Structures of oligomers of a peptide from β-amyloid.

J Am Chem Soc

Department of Chemistry, University of California, Irvine, Irvine, California 92697-2025, USA.

Published: August 2013

AI Article Synopsis

  • Amyloid oligomers, particularly those formed by the amyloid-β peptide (Aβ), are key players in Alzheimer's and other amyloid diseases, but their structures remain poorly defined.
  • This research utilizes a macrocyclic peptide to stabilize Aβ oligomers and successfully elucidates their structures through X-ray crystallography, revealing unique assembly forms such as cruciform tetramers and triangular dodecamers.
  • The study’s findings highlight the potential interactions of these oligomers with cell membranes and deepen our understanding of their role in amyloid-related diseases.

Article Abstract

Amyloid oligomers play a central role in Alzheimer's and other amyloid diseases, and yet the structures of these heterogeneous and unstable species are not well understood. To better understand the structures of oligomers formed by amyloid-β peptide (Aβ), we have incorporated a key amyloidogenic region of Aβ into a macrocyclic peptide that stabilizes oligomers and facilitates structural elucidation by X-ray crystallography. This paper reports the crystallographic structures of oligomers and oligomer assemblies formed by a macrocycle containing the Aβ(15-23) nonapeptide. The macrocycle forms hydrogen-bonded β-sheets that assemble into cruciform tetramers consisting of eight β-strands in a two-layered assembly. Three of the cruciform tetramers assemble into a triangular dodecamer. These oligomers further assemble in the lattice to form hexagonal pores. Molecular modeling studies suggest that the natural Aβ peptide can form similar oligomers and oligomer assemblies. The crystallographic and molecular modeling studies suggest the potential for interaction of the oligomers with cell membranes and provide insights into the role of oligomers in amyloid diseases.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3787202PMC
http://dx.doi.org/10.1021/ja4068854DOI Listing

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