TY - JOUR
T1 - NMR reveals two-step association of Congo Red to amyloid ß in low-molecular-weight aggregates
AU - Pedersen, Marie Ø
AU - Mikkelsen, Katrine
AU - Behrens, Manja Annette
AU - Pedersen, Jan Skov
AU - Enghild, Jan J.
AU - Skrydstrup, Troels
AU - Malmendal, Anders
AU - Nielsen, Niels Chr
PY - 2010/12/9
Y1 - 2010/12/9
N2 - Aggregation of the Amyloid β peptide into amyloid fibrils is closely related to development of Alzheimer's disease. Many small aromatic compounds have been found to act as inhibitors of fibril formation, and have inspired the search for new drug candidates. However, the detailed mechanisms of inhibition are largely unknown. In this study, we have examined in detail the binding of the fibril-formation inhibitor Congo Red (CR) to monomeric Aβ 1-40 using a combination of 1D, 2D, saturation transfer difference, and diffusion NMR, as well as dynamic light scattering experiments. Our results show that CR binds to the fibril forming stretches of Aβ1-40 monomers, and that complex formation occurs in two steps: An initial 1:1 CR:Aβ1-40 complex is formed by a relatively strong interaction (Kd ≈ 5 μM), and a 2:1 complex is formed by binding another CR molecule in a subsequent weaker binding step (Kd ≈ 300 μM). The size of these complexes is comparable to that of Aβ1-40 alone. The existence of two different complexes might explain the contradictory reports regarding the inhibitory effects of CR on the fibril-formation process.
AB - Aggregation of the Amyloid β peptide into amyloid fibrils is closely related to development of Alzheimer's disease. Many small aromatic compounds have been found to act as inhibitors of fibril formation, and have inspired the search for new drug candidates. However, the detailed mechanisms of inhibition are largely unknown. In this study, we have examined in detail the binding of the fibril-formation inhibitor Congo Red (CR) to monomeric Aβ 1-40 using a combination of 1D, 2D, saturation transfer difference, and diffusion NMR, as well as dynamic light scattering experiments. Our results show that CR binds to the fibril forming stretches of Aβ1-40 monomers, and that complex formation occurs in two steps: An initial 1:1 CR:Aβ1-40 complex is formed by a relatively strong interaction (Kd ≈ 5 μM), and a 2:1 complex is formed by binding another CR molecule in a subsequent weaker binding step (Kd ≈ 300 μM). The size of these complexes is comparable to that of Aβ1-40 alone. The existence of two different complexes might explain the contradictory reports regarding the inhibitory effects of CR on the fibril-formation process.
U2 - 10.1021/jp108035y
DO - 10.1021/jp108035y
M3 - Journal article
C2 - 21077638
SN - 1520-6106
VL - 114
SP - 16003
EP - 16010
JO - Journal of Physical Chemistry Part B: Condensed Matter, Materials, Surfaces, Interfaces & Biophysical
JF - Journal of Physical Chemistry Part B: Condensed Matter, Materials, Surfaces, Interfaces & Biophysical
IS - 48
ER -