New role for crinamine as a potent, safe and selective inhibitor of human monoamine oxidase B: In vitro and in silico pharmacology and modeling
Language English Country Ireland Media print-electronic
Document type Comparative Study, Journal Article
PubMed
31639490
DOI
10.1016/j.jep.2019.112305
PII: S0378-8741(19)32037-9
Knihovny.cz E-resources
- Keywords
- Alkaloid, Crinamine, Crossyne guttata, Drug-likeness, Monoamine oxidase,
- MeSH
- Amaryllidaceae Alkaloids chemistry pharmacokinetics pharmacology toxicity MeSH
- Patient Safety MeSH
- Models, Biological * MeSH
- Chlorocebus aethiops MeSH
- Risk Assessment MeSH
- Monoamine Oxidase Inhibitors chemistry pharmacokinetics pharmacology toxicity MeSH
- Protein Conformation MeSH
- Humans MeSH
- Monoamine Oxidase chemistry metabolism MeSH
- Mutation MeSH
- Salmonella typhimurium drug effects genetics MeSH
- Molecular Docking Simulation * MeSH
- Vero Cells MeSH
- Cell Survival drug effects MeSH
- Structure-Activity Relationship MeSH
- Animals MeSH
- Check Tag
- Humans MeSH
- Animals MeSH
- Publication type
- Journal Article MeSH
- Comparative Study MeSH
- Names of Substances
- Amaryllidaceae Alkaloids MeSH
- crinamine MeSH Browser
- Monoamine Oxidase Inhibitors MeSH
- Monoamine Oxidase MeSH
ETHNOPHARMACOLOGICAL RELEVANCE: The development of selective inhibitors of monoamine oxidase B (MAO-B) has been essential in treating Parkinson's disease. However, the apparent hepatotoxicity and drug-drug interactions of current inhibitors accentuate the need for the development of novel pharmacotherapies. Crossyne guttata (L.) D. & U. Müll-Doblies is used frequently by Rastafarian bush doctors to treat alcoholism, a disorder which is also accentuated by MAO. OBJECTIVE: The study sought to isolate, identify and characterise the biologically active constituents of C. guttata based on their ability to inhibit the MAO enzymes. MATERIALS AND METHODS: Column chromatography was used to isolate the biologically active alkaloids of C. guttata. The ability of the alkaloids to inhibit the biotransformation of 4-aminoantipyrine by the MAO enzymes was evaluated in vitro. In silico docking was conducted using AutoDock Vina server while the pharmacokinetic properties of the compounds were evaluated using SwissADME. RESULTS: Chromatographic separation of an ethanolic fraction of C. guttata yielded the alkaloids crinamine 1 and epibuphanisine 2. 1 and 2 along with structurally related alkaloids haemanthamine 3 and haemanthidine 4 were evaluated for their ability to inhibit the action of isozymes of MAO in vitro. Alkaloids effected submicromolar IC50 values against MAO-B, the most potent of which being crinamine 1 (0.014 μM) > haemanthidine 4 (0.017 μM) > epibuphanisine 2 (0.039 μM) > haemanthamine 3 (0.112 μM). Binding energies of the alkaloids correlated well with their inhibitory potential with crinamine displaying the best binding efficacy and binding energy score with MAO-B. DISCUSSION AND CONCLUSION: Crinamine and epibuphanisine exhibited potent and selective inhibitory activity towards MAO-B. After comprehensive in silico investigations encompassing robust molecular docking analysis, the drug-like attributes and safety of the alkaloids suggest the crinamine is a potentially safe drug for human application.
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