Beneficent and Maleficent Effects of Cations on Bufadienolide Binding to Na<sup>+</sup>,K<sup>+</sup>-ATPase

Ladefoged, Lucy Kate; Schiøtt, Birgit; Fedosova, Natalya U.

doi:10.1021/acs.jcim.0c01396

Cited by 3 publications

(2 citation statements)

References 37 publications

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“…Taking the high cardiotropic effects of bufadienolides [21,22,23] into consideration, we studied their effects on general toxicology with the purpose of possible implementation into medical practice as a cardiotropic drug. Therefore, our upcoming experiments were dedicated to investigating the influence on some biochemical parameters such as total protein, alanine aminotransferase, aspartate aminotransferase, cholesterol, glucose, and urea in the blood of rabbits.…”

Section: Blood Biochemical Parametersmentioning

confidence: 99%

Effects of Bufadienolides from Bufo viridis Toad Venom on Blood Biochemical Compositions and Thromboelastographic Parameters

MIRAKHMETOVA,

VYPOVA,

ASROROV

et al. 2023

jrp

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Bufadienolides, cyclopentanophenantrene derivatives that possess similar structures to cardiac glycosides, have been established to reveal cytotoxicity. Their higher concentrations as anticancer means are expected to affect the normal function of the heart, liver, and kidney. In this work, we established the mass ratio of bufadienolides isolated from the venom of Bufo viridis. Arenobufagin, gamabufotalin, telocinobufagin, and marinobufagin were found as the major compounds in the sum. Their effects on biological parameters, used as indicators of the normal functioning of organs, were determined in rabbits. The blood samples, taken on the 10 th and 30 th days following the drug administration, showed these paramaters reaching the control levels for 30 days in all studied doses: 0.15, 0.45, and 0.6 mg/kg. The 0.15 and 0.6 mg/kg doses were established not to cause significant changes in the activities of alanine aminotransferase and aspartate aminotransferase, and the quantities of cholesterol and fasting blood sugar in blood samples. Significant changes were found in quantities of glucose (a reduction) and urea (an increase) on the 10 th day of the administration. But their levels reached the control level for the next 20 days. We observed significant differences in thromboelastographic parameters in mice on the 10 th day after the drug administration in a 0.15 mg/kg dose. In mice, LD50 levels of intravenous, subcutaneous, and oral administrations made 14.5, 110, and 215 mg/kg, respectively. These results enable the suggestion of optimum concentration that does not cause severe damage to the functions of organs.

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Section: Blood Biochemical Parametersmentioning

confidence: 99%

Effects of Bufadienolides from Bufo viridis Toad Venom on Blood Biochemical Compositions and Thromboelastographic Parameters

MIRAKHMETOVA,

VYPOVA,

ASROROV

et al. 2023

jrp

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“…The Drude polarizable FF has been parametrized in conjunction with SWM4-NDP water for atomic and molecular ions. , Ion LJ parameters were tuned to reproduce QM ion–water interaction energy and experimental hydration free energy (HFE). The AMOEBA polarizable FF for atomic ions has also been developed by using a similar approach. , These ion models have been used to study a variety of biological problems, such as ion permeation in membrane channels, ATPases, and ion selectivity in proteins…”

Section: Introductionmentioning

confidence: 99%

Advanced Electrostatic Model for Monovalent Ions Based on Ab Initio Energy Decomposition

Jing

Liu

Ren

2021

J. Chem. Inf. Model.

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Ions play important roles in the structures and functions of biomolecules. In biomolecular simulations, ions either directly interact with biomolecules or provide an ionic environment that influences electrostatic interactions of solutes. The AMOEBA+ water model has demonstrated significant advancement of the classical force field for describing molecular interactions due to its improvements on the functional forms to account for essential physics. This work expands the applicability of the AMOEBA+ model toward alkali metal (Li, Na, K, Rb, and Cs) and halogen (F, Cl, Br, and I) ions. Various quantum chemical data on ion–ion and ion–water interactions, experimental ion hydration free energies, and lattice energies of salt crystals are used in the parametrization. The final parameters are verified with other properties outside of the parametrization data, including lattice energies of additional salt crystals and ionic activity coefficients in solution. The new model captures a wide range of ion properties from the gas phase to solution phase and crystals. More importantly, AMOEBA+ provides energy components that are consistent with ab initio energy decomposition. Thus, we expect AMOEBA+ to be more general, transferable, and valuable for the interpretation of intermolecular forces in efficient classical simulations.

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Geometry and water accessibility of the inhibitor binding site of Na+-pump: Pulse- and CW-EPR study

Aloi

Guo

Guzzi

et al. 2021

Biophysical Journal

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Spin labels based on cinobufagin, a specific inhibitor of the Na,K-ATPase, have proved valuable tools to characterize the binding site of cardiotonic steroids (CTSs), which also constitutes the extracellular cation pathway. Because existing literature suggests variations in the physiological responses caused by binding of different CTSs, we extended the original set of spin-labeled inhibitors to the more potent bufalin derivatives. Positioning of the spin labels within the Na,K-ATPase site was defined and visualized by molecular docking. Although the original cinobufagin labels exhibited lower affinity, continuouswave electron paramagnetic resonance spectra of spin-labeled bufalins and cinobufagins revealed a high degree of pairwise similarity, implying that these two types of CTS bind in the same way. Further analysis of the spectral lineshapes of bound spin labels was performed with emphasis on their structure (PROXYL vs. TEMPO), as well as length and rigidity of the linkers. For comparable structures, the dynamic flexibility increased in parallel with linker length, with the longest linker placing the spin label at the entrance to the binding site. Temperature-related changes in spectral lineshapes indicate that six-membered nitroxide rings undergo boat-chair transitions, showing that the binding-site cross section can accommodate the accompanying changes in methyl-group orientation. D 2 O-electron spin echo envelope modulation in pulse-electron paramagnetic resonance measurements revealed high water accessibilities and similar polarity profiles for all bound spin labels, implying that the vestibule leading to steroid-binding site and cation-binding sites is relatively wide and water-filled.

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Beneficent and Maleficent Effects of Cations on Bufadienolide Binding to Na⁺,K⁺-ATPase

Cited by 3 publications

References 37 publications

Effects of Bufadienolides from Bufo viridis Toad Venom on Blood Biochemical Compositions and Thromboelastographic Parameters

Effects of Bufadienolides from Bufo viridis Toad Venom on Blood Biochemical Compositions and Thromboelastographic Parameters

Advanced Electrostatic Model for Monovalent Ions Based on Ab Initio Energy Decomposition

Geometry and water accessibility of the inhibitor binding site of Na+-pump: Pulse- and CW-EPR study

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Beneficent and Maleficent Effects of Cations on Bufadienolide Binding to Na+,K+-ATPase

Cited by 3 publications

References 37 publications

Effects of Bufadienolides from Bufo viridis Toad Venom on Blood Biochemical Compositions and Thromboelastographic Parameters

Effects of Bufadienolides from Bufo viridis Toad Venom on Blood Biochemical Compositions and Thromboelastographic Parameters

Advanced Electrostatic Model for Monovalent Ions Based on Ab Initio Energy Decomposition

Geometry and water accessibility of the inhibitor binding site of Na+-pump: Pulse- and CW-EPR study

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Beneficent and Maleficent Effects of Cations on Bufadienolide Binding to Na⁺,K⁺-ATPase