An insight to the molecular interactions of the FDA approved HIV PR drugs against L38L↑N↑L PR mutant

Sanusi, Zainab K.; Govender, Thavendran; Maguire, Glenn E. M.; Maseko, Sibusiso B.; Lin, Johnson; Kruger, Hendrik G.; Honarparvar, Bahareh

doi:10.1007/s10822-018-0099-9

Cited by 11 publications

(6 citation statements)

References 107 publications

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“…Further analyses included system stability estimation and ligand−enzyme interaction profiling. Previous literature 49,99,100 showed the hybrid B3LYP approach is sufficient with relative energies in good trend with experimental values. Therefore, we selected the B3LYP/6-31+G(d):AMBER ONIOM level to optimize the metal complexes, CYP3A4, and Cu complex−CYP3A4 systems.…”

Section: Synthesis Of Complex [Cu(l 1 ) 2 ] (1)supporting

confidence: 63%

Design of New Schiff-Base Copper(II) Complexes: Synthesis, Crystal Structures, DFT Study, and Binding Potency toward Cytochrome P450 3A4

et al. 2021

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We report the synthesis and crystal structures of three new copper(II) Schiff-base complexes. The complexes have been characterized by elemental analysis and Fourier transform infrared (FT-IR) and UV–visible spectroscopies. The X-ray diffraction (XRD) analysis reveals that complexes 1 and 3 crystallize in a monoclinic space group C2/c and 2 in a triclinic space group P1̅, each adopting a square planar geometry around the metal center. We use a density functional theory method to explore the quantum chemical properties of these complexes. The calculation proceeds with the three-dimensional (3D) crystal structure characterization of the complexes in which the calculated IR and UV–vis values are comparable to the experimental results. Charge distribution and molecular orbital analyses enabled quantum chemical property prediction of these complexes. We study the drug-likeness properties and binding potentials of the synthesized complexes. The in silico outcome showed that they could serve as permeability-glycoprotein (P-gp) and different cytochrome P450 substrates. Our calculations showed that the complexes significantly bind to cytochrome P450 3A4.

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Section: Synthesis Of Complex [Cu(l 1 ) 2 ] (1)supporting

confidence: 63%

Design of New Schiff-Base Copper(II) Complexes: Synthesis, Crystal Structures, DFT Study, and Binding Potency toward Cytochrome P450 3A4

et al. 2021

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“…In all cases, fine details of side-chain interactions were detected on the atomic level, which could improve the efficacy of the corresponding modified compound. In a comprehensive investigation of nine U.S. Food and Drug Administration (FDA) approved drugs, the causes for the reduced binding of most of them to the South African C subtype (C-SA) were revealed in atomic detail [45]. Some HIV protease inhibitors only gained academic interest, e.g., the metallacarborane complexes, exhibiting two cage-like C 2 B 9 H 11 coordinated by a Co 2+ center [46,47].…”

Section: Mechanisms Of Aspartic Proteasesmentioning

confidence: 99%

Mechanisms of Proteolytic Enzymes and Their Inhibition in QM/MM Studies

Elsässer

Goettig

2021

IJMS

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Experimental evidence for enzymatic mechanisms is often scarce, and in many cases inadvertently biased by the employed methods. Thus, apparently contradictory model mechanisms can result in decade long discussions about the correct interpretation of data and the true theory behind it. However, often such opposing views turn out to be special cases of a more comprehensive and superior concept. Molecular dynamics (MD) and the more advanced molecular mechanical and quantum mechanical approach (QM/MM) provide a relatively consistent framework to treat enzymatic mechanisms, in particular, the activity of proteolytic enzymes. In line with this, computational chemistry based on experimental structures came up with studies on all major protease classes in recent years; examples of aspartic, metallo-, cysteine, serine, and threonine protease mechanisms are well founded on corresponding standards. In addition, experimental evidence from enzyme kinetics, structural research, and various other methods supports the described calculated mechanisms. One step beyond is the application of this information to the design of new and powerful inhibitors of disease-related enzymes, such as the HIV protease. In this overview, a few examples demonstrate the high potential of the QM/MM approach for sophisticated pharmaceutical compound design and supporting functions in the analysis of biomolecular structures.

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“…Therefore, the development of TYR inhibitors with efficient bioactivity and less toxicity is a relevant branch of scientific research. Recently, we have used molecular modeling approaches to investigate biomolecular systems with an emphasis on enzymatic reactions and inhibition [ 27 , 28 , 29 , 30 , 31 , 32 , 33 , 34 , 35 , 36 , 37 , 38 , 39 ].…”

Section: Introductionmentioning

confidence: 99%

Evaluating the Performance of a Non-Bonded Cu2+ Model Including Jahn−Teller Effect into the Binding of Tyrosinase Inhibitors

Martins

Lameira

Kruger

et al. 2020

IJMS

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Tyrosinase (TYR) is a metalloenzyme classified as a type-3 copper protein, which is involved in the synthesis of melanin through a catalytic process beginning with the conversion of the amino acid l-Tyrosine (l-Tyr) to l-3,4-dihydroxyphenylalanine (l-DOPA). It plays an important role in the mechanism of melanogenesis in various organisms including mammals, plants, and fungi. Herein, we used a combination of computational molecular modeling techniques including molecular dynamic (MD) simulations and the linear interaction energy (LIE) model to evaluate the binding free energy of a set of analogs of kojic acid (KA) in complex with TYR. For the MD simulations, we used a dummy model including the description of the Jahn–Teller effect for Cu2+ ions in the active site of this enzyme. Our results show that the LIE model predicts the TYR binding affinities of the inhibitor in close agreement to experimental results. Overall, we demonstrate that the classical model provides a suitable description of the main interactions between analogs of KA and Cu2+ ions in the active site of TYR.

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An insight to the molecular interactions of the FDA approved HIV PR drugs against L38L↑N↑L PR mutant

Cited by 11 publications

References 107 publications

Design of New Schiff-Base Copper(II) Complexes: Synthesis, Crystal Structures, DFT Study, and Binding Potency toward Cytochrome P450 3A4

Design of New Schiff-Base Copper(II) Complexes: Synthesis, Crystal Structures, DFT Study, and Binding Potency toward Cytochrome P450 3A4

Mechanisms of Proteolytic Enzymes and Their Inhibition in QM/MM Studies

Evaluating the Performance of a Non-Bonded Cu2+ Model Including Jahn−Teller Effect into the Binding of Tyrosinase Inhibitors

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