Investigating the Impact of First-Line Anti-Tuberculosis Drugs Encapsulated in a Eugenol-Based Nanoemulsion on Human Serum Albumin

Parvathy Mohan Menon; Natarajan Chandrasekaran; George Priya Doss C

doi:10.24976/Discov.Med.202436183.70

Investigating the Impact of First-Line Anti-Tuberculosis Drugs Encapsulated in a Eugenol-Based Nanoemulsion on Human Serum Albumin

Discov Med. 2024 Apr;36(183):739-752. doi: 10.24976/Discov.Med.202436183.70.

Authors

Parvathy Mohan Menon¹, Natarajan Chandrasekaran², George Priya Doss C¹

Affiliations

¹ Department of Integrative Biology, School of Bioscience and Technology, Vellore Institute of Technology, 632014 Vellore, India.
² Centre for Nanobiotechnology, Vellore Institute of Technology, 632014 Vellore, India.

PMID: 38665023
DOI: 10.24976/Discov.Med.202436183.70

Abstract

Background: Eugenol exhibits broad-spectrum antibacterial and anti-inflammatory properties. However, cytotoxicity at high concentrations limits the full utilization of eugenol-based drug complexes. Formulations of multidrug-loaded eugenol-based nanoemulsions have reduced cytotoxicity; however, it remains crucial to understand how these eugenol complexes interact with primary human carrier proteins to design and develop therapeutic alternatives. Consequently, this study primarily aims to investigate the impact on Human Serum Albumin (HSA) when it interacts with eugenol-based complexes loaded with first-line anti-tuberculosis drugs.

Methods: This study used various spectroscopic such as UV-visible spectroscopy, Fluorescence spectroscopy, Fourier-transform infrared spectroscopy and computational methods such as molecular docking and 100 ns molecular simulation to understand the impact of eugenol-based first-line anti-tuberculosis drug-loaded nanoemulsions on HSA structure.

Results: The binding of the HSA protein and eugenol-based complexes was studied using UV-visible spectroscopic analysis. Minor changes in the fluorophores of the protein further confirmed binding upon interaction with the complexes. The Fourier-transform infrared spectra showed no significant changes in protein structure upon interaction with eugenol-based multidrug-loaded nanoemulsions, suggesting that this complex is safe for internal administration. Unlike eugenol or first-line anti-tuberculosis alone, molecular docking revealed the strength of the binding interactions between the complexes and the protein through hydrogen bonds. The docked complexes were subjected to a 100 ns molecular dynamics simulation, which strongly supported the conclusion that the structure and stability of the protein were not compromised by the interaction.

Conclusions: From the results we could comprehend that the eugenol (EUG)-drug complex showed greater stability in HSA protein structure when compared to HSA interacting with isoniazid (INH), rifampicin (RIF), pyrazinamide (PYR), or ethambutol (ETH) alone or with EUG alone. Thus, inferring the potential of EUG-based drug-loaded formulations for a safer and efficient therapeutic use.

Keywords: HSA; eugenol; first-line anti-TB drugs; in-silico technique; nanoemulsions; spectroscopic technique.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Antitubercular Agents* / chemistry
Antitubercular Agents* / pharmacokinetics
Antitubercular Agents* / pharmacology
Emulsions* / chemistry
Eugenol* / chemistry
Eugenol* / pharmacology
Humans
Molecular Docking Simulation*
Protein Binding
Serum Albumin, Human* / chemistry
Serum Albumin, Human* / metabolism
Spectroscopy, Fourier Transform Infrared

Substances

Eugenol
Antitubercular Agents
Serum Albumin, Human
Emulsions