Novel Sulfonamide-Based Carbamates as Selective Inhibitors of BChE

Magar, Pratibha; Parravicini, Oscar; Štěpánková, Šárka; Svrčková, Katarína; Garro, Adriana; Jendrzejewska, Izabela; Pauk, Karel; Hošek, Jan; Jampílek, Josef; Enriz, Ricardo Daniel; Imramovský, Aleš

doi:10.3390/ijms22179447

Cited by 12 publications

(8 citation statements)

References 94 publications

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“…The selective index for BChE (SI (AChE/BChE) ) was 3.76 and 3.46 for MYR-PVP 1:8 w / w and 1:9 w / w respectively). The selectivity of MYR can be attributed to differences in the active sites of AChE and BChE enzymes [ 94 , 95 ]. BChE has a larger and more flexible active site compared to AChE, allowing for a wider range of interactions with inhibitors such as MYR.…”

Section: Resultsmentioning

confidence: 99%

Myricetin Amorphous Solid Dispersions—Antineurodegenerative Potential

Rosiak,

Tykarska,

Cielecka-Piontek

2024

Molecules

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Our research aimed to develop an amorphous solid dispersion (ASD) of myricetin (MYR) with Polyvinylpyrrolidone K30 (PVP30) to enhance its solubility, dissolution rate, antioxidant, and neuroprotective properties. Employing a combination of solvent evaporation and freeze drying, we successfully formed MYR ASDs. XRPD analysis confirmed complete amorphization in 1:8 and 1:9 MYR-PVP weight ratios. DSC thermograms exhibited a single glass transition (Tg), indicating full miscibility. FT-IR results and molecular modeling confirmed hydrogen bonds stabilizing MYR’s amorphous state. HPLC analysis indicated the absence of degradation products, ensuring safe MYR delivery systems. Solubility, dissolution rate (pH 1.2 and 6.8), antioxidant (ABTS, DPPH, CUPRAC, and FRAP assays), and in vitro neuroprotective activities (inhibition of cholinesterases: AChE and BChE) were significantly improved compared to the pure compound. Molecular docking studies revealed that MYR had made several hydrogen, hydrophobic, and π-π stacking interactions, which could explain the compound’s potency to inhibit AChE and BChE. MYR-PVP 1:9 w/w ASD has the best solubility, antioxidant, and neuroprotective activity. Stability studies confirmed the physical stability of MYR-PVP 1:9 w/w ASD immediately after dissolution and for two months under ambient conditions. Our study showed that the obtained ASDs are promising systems for the delivery of MYR with the potential for use in alleviating the symptoms of neurodegenerative diseases.

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Section: Resultsmentioning

confidence: 99%

Myricetin Amorphous Solid Dispersions—Antineurodegenerative Potential

Rosiak,

Tykarska,

Cielecka-Piontek

2024

Molecules

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“…(2021) performed 20 ns MD simulations of the uncleaved tcAChE-rivastigmine complex in triplicates using Amber16 software. Despite studying a different organism, Magar et al 82 also observed that rivastigmine is deeply buried inside the active-site gorge of AChE, interacting with the catalytic triad and nearby residues throughout the simulations. 82 Distinct interactions with rivastigmine were observed between the docking solution (Figure 3) and the representative structure of wild type hAChE (Figure 5).…”

Section: Molecular Dynamics Simulationmentioning

confidence: 99%

“…Despite studying a different organism, Magar et al 82 also observed that rivastigmine is deeply buried inside the active-site gorge of AChE, interacting with the catalytic triad and nearby residues throughout the simulations. 82 Distinct interactions with rivastigmine were observed between the docking solution (Figure 3) and the representative structure of wild type hAChE (Figure 5). This difference may occur since docking algorithms assign some approximations such as rigid receptors, which can affect final predictions.…”

Section: Molecular Dynamics Simulationmentioning

confidence: 99%

In silico analyses of acetylcholinesterase (AChE) and its genetic variants in interaction with the anti‐Alzheimer drug Rivastigmine

Pereira

Gonçalves

Abrahim-Vieira

et al. 2022

J of Cellular Biochemistry

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Alzheimer's disease (AD) is the leading cause of dementia worldwide. Despite causing great social and economic impact, there is currently no cure for AD. The most effective therapy to manage AD symptoms is based on acetylcholinesterase inhibitors (AChEi), from which rivastigmine presented numerous benefits. However, mutations in AChE, which affect approximately 5% of the population, can modify protein structure and function, changing the individual response to Alzheimer's treatment. In this study, we performed computer simulations of AChE wild type and variants R34Q, P135A, V333E, and H353N, identified by one or more genome‐wide association studies, to evaluate their effects on protein structure and interaction with rivastigmine. The functional effects of AChE variants were predicted using eight machine learning algorithms, while the evolutionary conservation of AChE residues was analyzed using the ConSurf server. Autodock4.2.6 was used to predict the binding modes for the hAChE–rivastigmine complex, which is still unknown. Molecular dynamics (MD) simulations were performed in triplicates for the AChE wild type and mutants using the GROMACS packages. Among the analyzed variants, P135A was classified as deleterious by all the functional prediction algorithms, in addition to occurring at highly conserved positions, which may have harmful consequences on protein function. The molecular docking results suggested that rivastigmine interacts with hAChE at the upper active‐site gorge, which was further confirmed by MD simulations. Our MD findings also suggested that the complex hAChE‐rivastigmine remains stable over time. The essential dynamics revealed flexibility alterations at the active‐site gorge upon mutations P135A, V333E, and H353N, which may lead to strong and nonintuitive consequences to hAChE binding. Nonetheless, similar binding affinities were registered in the MMPBSA analysis for the hAChE wild type and variants when complexed to rivastigmine. Finally, our findings indicated that the rivastigmine binding to hAChE is an energetically favorable process mainly driven by negatively charged amino acids.

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“…Our group has previously reported several studies using this approach for different types of L–R complexes from different biological systems. 24–29 Recently, we reported a study showing the possibilities and limitations of this approach. 30…”

Section: Introductionmentioning

confidence: 99%