High-Throughput Chemical Screening and Structure-Based Models to Predict hERG Inhibition

Krishna, Shagun; Borrel, Alexandre; Huang, Ruili; Zhao, Jinghua; Xia, Menghang; Kleinstreuer, Nicole

doi:10.3390/biology11020209

Cited by 9 publications

(6 citation statements)

References 79 publications

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“…It is likely that blocking the potassium channels that hERG encodes would result in dangerous ventricular arrhythmia. All examined compounds can suppress hERG II but not hERG I, according to numerous studies [ 37 ]. However, it was anticipated that papaverine and metabolites 3 – 5 would be hepatotoxic and cause liver damage as a result of the drugs.…”

Section: Resultsmentioning

confidence: 97%

Papaverinol-N-Oxide: A Microbial Biotransformation Product of Papaverine with Potential Antidiabetic and Antiobesity Activity Unveiled with In Silico Screening

et al. 2023

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Bioconversion of biosynthetic heterocyclic compounds has been utilized to produce new semisynthetic pharmaceuticals and study the metabolites of bioactive drugs used systemically. In this investigation, the biotransformation of natural heterocyclic alkaloid papaverine via filamentous fungi was explored. Molecular docking simulations, using protein tyrosine phosphatase 1B (PTP1B), α-glucosidase and pancreatic lipase (PL) as target enzymes, were performed to investigate the antidiabetic potential of papaverine and its metabolites in silico. The metabolites were isolated from biotransformation of papaverine with Cunninghamella elegans NRRL 2310, Rhodotorula rubra NRRL y1592, Penicillium chrysogeneum ATCC 10002 and Cunninghamella blackesleeana NRRL 1369 via reduction, demethylation, N-oxidation, oxidation and hydroxylation reactions. Seven metabolites were isolated: namely, 3,4-dihydropapaverine (metabolite 1), papaveroline (metabolite 2), 7-demethyl papaverine (metabolite 3), 6,4′-didemethyl papaverine (metabolite 4), papaverine-3-ol (metabolite 5), papaverinol (metabolite 6) and papaverinol N-oxide (metabolite 7). The structural elucidation of the metabolites was investigated with 1D and 2D NMR and mass spectroscopy (EI and ESI). The molecular docking studies showed that metabolite 7 exhibited better binding interactions with the target enzymes PTP1B, α-glucosidase and PL than did papaverine. Furthermore, papaverinol-N-oxide (7) also displayed inhibition of α-glucosidase and lipase enzymes comparable to that of their ligands (acarbose and orlistat, respectively), as unveiled with an in silico ADMET profile, molecular docking and molecular dynamics studies. In conclusion, this study provides evidence for enhanced inhibition of PTP1B, α-glucosidase and PL via some papaverine fungal transformation products and, therefore, potentially better antidiabetic and antiobesity effects than those of papaverine and other known therapeutic agents.

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Section: Resultsmentioning

confidence: 97%

Papaverinol-N-Oxide: A Microbial Biotransformation Product of Papaverine with Potential Antidiabetic and Antiobesity Activity Unveiled with In Silico Screening

et al. 2023

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“…Chemical(s) in early drug development phase or candidate drug related to cardio-toxicity issue can be predicated via inhibition of affinity to hERG by animal, ex vivo, or in Silico studies. In Silico method is a favorite method because it is low costly, high throughput, computerized output, with absence of experimental lab requirements providing faster cardio-toxicity estimation [53]. Here, online estimation machine model by http://biosig.unimelb.edu.au/pkcsm/ website specified unexpected results where all 30 herbicides under testing showed NO hERG I inhibition while only P1 had hERG II inhibition (Tables 2 & 3) and (Figure 8).…”

Section: Figure (8) Total Clearance Human Maximum Tolerated Dose Herg...mentioning

confidence: 99%

Activity Prediction of Various Herbicides against Honey Bee, Avian, and Multiple Human Leukemia, CNS, Ovarian, Prostate Cancer Cell Lines

Hammud

2023

IJOIR

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Herbicides classify as chemicals targeting specific biochemical pathways in plants and may influence human or animal health according to their chemistry, concentration, environment, biological target and others. With safety concern, International Agency for Research on Cancer (IARC) classified herbicides and their metabolites as fetal developments may be a consequence of enzymatic inhibition or other mechanisms. Thirty phytotoxins were subjected to online pkCSM website, as a Quantitative Structure Activity Relationship (QSAR) prediction activity against honey bee, avian, and multiple human Leukemia, CNS, Ovarian, Prostate Cancer cell lines. Prediction outcomes were varied and influenced by chemical structure of each tested herbicide. Sulfentrazone having evidence of human non- carcinogenic character (Group E) had hepatotoxicity prediction and cancer cell lines activity less than 5 of Leukemia, CNS, Ovarian, and Prostate. Also, it had CYP1A2 inhibition, negative response of p- glycoprotein, Ames, skin sensitization, renal OCT2, and hERG. All above characters beside low intestinal absorption and Blood- Brain Barrier (BBB) presented encouraging online funding as more structurally safe having active – multiple toxicological and cellular interactions. Simetryn and Simazine that have the same core structure except (-SCH3) group replaced with chloro group gave semi identical results of many calculated characters and inactive materials to cancer cell lines and herbicide activity, honey bee and avian toxicities but not BBB, total clearance, and oral rat chronic (LOAEL) confirming structure influences upon prediction.

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“…Imatinib has shown in vitro antiviral activity against SARS-CoV-1 and Middle East respiratory syndrome (MERS)-CoV, which is related to SARS-CoV-2; thus, it has been postulated that this drug could be an unexplored treatment for SARS-CoV-2 infection. [55] , [56] Several clinical trials (e.g., NCT04394416, Phase III) are underway to evaluate the safety and efficacy of imatinib for the treatment of SARS-CoV-2. Similarly, chlorpromazine (high hERG liability, cluster 99) has been shown to inhibit in vitro viral replication of SARS-CoV-1 and MERS-CoV.…”

Section: Toxicity Potential Of Anti- Sars -Cov-2 D...mentioning

confidence: 99%

Repurposing drugs as COVID-19 therapies: A toxicity evaluation

Ngan

Xia

et al. 2022

Drug Discovery Today

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High-Throughput Chemical Screening and Structure-Based Models to Predict hERG Inhibition

Cited by 9 publications

References 79 publications

Papaverinol-N-Oxide: A Microbial Biotransformation Product of Papaverine with Potential Antidiabetic and Antiobesity Activity Unveiled with In Silico Screening

Papaverinol-N-Oxide: A Microbial Biotransformation Product of Papaverine with Potential Antidiabetic and Antiobesity Activity Unveiled with In Silico Screening

Activity Prediction of Various Herbicides against Honey Bee, Avian, and Multiple Human Leukemia, CNS, Ovarian, Prostate Cancer Cell Lines

Repurposing drugs as COVID-19 therapies: A toxicity evaluation

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