Self-Assembly of a Model Peptide Incorporating a Hexa-Histidine Sequence Attached to an Oligo-Alanine Sequence, and Binding to Gold NTA/Nickel Nanoparticles
Author(s) -
Ian W. Hamley,
Steven Kirkham,
Ashkan Dehsorkhi,
Valeria Castelletto,
Jozef Adamčík,
Raffaele Mezzenga,
Janne Ruokolainen,
Claudia Mazzuca,
Emanuela Gatto,
Mariano Venanzi,
E. Placidi,
Panayiotis Bilalis,
Hermis Iatrou
Publication year - 2014
Publication title -
biomacromolecules
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.689
H-Index - 220
eISSN - 1526-4602
pISSN - 1525-7797
DOI - 10.1021/bm500950c
Subject(s) - peptide , chemistry , fibril , circular dichroism , colloidal gold , nanoparticle , hexa , histidine , sequence (biology) , peptide sequence , amyloid (mycology) , biophysics , crystallography , nanotechnology , biochemistry , amino acid , materials science , inorganic chemistry , biology , gene
Amyloid fibrils are formed by a model surfactant-like peptide (Ala)10-(His)6 containing a hexa-histidine tag. This peptide undergoes a remarkable two-step self-assembly process with two distinct critical aggregation concentrations (cac's), probed by fluorescence techniques. A micromolar range cac is ascribed to the formation of prefibrillar structures, whereas a millimolar range cac is associated with the formation of well-defined but more compact fibrils. We examine the labeling of these model tagged amyloid fibrils using Ni-NTA functionalized gold nanoparticles (Nanogold). Successful labeling is demonstrated via electron microscopy imaging. The specificity of tagging does not disrupt the β-sheet structure of the peptide fibrils. Binding of fibrils and Nanogold is found to influence the circular dichroism associated with the gold nanoparticle plasmon absorption band. These results highlight a new approach to the fabrication of functionalized amyloid fibrils and the creation of peptide/nanoparticle hybrid materials.
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