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Article type: Short Communication
Authors: Stipho, Faissal | Jackson, Robert | Sabbagh, Marwan N.; *
Affiliations: [a] Department of Neurology, Barrow Neurological Institute, St. Joseph’s Hospital and Medical Center, Phoenix, AZ, USA
Correspondence: [*] Correspondence to: Marwan N. Sabbagh, MD, c/o Neuroscience Publications; Barrow Neurological Institute, St. Joseph’s Hospital and Medical Center, 350 W. Thomas Rd., Phoenix, AZ 85013, USA. Tel.: +1 602 406 3593; Fax: +1 602 406 4104; E-mail: [email protected].
Abstract: Background:Homozygous APOE ɛ4 status is a well-known risk factor in the development of Alzheimer’s disease (AD). However, other genotypes of APOE have not yet been found to have equal clinical significance. There is a paucity of reports regarding clinically or pathologically described AD in APOE ɛ2 homozygotes compared to the other alleles. Objective:To notify clinicians that patients with homozygous APOE ɛ2 are also at risk of developing AD based on results from the largest prospectively gathered registry of brain samples to date. Methods:We queried the National Alzheimer’s Coordinating Center (NACC) database for autopsy-confirmed AD cases. Of the Uniform Data Set (UDS) participants who are deceased, 5,779 were diagnosed with dementia at their last UDS visit prior to death, and autopsy data is available for 3,518. Results:Of the brains in the NACC database with pathologically confirmed dementia, seven were found to be homozygous for APOE ɛ2, which represents only 0.2% of the autopsy-confirmed sample. Furthermore, pathology-confirmed AD represents 29% (2/7) of the APOE ɛ2/ɛ2 patients diagnosed with dementia. Conclusions:Although rare, autopsy-confirmed AD can be present in APOE ɛ2/ɛ2 carriers.
Keywords: Alzheimer’s disease, apolipoprotein, brain-derived neurotrophic factor, corticobasal degeneration, dementia, frontotemporal dementia
DOI: 10.3233/JAD-171060
Journal: Journal of Alzheimer's Disease, vol. 62, no. 4, pp. 1527-1530, 2018
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