Investigations of Albumin–Insulin Detemir Complexes Using Molecular Dynamics Simulations and Free Energy Calculations

Ryberg, Line Abildgaard; Sønderby, Pernille; Bukrinski, Jens Thostrup; Harris, Pernille; Peters, Günther H.J.

doi:10.1021/acs.molpharmaceut.9b00839

Cited by 8 publications

(2 citation statements)

References 106 publications

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“…Therapeutics have been explored through liver fructose 1,6-bisphosphate inhibitors to control gluconeogenesis-mediated overproduction of glucose ( Proenca et al, 2020 ) and dipeptidyl peptidase 4 inhibitors to block degradation of incretins that stimulate decrease of blood glucose ( Rahman et al, 2020 ). Half-life extension of insulin determir by complex formation with human serum albumin has been examined as a platform for drug delivery ( Ryberg et al, 2020 ). Further studies assess the role of conformational changes in AcrB transporter contributing to multidrug resistance ( Matsunaga et al, 2018 ), transport of cholesterol by the Aster-A protein ( Moesgaard et al, 2020 ), and reduction of chronic inflammation by treatment with the peptide KCF18 binding to TNF-α and interleukin-6 ( Jiang et al, 2019 ).…”

Section: Applications To Drug Discoverymentioning

confidence: 99%

Recent Developments in Free Energy Calculations for Drug Discovery

King

Aitchison

et al. 2021

Front. Mol. Biosci.

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The grand challenge in structure-based drug design is achieving accurate prediction of binding free energies. Molecular dynamics (MD) simulations enable modeling of conformational changes critical to the binding process, leading to calculation of thermodynamic quantities involved in estimation of binding affinities. With recent advancements in computing capability and predictive accuracy, MD based virtual screening has progressed from the domain of theoretical attempts to real application in drug development. Approaches including the Molecular Mechanics Poisson Boltzmann Surface Area (MM-PBSA), Linear Interaction Energy (LIE), and alchemical methods have been broadly applied to model molecular recognition for drug discovery and lead optimization. Here we review the varied methodology of these approaches, developments enhancing simulation efficiency and reliability, remaining challenges hindering predictive performance, and applications to problems in the fields of medicine and biochemistry.

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Section: Applications To Drug Discoverymentioning

confidence: 99%

Recent Developments in Free Energy Calculations for Drug Discovery

King

Aitchison

et al. 2021

Front. Mol. Biosci.

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“…Additionally, the free energy of solvation ΔG sol can be calculated as the sum of the electrostatic component (ΔG ele, sol ) and the non-polar component (ΔG nonpolar, sol ), as shown in equation 13 [50,51] :…”

Section: Analysis Of the Structure By Ultraviolet-visible Spectroscopymentioning

confidence: 99%

Exploring the toxic effects and mechanism of methoxylated polybrominated diphenyl ethers (MeO‐PBDEs) on thyroxine‐binding globulin (TBG): Synergy between spectroscopic and computations

Huang

Zuo

et al. 2021

Luminescence

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The interaction mechanism between thyroxine-binding globulin (TBG) and three methoxylated polybrominated diphenyl ethers (MeO-PBDEs) was analyzed by steady-state fluorescence, ultraviolet-visible (UV-visible) spectroscopy, circular dichroism (CD), molecular docking and molecular dynamics simulation methods. The results of the molecular docking technique revealed that 2 0 -MeO-BDE-3, 5-MeO-BDE-47, and 3-MeO-BDE-100 combined with TBG at the active site. The steady-state fluorescence spectra displayed that MeO-PBDEs quenched the endogenous fluorescence of TBG through static quenching mechanism, and complex formation between MeO-PBDEs and TBG was further indicated by UV-vis spectroscopy. The thermodynamic quantities showed that the binding process is spontaneous, and the major forces responsible for the binding are hydrogen bonding and hydrophobic interactions, which are consistent with the results of molecular docking to a certain extent. The results of CD confirmed that the secondary structure of TBG was changed after combining with MeO-PBDEs. The dynamic simulation results illustrated that the protein structure is more compact and changes in the secondary structure of TBG after binding to MeO-PBDEs. Additionally, we also utilized the molecular mechanics/Poisson-Boltzmann surface area (MM-PBSA) method to analyze the binding free energy of TBG and MeO-PBDEs. The results suggest that van der Waals force plays an essential role in the combination.

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