Increased amyloid beta-peptide deposition in cerebral cortex as a consequence of apolipoprotein E genotype in late-onset Alzheimer disease.

D. E. Schmechel; Ann M. Saunders; Warren J. Strittmatter; Barbara J. Crain; Christine M. Hulette; Sun Hyung Joo; Margaret A. Pericak‐Vance; Dmitry Goldgaber; Allen D. Roses

doi:10.1073/pnas.90.20.9649

Increased amyloid beta-peptide deposition in cerebral cortex as a consequence of apolipoprotein E genotype in late-onset Alzheimer disease.

D. E. Schmechel(Duke Medical Center), Ann M. Saunders(Duke Medical Center), Warren J. Strittmatter(Duke Medical Center), Barbara J. Crain(Duke Medical Center), Christine M. Hulette(Duke Medical Center), Sun Hyung Joo(Duke Medical Center), Margaret A. Pericak‐Vance(Duke Medical Center), Dmitry Goldgaber(Duke Medical Center), Allen D. Roses(Duke Medical Center)

Proceedings of the National Academy of Sciences

October 15, 1993

10.1073/pnas.90.20.9649

Cited by 1,525Open Access

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Abstract

Amyloid beta-peptide (A beta) deposition in senile plaques and cerebral vessels is a neuropathological feature of Alzheimer disease (AD). We examined the possibility that commonly observed variability in A beta deposition in late-onset AD might be related to apolipoprotein E genotype (APOE gene; the two most common alleles are 3 and 4), since APOE4 is a susceptibility gene for late-onset AD and apolipoprotein E interacts strongly with A beta in vitro. In an autopsy series of brains of late-onset AD patients, we found a strong association of APOE4 allele with increased vascular and plaque A beta deposits. Late-onset AD patients with one or two APOE4 alleles have a distinct neuropathological phenotype compared with patients homozygous for APOE3.

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