Nanomarker for early detection of Alzheimer’s disease combining ab initio DFT simulations and molecular docking approach

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Abstract

The tau protein is considered an important qualitative and quantitative biomarker for Alzheimer’s disease in its asymptomatic phase. In 2011, biomarkers were suggested by the National Institute on Aging-Azheimer’s Association as a new criterion for the early diagnosis of Alzheimer’s disease. Thus, highlighting the non-existence of theoretical research on the subject, we investigated the binding interaction properties between phosphorylated tau protein and a theoretically modeled ligands constituted by the fullerol functionalized with radiopharmaceuticals from an in silico approach via molecular docking and density functional theory (DFT) ab initio computational simulation. The results demonstrated that the ligand with the greatest affinity-based binding energy to the protein was fullerol + F-THK5105. However, all systems were considered promising for the development of a potential diagnostic nanomarker. These theoretical results could efficiently contribute to reduce the time and the cost for future experimental preclinical studies and open new opportunities toward molecular recognition in nanomedicine

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Ferreira Schopf, P., Zanella, I., D. S. Cordeiro, M. N., Ruso, J. M., González-Durruthy, M., & Ortiz Martins, M. (2021). Nanomarker for Early Detection of Alzheimer’s Disease Combining Ab initio DFT Simulations and Molecular Docking Approach. Biophysica, 1(2), 76-86. https://doi.org/10.3390/biophysica1020007

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This research was funded by Institute of Carbon Nanomaterials-INCT/CNPq; Fapergs, CAPES, and UFN (Patricia Ferreira Schopf, Ivana Zanella da Silva, and Mirkos Ortiz Martins). In addition, research funding were provided by FCT/MCTES through national funds (Michael González-Durruthy, and M. Natália D.S. Cordeiro), grant UID/QUI/50006/2020, as well as by Xunta de Galicia (Juan M. Ruso), grant ED41E2018/08. The APC was funded by MDPI

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Attribution 4.0 International