Issue 3, 2025

From experimental studies to computational approaches: recent trends in designing novel therapeutics for amyloidogenesis

Abstract

Amyloidosis is a condition marked by misfolded proteins that build up in tissues and eventually destroy organs. It has been connected to a number of fatal illnesses, including non-neuropathic and neurodegenerative conditions, which in turn have a significant influence on the worldwide health sector. The inability to identify the underlying etiology of amyloidosis has hampered efforts to find a treatment for the condition. Despite the identification of a multitude of putative pathogenic variables that may operate independently or in combination, the molecular mechanisms responsible for the development and progression of the disease remain unclear. A thorough investigation into protein aggregation and the impacts of toxic aggregated species will help to clarify the cytotoxicity of aggregation-mediated cellular apoptosis and lay the groundwork for future studies aimed at creating effective treatments and medications. This review article provides a thorough summary of the combination of various experimental and computational approaches to modulate amyloid aggregation. Further, an overview of the latest developments of novel therapeutic agents is given, along with a discussion of the possible obstacles and viewpoints on this developing field. We believe that the information provided by this review will help scientists create innovative treatment strategies that affect the way proteins aggregate.

Graphical abstract: From experimental studies to computational approaches: recent trends in designing novel therapeutics for amyloidogenesis

Article information

Article type
Review Article
Submitted
22 Aug 2024
Accepted
01 Dec 2024
First published
12 Dec 2024

J. Mater. Chem. B, 2025,13, 858-881

From experimental studies to computational approaches: recent trends in designing novel therapeutics for amyloidogenesis

P. Ghosh, A. Kundu and D. Ganguly, J. Mater. Chem. B, 2025, 13, 858 DOI: 10.1039/D4TB01890G

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