Your search keyword '"Nicotinic Antagonists classification"' showing total 7 results

1. Scorpion toxins interact with nicotinic acetylcholine receptors.

Author

Kasheverov IE, Oparin PB, Zhmak MN, Egorova NS, Ivanov IA, Gigolaev AM, Nekrasova OV, Serebryakova MV, Kudryavtsev DS, Prokopev NA, Hoang AN, Tsetlin VI, Vassilevski AA, and Utkin YN

Subjects

Animals, Mice, Nicotinic Antagonists chemistry, Nicotinic Antagonists classification, Protein Binding, Receptors, Nicotinic chemistry, Scorpion Venoms chemistry, Scorpion Venoms classification, Xenopus, Nicotinic Antagonists pharmacology, Receptors, Nicotinic metabolism, Scorpion Venoms pharmacology

Abstract

Neurotoxins are among the main components of scorpion and snake venoms. Scorpion neurotoxins affect voltage-gated ion channels, while most snake neurotoxins target ligand-gated ion channels, mainly nicotinic acetylcholine receptors (nAChRs). We report that scorpion venoms inhibit α-bungarotoxin binding to both muscle-type nAChR from Torpedo californica and neuronal human α7 nAChR. Toxins inhibiting nAChRs were identified as OSK-1 (α-KTx family) from Orthochirus scrobiculosus and HelaTx1 (κ-KTx family) from Heterometrus laoticus, both being blockers of voltage-gated potassium channels. With an IC 50 of 1.6 μm, OSK1 inhibits acetylcholine-induced current through mouse muscle-type nAChR heterologously expressed in Xenopus oocytes. Other well-characterized scorpion toxins from these families also bind to Torpedo nAChR with micromolar affinities. Our results indicate that scorpion neurotoxins present target promiscuity., (© 2019 Federation of European Biochemical Societies.)

Published

2019

2. Novel alpha D-conopeptides and their precursors identified by cDNA cloning define the D-conotoxin superfamily.

Author

Loughnan ML, Nicke A, Lawrence N, and Lewis RJ

Subjects

Amino Acid Sequence, Animals, Base Sequence, Cloning, Molecular, Conotoxins classification, Conotoxins isolation & purification, Conus Snail physiology, Molecular Sequence Data, Neural Inhibition physiology, Neurons chemistry, Neurons metabolism, Neurotoxins classification, Neurotoxins pharmacology, Nicotinic Antagonists classification, Peptide Fragments classification, Peptide Fragments physiology, Protein Precursors classification, Protein Precursors physiology, Rats, Receptors, Nicotinic biosynthesis, Receptors, Nicotinic metabolism, alpha7 Nicotinic Acetylcholine Receptor, Conotoxins genetics, Conus Snail genetics, DNA, Complementary isolation & purification, Multigene Family, Neurotoxins genetics, Nicotinic Antagonists isolation & purification, Peptide Fragments genetics, Protein Precursors genetics

Abstract

AlphaD-conotoxins are peptide inhibitors of nicotinic acetylcholine receptors (nAChRs) first described from Conus vexillum (alphaD-VxXIIA-C and renamed here to alphaD-VxXXA, alphaD-VxXXB, and alphaD-VxXXC). In this study, we report cDNA sequences encoding D-superfamily conopeptides identified in the Clade XII Conidae Conus vexillum, Conus capitaneus, Conus mustelinus, and Conus miles, together with partial sequences of corresponding peptides from this family. The D-superfamily signal peptide sequences display greater heterogeneity than reported for other conotoxin superfamilies. Phylogenetic analysis of the relationships among alphaD-conotoxin precursors reveals two distinct groups containing either an EMM or AVV signal peptide sequence motif. Homodimer and heterodimer combinations of predicted mature toxin sequences likely account for the partial amino acid sequences and mass values observed for several of the native dimeric peptide components identified in C. capitaneus, C. miles, and C. mustelinus venom. The discovery of the precursors and several novel conotoxins from different species defines this large conotoxin family and expands our understanding of sequence diversification mechanisms in Conus species.

Published

2009

3. QSAR modeling of mono- and bis-quaternary ammonium salts that act as antagonists at neuronal nicotinic acetylcholine receptors mediating dopamine release.

Author

Zheng F, Bayram E, Sumithran SP, Ayers JT, Zhan CG, Schmitt JD, Dwoskin LP, and Crooks PA

Subjects

Inhibitory Concentration 50, Models, Biological, Molecular Structure, Neural Networks, Computer, Nicotinic Antagonists chemistry, Nicotinic Antagonists classification, Quantitative Structure-Activity Relationship, Dopamine metabolism, Neurons drug effects, Neurons metabolism, Nicotinic Antagonists chemical synthesis, Nicotinic Antagonists pharmacology, Quaternary Ammonium Compounds chemistry, Receptors, Nicotinic metabolism

Abstract

Back-propagation artificial neural networks (ANNs) were trained on a dataset of 42 molecules with quantitative IC50 values to model structure-activity relationships of mono- and bis-quaternary ammonium salts as antagonists at neuronal nicotinic acetylcholine receptors (nAChR) mediating nicotine-evoked dopamine release. The ANN QSAR models produced a reasonable level of correlation between experimental and calculated log(1/IC50) (r2=0.76, r(cv)2=0.64). An external test for the models was performed on a dataset of 18 molecules with IC50 values >1 microM. Fourteen of these were correctly classified. Classification ability of various models, including self-organizing maps (SOM), for all 60 molecules was also evaluated. A detailed analysis of the modeling results revealed the following relative contributions of the used descriptors to the trained ANN QSAR model: approximately 44.0% from the length of the N-alkyl chain attached to the quaternary ammonium head group, approximately 20.0% from Moriguchi octanol-water partition coefficient of the molecule, approximately 13.0% from molecular surface area, approximately 12.6% from the first component shape directional WHIM index/unweighted, approximately 7.8% from Ghose-Crippen molar refractivity, and 2.6% from the lowest unoccupied molecular orbital energy. The ANN QSAR models were also evaluated using a set of 13 newly synthesized compounds (11 biologically active antagonists and two biologically inactive compounds) whose structures had not been previously utilized in the training set. Twelve among 13 compounds were predicted to be active which further supports the robustness of the trained models. Other insights from modeling include a structural modification in the bis-quinolinium series that involved replacing the 5 and/or 8 as well as the 5' and/or 8' carbon atoms with nitrogen atoms, predicting inactive compounds. Such data can be effectively used to reduce synthetic and in vitro screening activities by eliminating compounds of predicted low activity from the pool of candidate molecules for synthesis. The application of the ANN QSAR model has led to the successful discovery of six new compounds in this study with experimental IC50 values of less than 0.1 microM at nAChR subtypes responsible for mediating nicotine-evoked dopamine release, demonstrating that the ANN QSAR model is a valuable aid to drug discovery.

Published

2006

4. N-n-alkylnicotinium analogs, a novel class of nicotinic receptor antagonist: inhibition of S(-)-nicotine-evoked [(3)H]dopamine overflow from superfused rat striatal slices.

Author

Wilkins LH Jr, Haubner A, Ayers JT, Crooks PA, and Dwoskin LP

Subjects

Alkylation, Animals, Dose-Response Relationship, Drug, In Vitro Techniques, Male, Nicotinic Agonists chemistry, Nicotinic Agonists pharmacology, Nicotinic Antagonists chemistry, Perfusion, Rats, Rats, Sprague-Dawley, Stereoisomerism, Corpus Striatum drug effects, Corpus Striatum metabolism, Dopamine metabolism, Nicotine analogs & derivatives, Nicotine pharmacology, Nicotinic Antagonists classification, Nicotinic Antagonists pharmacology, Receptors, Nicotinic physiology

Abstract

The structure of the S(-)-nicotine molecule was modified via N-n-alkylation of the pyridine-N atom to afford a series of N-n-alkylnicotinium iodide salts with carbon chain lengths varying between C(1) and C(12). The ability of these analogs to evoke [(3)H] overflow and inhibit S(-)-nicotine-evoked [(3)H] overflow from [(3)H]dopamine ([(3)H]DA)-preloaded rat striatal slices was determined. At high concentrations, analogs with chain lengths > or =C(6) evoked [(3)H] overflow. Specifically, N-n-decylnicotinium iodide (NDNI; C(10)) evoked significant [(3)H] overflow at 1 microM, and N-n-dodecylnicotinium iodide (NDDNI; C(12)) at 10 microM, whereas N-n-octylnicotinium iodide (NONI; C(8)), N-n-heptylnicotinium iodide (NHpNI; C(7)), and N-n-hexylnicotinium iodide (C(6)) evoked [(3)H] overflow at 100 microM. Thus, intrinsic activity at these concentrations prohibited assessment of inhibitory activity. The most potent N-n-alkylnicotinium analog to inhibit S(-)-nicotine-evoked [(3)H] overflow was NDDNI, with an IC(50) value of 9 nM. NHpNI, NONI, and N-n-nonylnicotinium iodide (C(9)) also inhibited S(-)-nicotine-evoked [(3)H] overflow with IC(50) values of 0.80, 0.62, and 0.21 microM, respectively. In comparison, the competitive neuronal nicotinic acetylcholine receptor (nAChR) antagonist, dihydro-beta-erythroidine, had an IC(50) of 1.6 microM. A significant correlation of N-n-alkyl chain length with analog-induced inhibition was observed, with the exception of NDNI, which was devoid of inhibitory activity. The mechanism of N-n-alkylnicotinium-induced inhibition of the high-affinity, low-capacity component of S(-)-nicotine-evoked [(3)H] overflow was determined via Schild analysis, using the representative analog, NONI. Linear Schild regression and slope not different from unity suggested that NONI competitively interacts with a single nAChR subtype to inhibit S(-)-nicotine-evoked [(3)H]DA release (K(i) value = 80.2 nM). Thus, modification of the S(-)-nicotine molecule converts this agonist into an antagonist at nAChRs, mediating S(-)-nicotine-evoked DA release in striatum.

Published

2002

5. Exploring the nature of molecular recognition in nicotinic acetylcholine receptors.

Author

Schmitt JD

Subjects

Acetylcholine metabolism, Animals, Binding Sites, Chemistry, Pharmaceutical, Ligands, Models, Molecular, Molecular Structure, Nicotine metabolism, Nicotinic Agonists classification, Nicotinic Agonists metabolism, Nicotinic Antagonists classification, Nicotinic Antagonists metabolism, Protein Structure, Quaternary, Receptors, Nicotinic metabolism, Structure-Activity Relationship, Acetylcholine chemistry, Nicotine chemistry, Receptors, Nicotinic chemistry

Abstract

Nicotinic acetylcholine receptors (nAChRs) are the subject of ever increasing interest because of their presumed involvement in the etiology of numerous clinical disorders. Unfortunately, the absence of atomic-level structural data, as well as the pharmacological complexity of these receptors leaves many fundamental questions unanswered. An understanding of how ligands interact with the receptor and, in-turn, how these interactions lead to pharmacological effect is vital in the advancement of nAChR-based therapeutics. We will first explore physico-chemical themes that are evidenced to be of particular importance in nAChR molecular recognition; these are- pi-cation interaction, conformational entropy and stereochemistry. The second objective of this review is an interpretive encapsulation of the extensive and disparate body of structure-activity data that now exists for nAChRs. Finally, this review will advocate a re-investigation of distance geometry based methods as well as the need for additional approaches in nicotinic receptor pharmacophore generation.

Published

2000

6. Development of a novel class of subtype-selective nicotinic receptor antagonist: pyridine-N-substituted nicotine analogs.

Author

Dwoskin LP, Wilkins LH, Pauly JR, and Crooks PA

Subjects

Animals, Binding Sites, Binding, Competitive, Brain drug effects, Corpus Striatum drug effects, Dihydro-beta-Erythroidine pharmacology, Dopamine metabolism, Nicotinic Antagonists classification, Rats, Rubidium metabolism, Synaptosomes drug effects, Nicotine analogs & derivatives, Nicotinic Antagonists chemistry, Pyridines pharmacology, Receptors, Nicotinic metabolism

Published

1999

7. Spiropyrrolizidines: a new class of blockers of nicotinic receptors.

Author

Badio B, Shi D, Shin Y, Hutchinson KD, Padgett WL, and Daly JW

Subjects

Animals, Cells, Cultured drug effects, Dose-Response Relationship, Drug, Guinea Pigs, Humans, Mice, Nicotinic Antagonists classification, PC12 Cells drug effects, Pyrrolizidine Alkaloids classification, Radioligand Assay, Rats, Nicotinic Antagonists metabolism, Pyrrolizidine Alkaloids metabolism

Abstract

The spiropyrrolizidine oximes 236 and 222 and a related spiropyrrolizidine alkaloid, nitropolyzonamine, block nicotinic receptor channels in rat pheochromocytoma PC12 cells and in human medulloblastoma TE671 cells. In PC12 cells with an alpha 3 beta 4(5)-nicotinic receptor, both the spiropyrrolizidine oxime 236 and nitropolyzonamine had IC50 values of about 1.5 microM, while spiropyrrolizidine oxime 222 had an IC50 value of 2.6 microM versus carbamylcholine-elicited sodium-22 influx. In TE671 cells with an alpha 1 beta 1 gamma delta nicotinic receptor, the spiropyrrolizidine oximes 236, 222, and nitropolyzonamine had IC50 values of 9.5, 14, and 67 microM, respectively. The inhibitions by the spiropyrrolizidine oxime 236 and nitropolyzonamine appeared to be noncompetitive in nature in both cell lines. In rat cerebral cortical membranes, binding of [3H]nicotine to alpha 4 beta 2 nicotinic receptors was not inhibited significantly by 10 microM concentrations of the spiropyrrolizidine oxime 236, or by nitropolyzonamine, as expected for a noncompetitive blocker. Both compounds at 10 microM had marginal effects on a variety of central receptors, but did inhibit binding of [3H]1,3-di(2-tolyl) guanidine to sigma receptors in mouse brain membranes with IC50 values of about 0.5 microM. The spiropyrrolizidine oxime 236 at 10 microM had no effect on batrachotoxin-elicited sodium influx in guinea pig cerebral cortical synaptoneurosomes or on ATP-elicited calcium influx in PC12 cells. Such spiropyrrolizidines represent a new structural class of blockers of nicotinic receptor channels with selectivity for ganglionic-type receptors.

Published

1996