Heterogeneity of water‐soluble amyloid β‐peptide in Alzheimer's disease and Down's syndrome brains

Claudio Russo; Takaomi C. Saido; Laura M. DeBusk; Massimo Tabaton; Pierluigi Gambetti; Jan K. Teller

doi:10.1016/s0014-5793(97)00564-4

Heterogeneity of water‐soluble amyloid β‐peptide in Alzheimer's disease and Down's syndrome brains

Claudio Russo(Case Western Reserve University), Takaomi C. Saido(Tokyo Metropolitan Institute of Medical Science), Laura M. DeBusk(Case Western Reserve University), Massimo Tabaton(University of Genoa), Pierluigi Gambetti(Case Western Reserve University), Jan K. Teller(Case Western Reserve University)

FEBS Letters

June 16, 1997

10.1016/s0014-5793(97)00564-4

Cited by 123Open Access

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Abstract

Water-soluble amyloid beta-peptides (sA beta), ending at residue 42, precede amyloid plaques in Down's syndrome (DS). Here we report that sA beta consists of the full-length A beta(1-42) and peptides truncated and modified by cyclization of the N-terminal glutamates, A beta[3(pE)-42] and A beta[11(pE)-42]. The A beta[3(pE)-42] peptide is the most abundant form of sA beta in Alzheimer's disease (AD) brains. In DS, sA beta[3(pE)-42] concentration increases with age and the peptide becomes a dominant species in the presence of plaques. Both pyroglutamate-modified peptides and the full-length A beta form a stable aggregate that is water soluble. The findings point to a crucial role of the aggregated and modified sA beta in the plaque formation and pathogenesis of AD.

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