Development of an in-vivo active reversible butyrylcholinesterase inhibitor

Košak, Urban; Brus, Boris; Knez, Damijan; Šink, Roman; Žakelj, Simon; Trontelj, Jurij; Pišlar, Anja; Šlenc, Jasna; Gobec, Martina; Živin, Marko; Tratnjek, Larisa; Perše, Martina; Sałat, Kinga; Podkowa, Adrian; Filipek, Barbara; Nachon, Florian; Brazzolotto, Xavier; Więckowska, Anna; Malawska, Barbara; Stojan, Jure; Mlinarič-Raščan, Irena; Kos, Janko; Coquelle, Nicolas; Colletier, J.P.; Gobec, Stanislav

doi:10.1038/srep39495

Cited by 118 publications

(103 citation statements)

References 64 publications

(87 reference statements)

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“…The binding mode of inhibitor 3 is somewhat different compared to that of inhibitors 1 and 2 [15][16][17] . The common property of all of these three types of inhibitors is the position of the naphthalene Figure 1.…”

Section: Structure-activity Relationshipsmentioning

confidence: 89%

“…The naphthalene-sulphonamide derivatives 3A and 3B have similar binding modes, where the naphthalene moiety points towards the acyl-binding pocket (Figures 4(B), 5(B)). The piperidine moiety is inverted compared to the naphthalene carboxamide of 2C (5NN0), although it retains the same orientation as in the parent sulphonamide (5DYW) 16 (Figure 5(B)), where the benzyl ring protrudes into a highly hydrophobic pocket that is formed by residues Phe73, Trp82, Tyr332, Trp430, and Tyr440. As seen for the complex structure of parent inhibitor 3 with BChE, the sulphonamide oxygens of 3A and 3B form H-bonds with the hydroxyl group of Thr120.…”

Section: Crystal Structure Of Hubche In Complex With Probes 2c 3a Amentioning

confidence: 99%

“…Inhibition of BChE in rat brain slices was therefore examined for probes 2C and 3B, to evaluate these two probes under more biologically relevant conditions. Sections of rat brain with the highest BChE activity were selected and the modified Koelle À Karnovsky histochemical method was used to detect BChE activity 16,[40][41][42] . For these probes 2C and 3B, 1 mM was needed to achieve substantial inhibition of BChE, as measured by less formation of the dark-brown/black granular BChE reaction product (Figure 8).…”

Section: Rat Brain Slicesmentioning

confidence: 99%

“…In the present study, we report on the two BChE-specific fluorescent probes that were derived from previously described highly potent and reversible BChE-selective inhibitors [15][16][17] . Although the incorporation of the fluorophore moieties had a negative impact on their BChE inhibition potency, the best three of these fluorescent inhibitors retained excellent activities in the low nanomolar range: probes 2A, 3A, and 3B.…”

Section: Introductionmentioning

confidence: 99%

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Development of potent reversible selective inhibitors of butyrylcholinesterase as fluorescent probes

Pajk

Knez

Košak

et al. 2020

Journal of Enzyme Inhibition and Medicinal Chemistry

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Brain butyrylcholinesterase (BChE) is an attractive target for drugs designed for the treatment of Alzheimer's disease (AD) in its advanced stages. It also potentially represents a biomarker for progression of this disease. Based on the crystal structure of previously described highly potent, reversible, and selective BChE inhibitors, we have developed the fluorescent probes that are selective towards human BChE. The most promising probes also maintain their inhibition of BChE in the low nanomolar range with high selectivity over acetylcholinesterase. Kinetic studies of probes reveal a reversible mixed inhibition mechanism, with binding of these fluorescent probes to both the free and acylated enzyme. Probes show environment-sensitive emission, and additionally, one of them also shows significant enhancement of fluorescence intensity upon binding to the active site of BChE. Finally, the crystal structures of probes in complex with human BChE are reported, which offer an excellent base for further development of this library of compounds.

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Section: Structure-activity Relationshipsmentioning

confidence: 89%

Section: Crystal Structure Of Hubche In Complex With Probes 2c 3a Amentioning

confidence: 99%

Section: Rat Brain Slicesmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Development of potent reversible selective inhibitors of butyrylcholinesterase as fluorescent probes

Pajk

Knez

Košak

et al. 2020

Journal of Enzyme Inhibition and Medicinal Chemistry

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“…However, the sulfonamide moiety has also been incorporated to known biologically relevant backbones to generate novel biological activity [ 3 ]. For instance, new anti-AD (Alzheimer’s disease) agents with inhibitory properties towards butyrylcholinestarase (BChE) have been synthesized by incorporation of sulfonamide moiety to earlier hit compounds [ 14 ]. These results suggest that sulfonamide-based compounds exert multi-directional biological activity.…”

Section: Introductionmentioning

confidence: 99%

Novel Sulfonamide-Based Analogs of Metformin Exert Promising Anti-Coagulant Effects without Compromising Glucose-Lowering Activity

et al. 2020

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Metformin, one of the most frequently prescribed oral anti-diabetic drugs, is characterized by multidirectional activity, including lipid lowering, cardio-protective and anti-inflammatory properties. This study presents synthesis and stability studies of 10 novel sulfonamide-based derivatives of metformin with alkyl substituents in the aromatic ring. The potential of the synthesized compounds as glucose-lowering agents and their effects on selected parameters of plasma and vascular hemostasis were examined. Compounds with two or three methyl groups in the aromatic ring (6, 7, 9, 10) significantly increased glucose uptake in human umbilical vein endothelial cells (HUVECs), e.g., 15.8 µmol/L for comp. 6 at 0.3 µmol/mL versus 11.4 ± 0.7 µmol/L for control. Basic coagulation studies showed that all examined compounds inhibit intrinsic coagulation pathway and the process of fibrin polymerization stronger than the parent drug, metformin, which give evidence of their greater anti-coagulant properties. Importantly, synthesized compounds decrease the activity of factor X, a first member of common coagulation pathway, while metformin does not affect coagulation factor X (FX) activity. A multiparametric clot formation and lysis test (CL-test) revealed that the examined compounds significantly prolong the onset of clot formation; however, they do not affect the overall potential of clot formation and fibrinolysis. Erythrotoxicity studies confirmed that none of the synthesized compounds exert an adverse effect on erythrocyte integrity, do not contribute to the massive hemolysis and do not interact strongly with the erythrocyte membrane. In summary, chemical modification of metformin scaffold into benzenesulfonamides containing alkyl substituents leads to the formation of potential dual-action agents with comparable glucose-lowering properties and stronger anti-coagulant activity than the parent drug, metformin.

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Conjugates of amiridine and thiouracil derivatives as effective inhibitors of butyrylcholinesterase with the potential to block β‐amyloid aggregation

Khudina,

Grishchenko,

Makhaeva

et al. 2023

Archiv der Pharmazie

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New amiridine‐thiouracil conjugates with different substituents in the pyrimidine fragment (R = CH3, CF2Н, CF3, (CF2)2H) and different spacer lengths (n = 1–3) were synthesized. The conjugates rather weakly inhibit acetylcholinesterase (AChE) and exhibit high inhibitory activity (IC50 up to 0.752 ± 0.021 µM) and selectivity to butyrylcholinesterase (BChE), which increases with spacer elongation; the lead compounds are 11c, 12c, and 13c. The conjugates are mixed‐type reversible inhibitors of both cholinesterases and practically do not inhibit the structurally related off‐target enzyme carboxylesterase. The results of molecular docking to AChE and BChE are consistent with the experiment on enzyme inhibition and explain the structure–activity relationships, including the rather low anti‐AChE activity and the high anti‐BChE activity of long‐chain conjugates. The lead compounds displace propidium from the AChE peripheral anion site (PAS) at the level of the reference compound donepezil, which agrees with the mixed‐type mechanism of AChE inhibition and the main mode of binding of conjugates in the active site of AChE due to the interaction of the pyrimidine moiety with the PAS. This indicates the ability of the studied conjugates to block AChE‐induced aggregation of β‐amyloid, thereby exerting a disease‐modifying effect. According to computer calculations, all synthesized conjugates have an ADME profile acceptable for drugs.

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Development of an in-vivo active reversible butyrylcholinesterase inhibitor

Cited by 118 publications

References 64 publications

Development of potent reversible selective inhibitors of butyrylcholinesterase as fluorescent probes

Development of potent reversible selective inhibitors of butyrylcholinesterase as fluorescent probes

Novel Sulfonamide-Based Analogs of Metformin Exert Promising Anti-Coagulant Effects without Compromising Glucose-Lowering Activity

Conjugates of amiridine and thiouracil derivatives as effective inhibitors of butyrylcholinesterase with the potential to block β‐amyloid aggregation

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