Issue 36, 2023

The inhibitory effects of platinum(ii) complexes on amyloid aggregation: a theoretical and experimental approach

Abstract

Platinum (Pt)(II) square planar complexes are well-known anticancer drugs whose Mechanism of Action (MOA) are finely tuned by the polar, hydrophobic and aromatic features of the ligands. In the attempt to translate this tunability to the identification of potential neurodrugs, herein, four Pt(II) complexes were investigated in their ability to modulate the self-aggregation processes of two amyloidogenic models: Sup35p7–13 and NPM1264–277 peptides. In particular, phenanthriplatin revealed the most efficient agent in the modulation of amyloid aggregation: through several biophysical assays, as Thioflavin T (ThT), electrospray ionization mass spectrometry (ESI-MS) and ultraviolet-visible (UV-vis) absorption spectroscopy, this complex revealed able to markedly suppress aggregation and to disassemble small soluble aggregates. This effect was due to a direct coordination of phenanthriplatin to the amyloid, with the loss of several ligands and different stoichiometries, by the formation of π–π and π–cation interactions as indicated from molecular dynamic simulations. Presented data support a growing and recent approach concerning the repurposing of metallodrugs as potential novel neurotherapeutics.

Graphical abstract: The inhibitory effects of platinum(ii) complexes on amyloid aggregation: a theoretical and experimental approach

Supplementary files

Article information

Article type
Paper
Submitted
11 Jul 2023
Accepted
14 Aug 2023
First published
25 Aug 2023
This article is Open Access
Creative Commons BY-NC license

Dalton Trans., 2023,52, 12677-12685

The inhibitory effects of platinum(II) complexes on amyloid aggregation: a theoretical and experimental approach

S. La Manna, V. Roviello, V. Monaco, J. A. Platts, M. Monti, E. Gabano, M. Ravera and D. Marasco, Dalton Trans., 2023, 52, 12677 DOI: 10.1039/D3DT02187D

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