Theoretical and Experimental Relationships between Percent Inhibition and IC50 Data Observed in High-Throughput Screening

Gubler, Hanspeter; Schopfer, Ulrich; Jacoby, Edgar

doi:10.1177/1087057112455219

Cited by 30 publications

(34 citation statements)

References 23 publications

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“…Inhibitor potency was quantified by determination of IC 50 values. IC 50 determinations are typically performed at a fixed substrate concentration and the relationship between inhibitor concentrations (Gubler et al 2013). Selected dietary bioactive constituents were assayed between concentrations ranging from 1.5 to 25 μg/ml.…”

Section: Resultsmentioning

confidence: 99%

Comparative inhibitory potential of selected dietary bioactive polyphenols, phytosterols on CYP3A4 and CYP2D6 with fluorometric high-throughput screening

et al. 2014

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Cytochrome P450 (CYP450) inhibition by the bioactive molecules of dietary supplements or herbal products leading to greater potential for toxicity of co-administered drugs. The present study was aimed to compare the inhibitory potential of selected common dietary bioactive molecules (Gallic acid, Ellagic acid, β-Sitosterol, Stigmasterol, Quercetin and Rutin) on CYP3A4 and CYP2D6 to assess safety through its inhibitory potency and to predict interaction potential with co-administered drugs. CYP450-CO complex assay was carried out for all the selected dietary bioactive molecules in isolated rat microsomes. CYP450 concentration of the rat liver microsome was found to be 0.474 nmol/mg protein, quercetin in DMSO has shown maximum inhibition on CYP450 (51.02±1.24 %) but less when compared with positive control (79.02±1.61 %). In high throughput fluorometric assay, IC 50 value of quercetin (49.08±1.02-54.36± 0.85 μg/ml) and gallic acid (78.46±1.32-83.84±1.06 μg/ml) was lower than other bioactive compounds on CYP3A4 and CYP2D6 respectively but it was higher than positive controls (06.28±1.76-07.74±1.32 μg/ml). In comparison of in vitro inhibitory potential on CYP3A4 and CYP2D6, consumption of food or herbal or dietary supplements containing quercetin and gallic acid without any limitation should be carefully considered when narrow therapeutic drugs are administered together.

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Section: Resultsmentioning

confidence: 99%

Comparative inhibitory potential of selected dietary bioactive polyphenols, phytosterols on CYP3A4 and CYP2D6 with fluorometric high-throughput screening

et al. 2014

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“…Selectivity entropies were calculated from the IC 50 data of Kitagawa et al [11] or estimated from single concentration profiles as explained and validated in Figure S8 and Gubler et al . [54]. Only wild type kinases were included.…”

Section: Methodsmentioning

confidence: 99%

Comparison of the Cancer Gene Targeting and Biochemical Selectivities of All Targeted Kinase Inhibitors Approved for Clinical Use

et al. 2014

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The anti-proliferative activities of all twenty-five targeted kinase inhibitor drugs that are in clinical use were measured in two large assay panels: (1) a panel of proliferation assays of forty-four human cancer cell lines from diverse tumour tissue origins; and (2) a panel of more than 300 kinase enzyme activity assays. This study provides a head-on comparison of all kinase inhibitor drugs in use (status Nov. 2013), and for six of these drugs, the first kinome profiling data in the public domain. Correlation of drug activities with cancer gene mutations revealed novel drug sensitivity markers, suggesting that cancers dependent on mutant CTNNB1 will respond to trametinib and other MEK inhibitors, and cancers dependent on SMAD4 to small molecule EGFR inhibitor drugs. Comparison of cellular targeting efficacies reveals the most targeted inhibitors for EGFR, ABL1 and BRAF(V600E)-driven cell growth, and demonstrates that the best targeted agents combine high biochemical potency with good selectivity. For ABL1 inhibitors, we computationally deduce optimized kinase profiles for use in a next generation of drugs. Our study shows the power of combining biochemical and cellular profiling data in the evaluation of kinase inhibitor drug action.

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“…However, it is possible to estimate the IC 50 (assuming ideal conditions) using the four-parameter logistic Hill Equation (1). 14, 51 It describes the ideal relationship of inhibition percentage y at given screening concentration x with IC 50 and Hill coefficient n , and the asymptotic plateau A0 and Ainf values at low and high concentration.…”

Section: Practical Recommendationsmentioning

confidence: 99%

Hit Identification and Optimization in Virtual Screening: Practical Recommendations Based on a Critical Literature Analysis

et al. 2013

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A critical analysis of virtual screening results published between 2007 and 2011 was performed. The activity of reported hit compounds from over 400 studies was compared to their hit identification criteria. Hit rates and ligand efficiencies were calculated to assist in these analyses and the results were compared with factors such as the size of the virtual library and the number of compounds tested. A series of promiscuity, drug-like, and ADMET filters were applied to the reported hits to assess the quality of compounds reported and a careful analysis of a subset of the studies which presented hit optimization was performed. This data allowed us to make several practical recommendations with respect to selection of compounds for experimental testing, defining hit identification criteria, and general virtual screening hit criteria to allow for realistic hit optimization. A key recommendation is the use of size-targeted ligand efficiency values as hit identification criteria.

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Theoretical and Experimental Relationships between Percent Inhibition and IC50 Data Observed in High-Throughput Screening

Cited by 30 publications

References 23 publications

Comparative inhibitory potential of selected dietary bioactive polyphenols, phytosterols on CYP3A4 and CYP2D6 with fluorometric high-throughput screening

Comparative inhibitory potential of selected dietary bioactive polyphenols, phytosterols on CYP3A4 and CYP2D6 with fluorometric high-throughput screening

Comparison of the Cancer Gene Targeting and Biochemical Selectivities of All Targeted Kinase Inhibitors Approved for Clinical Use

Hit Identification and Optimization in Virtual Screening: Practical Recommendations Based on a Critical Literature Analysis

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