2. Academic Validation
  3. Inhibition of Aβ Amyloid Growth and Toxicity by Silybins: The Crucial Role of Stereochemistry

Inhibition of Aβ Amyloid Growth and Toxicity by Silybins: The Crucial Role of Stereochemistry

  • ACS Chem Neurosci. 2017 Aug 16;8(8):1767-1778. doi: 10.1021/acschemneuro.7b00110.
Michele F M Sciacca 1 Valeria Romanucci 2 Armando Zarrelli 2 Irene Monaco 1 Fabio Lolicato 3 4 Natalia Spinella 5 Clelia Galati 5 Giuseppe Grasso 6 Luisa D'Urso 6 Margherita Romeo 7 Luisa Diomede 7 Mario Salmona 7 Corrado Bongiorno 8 Giovanni Di Fabio 2 Carmelo La Rosa 6 Danilo Milardi 1
Affiliations

Affiliations

  • 1 Institute of Biostructures and Bioimages-Catania, National Research Council, Via Paolo Gaifami 8, 95126 Catania, Italy.
  • 2 Department of Chemical Sciences, University of Napoli "Federico II" , Via Cintia 4, I-80126 Napoli, Italy.
  • 3 Department of Physics, University of Helsinki , P.O. Box 64, FI-00014 Helsinki, Finland.
  • 4 Department of Physics, Tampere University of Technology , P.O. Box 692, FI-33101 Tampere, Finland.
  • 5 STMicroelectronics , Stradale Primosole 50, 95121 Catania, Italy.
  • 6 Dipartimento di Scienze Chimiche, Università degli Studi di Catania , Viale Andrea Doria 6, 95125 Catania, Italy.
  • 7 IRCCS-Istituto di Ricerche Farmacologiche "Mario Negri" , Via Giuseppe La Masa 19, 20156, Milano, Italy.
  • 8 Institute for Microelectronics and Microsystems, National Research Council, Stradale Primosole 50, 95121 Catania, Italy.
PMID: 28562008 DOI: 10.1021/acschemneuro.7b00110
Abstract

The self-assembling of the amyloid β (Aβ) peptide into neurotoxic aggregates is considered a central event in the pathogenesis of Alzheimer's disease (AD). Based on the "amyloid hypothesis", many efforts have been devoted to designing molecules able to halt disease progression by inhibiting Aβ self-assembly. Here, we combine biophysical (ThT assays, TEM and AFM imaging), biochemical (WB and ESI-MS), and computational (all-atom molecular dynamics) techniques to investigate the capacity of four optically pure components of the natural product silymarin (silybin A, silybin B, 2,3-dehydrosilybin A, 2,3-dehydrosilybin B) to inhibit Aβ aggregation. Despite TEM analysis demonstrated that all the four investigated Flavonoids prevent the formation of mature fibrils, ThT assays, WB and AFM investigations showed that only silybin B was able to halt the growth of small-sized protofibrils thus promoting the formation of large, amorphous aggregates. Molecular dynamics (MD) simulations indicated that silybin B interacts mainly with the C-terminal hydrophobic segment 35MVGGVV40 of Aβ40. Consequently to silybin B binding, the peptide conformation remains predominantly unstructured along all the simulations. By contrast, silybin A interacts preferentially with the segments 17LVFF20 and 27NKGAII32 of Aβ40 which shows a high tendency to form bend, turn, and β-sheet conformation in and around these two domains. Both 2,3-dehydrosilybin enantiomers bind preferentially the segment 17LVFF20 but lead to the formation of different small-sized, ThT-positive Aβ aggregates. Finally, in vivo studies in a transgenic Caenorhabditis elegans strain expressing human Aβ indicated that silybin B is the most effective of the four compounds in counteracting Aβ proteotoxicity. This study underscores the pivotal role of stereochemistry in determining the neuroprotective potential of silybins and points to silybin B as a promising lead compound for further development in anti-AD therapeutics.

Keywords

Alzheimer’s disease; Chiral drugs; natural compounds; neurodegeneration; neuroprotection.

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