-T.), Mayo Clinic Florida, Jacksonville; and Departments of Biostatistics (J.A., V.S.P.) and Neurology (R.C.P., B.F.B.), Mayo Clinic Minnesota, Rochester.
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Thuy Nguyen
From the Departments of Neuroscience (M.M.C., M.E.M., S.K., T.N., L.M., G.B., S.G.Y., D.W.D., N.E.-T.) and Neurology (Q.u.A.K., N.R.G.-R., N.E.-T.), Mayo Clinic Florida, Jacksonville; and Departments of Biostatistics (J.A., V.S.P.) and Neurology (R.C.P., B.F.B.), Mayo Clinic Minnesota, Rochester.
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Li Ma
From the Departments of Neuroscience (M.M.C., M.E.M., S.K., T.N., L.M., G.B., S.G.Y., D.W.D., N.E.-T.) and Neurology (Q.u.A.K., N.R.G.-R., N.E.-T.), Mayo Clinic Florida, Jacksonville; and Departments of Biostatistics (J.A., V.S.P.) and Neurology (R.C.P., B.F.B.), Mayo Clinic Minnesota, Rochester.
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Gina Bisceglio
From the Departments of Neuroscience (M.M.C., M.E.M., S.K., T.N., L.M., G.B., S.G.Y., D.W.D., N.E.-T.) and Neurology (Q.u.A.K., N.R.G.-R., N.E.-T.), Mayo Clinic Florida, Jacksonville; and Departments of Biostatistics (J.A., V.S.P.) and Neurology (R.C.P., B.F.B.), Mayo Clinic Minnesota, Rochester.
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Ronald C. Petersen
From the Departments of Neuroscience (M.M.C., M.E.M., S.K., T.N., L.M., G.B., S.G.Y., D.W.D., N.E.-T.) and Neurology (Q.u.A.K., N.R.G.-R., N.E.-T.), Mayo Clinic Florida, Jacksonville; and Departments of Biostatistics (J.A., V.S.P.) and Neurology (R.C.P., B.F.B.), Mayo Clinic Minnesota, Rochester.
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Steven G. Younkin
From the Departments of Neuroscience (M.M.C., M.E.M., S.K., T.N., L.M., G.B., S.G.Y., D.W.D., N.E.-T.) and Neurology (Q.u.A.K., N.R.G.-R., N.E.-T.), Mayo Clinic Florida, Jacksonville; and Departments of Biostatistics (J.A., V.S.P.) and Neurology (R.C.P., B.F.B.), Mayo Clinic Minnesota, Rochester.
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Dennis W. Dickson
From the Departments of Neuroscience (M.M.C., M.E.M., S.K., T.N., L.M., G.B., S.G.Y., D.W.D., N.E.-T.) and Neurology (Q.u.A.K., N.R.G.-R., N.E.-T.), Mayo Clinic Florida, Jacksonville; and Departments of Biostatistics (J.A., V.S.P.) and Neurology (R.C.P., B.F.B.), Mayo Clinic Minnesota, Rochester.
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Bradley F. Boeve
From the Departments of Neuroscience (M.M.C., M.E.M., S.K., T.N., L.M., G.B., S.G.Y., D.W.D., N.E.-T.) and Neurology (Q.u.A.K., N.R.G.-R., N.E.-T.), Mayo Clinic Florida, Jacksonville; and Departments of Biostatistics (J.A., V.S.P.) and Neurology (R.C.P., B.F.B.), Mayo Clinic Minnesota, Rochester.
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Neill R. Graff-Radford
From the Departments of Neuroscience (M.M.C., M.E.M., S.K., T.N., L.M., G.B., S.G.Y., D.W.D., N.E.-T.) and Neurology (Q.u.A.K., N.R.G.-R., N.E.-T.), Mayo Clinic Florida, Jacksonville; and Departments of Biostatistics (J.A., V.S.P.) and Neurology (R.C.P., B.F.B.), Mayo Clinic Minnesota, Rochester.
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Nilüfer Ertekin-Taner
From the Departments of Neuroscience (M.M.C., M.E.M., S.K., T.N., L.M., G.B., S.G.Y., D.W.D., N.E.-T.) and Neurology (Q.u.A.K., N.R.G.-R., N.E.-T.), Mayo Clinic Florida, Jacksonville; and Departments of Biostatistics (J.A., V.S.P.) and Neurology (R.C.P., B.F.B.), Mayo Clinic Minnesota, Rochester.
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Full PDF
Citation
Late-onset Alzheimer disease genetic variants in posterior cortical atrophy and posterior AD
Minerva M. Carrasquillo, Qurat ul Ain Khan, Melissa E. Murray, Siddharth Krishnan, Jeremiah Aakre, V. Shane Pankratz, Thuy Nguyen, Li Ma, Gina Bisceglio, Ronald C. Petersen, Steven G. Younkin, Dennis W. Dickson, Bradley F. Boeve, Neill R. Graff-Radford, Nilüfer Ertekin-Taner
Neurology Apr 2014, 82 (16) 1455-1462; DOI: 10.1212/WNL.0000000000000335

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Abstract

Objective: To investigate association of genetic risk factors for late-onset Alzheimer disease (LOAD) with risk of posterior cortical atrophy (PCA), a syndrome of visual impairment with predominant Alzheimer disease (AD) pathology in posterior cortical regions, and with risk of “posterior AD” neuropathology.

Methods: We assessed 81 participants with PCA diagnosed clinically and 54 with neuropathologic diagnosis of posterior AD vs 2,523 controls for association with 11 significant single nucleotide polymorphisms (SNPs) from published LOAD risk genome-wide association studies.

Results: There was highly significant association with APOE ε4 and increased risk of PCA (p = 0.0003, odds ratio [OR] = 3.17) and posterior AD (p = 1.11 × 10−17, OR = 6.43). No other locus was significant after corrections for multiple testing, although rs11136000 near CLU (p = 0.019, OR = 0.60) and rs744373 near BIN1 (p = 0.025, OR = 1. 63) associated nominally significantly with posterior AD, and rs3851179 at the PICALM locus had significant association with PCA (p = 0.0003, OR = 2.84). ABCA7 locus SNP rs3764650, which was also tested under the recessive model because of Hardy-Weinberg disequilibrium, also had nominally significant association with PCA risk. The direction of association at APOE, CLU, and BIN1 loci was the same for participants with PCA and posterior AD. The effects for all SNPs, except rs3851179, were consistent with those for LOAD risk.

Conclusions: We identified a significant effect for APOE and nominate CLU, BIN1, and ABCA7 as additional risk loci for PCA and posterior AD. Our findings suggest that at least some of the genetic risk factors for LOAD are shared with these atypical conditions and provide effect-size estimates for their future genetic studies.

GLOSSARY

AD=
Alzheimer disease;
BA=
Brodmann area;
CI=
confidence interval;
GWAS=
genome-wide association study;
LOAD=
late-onset Alzheimer disease;
MAF=
minor allele frequency;
NFT=
neurofibrillary tangle;
OR=
odds ratio;
PCA=
posterior cortical atrophy;
SNP=
single nucleotide polymorphism

Footnotes

  • Go to Neurology.org for full disclosures. Funding information and disclosures deemed relevant by the authors, if any, are provided at the end of the article.

  • Supplemental data at Neurology.org

  • Received July 5, 2013.
  • Accepted in final form January 21, 2014.
  • © 2014 American Academy of Neurology
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