Your search keyword '"hERG"' showing total 5,162 results

51. Effect of vinpocetine on embryonic heart rate in vitro

Author

Helen Elizabeth Ritchie, Jaimie W. Polson, Andrea Xia, and William Webster

Subjects

Vinpocetine, hERG, In vitro screen, Heart function, Birth defects, Toxicology. Poisons, RA1190-1270

Abstract

Vinpocetine is a readily available nutritional supplement claimed to improve memory and weight loss. However, it blocks the Ikr current essential for cardiac action potential repolarisation and Ikr inhibition can cause “torsade de pointes” arrhythmias and sudden death. Moreover, Ikr blockers have exhibited teratogenic effects in reproductive toxicology studies, leading to increased birth defects and embryonic mortality. The FDA advises against vinpocetine use in pregnant and prospective mothers based on animal studies showing dose-dependent fetal mortality in rats and rabbits, and cardiovascular malformations in surviving fetuses. However, the mechanisms responsible for vinpocetine's fetal toxicity remain unclear.The present study used rat embryo culture to evaluate vinpocetine and its major metabolite, apovincaminic acid, on embryonic heart rate, a possible causative factor behind its adverse effects. Both compounds induced embryonic bradycardia in a concentration-dependent manner, with vinpocetine proving more potent.The minimum vinpocentine concentration to induce bradycardia was 100 nM, a level unlikely to be reached in humans following typical doses. Embryonic arrhythmias were also observed at the highest concentrations.These results suggest that the FDA's cautionary statement may generate undue anxiety, although re-evaluation of teratogenicity risk associated with vinpocetine should be revisited if a link to cardiac arrhythmias in adults is established.

Published

2023

52. Digging into Lipid Membrane Permeation for Cardiac Ion Channel Blocker d-Sotalol with All-Atom Simulations

Author

DeMarco, Kevin R, Bekker, Slava, Clancy, Colleen E, Noskov, Sergei Y, and Vorobyov, Igor

Subjects

Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, Cardiovascular, Bioengineering, Generic health relevance, hERG, long QT syndrome, cardiotoxicity, CHARMM force field, molecular dynamics, umbrella sampling, lipophilicity, water-membrane partitioning, Pharmacology and pharmaceutical sciences

Abstract

Interactions of drug molecules with lipid membranes play crucial role in their accessibility of cellular targets and can be an important predictor of their therapeutic and safety profiles. Very little is known about spatial localization of various drugs in the lipid bilayers, their active form (ionization state) or translocation rates and therefore potency to bind to different sites in membrane proteins. All-atom molecular simulations may help to map drug partitioning kinetics and thermodynamics, thus providing in-depth assessment of drug lipophilicity. As a proof of principle, we evaluated extensively lipid membrane partitioning of d-sotalol, well-known blocker of a cardiac potassium channel Kv11.1 encoded by the hERG gene, with reported substantial proclivity for arrhythmogenesis. We developed the positively charged (cationic) and neutral d-sotalol models, compatible with the biomolecular CHARMM force field, and subjected them to all-atom molecular dynamics (MD) simulations of drug partitioning through hydrated lipid membranes, aiming to elucidate thermodynamics and kinetics of their translocation and thus putative propensities for hydrophobic and aqueous hERG access. We found that only a neutral form of d-sotalol accumulates in the membrane interior and can move across the bilayer within millisecond time scale, and can be relevant to a lipophilic channel access. The computed water-membrane partitioning coefficient for this form is in good agreement with experiment. There is a large energetic barrier for a cationic form of the drug, dominant in water, to cross the membrane, resulting in slow membrane translocation kinetics. However, this form of the drug can be important for an aqueous access pathway through the intracellular gate of hERG. This route will likely occur after a neutral form of a drug crosses the membrane and subsequently re-protonates. Our study serves to demonstrate a first step toward a framework for multi-scale in silico safety pharmacology, and identifies some of the challenges that lie therein.

Published

2018

53. Ligand-based prediction of hERG-mediated cardiotoxicity based on the integration of different machine learning techniques.

Author

Delre, Pietro, Lavado, Giovanna J., Lamanna, Giuseppe, Saviano, Michele, Roncaglioni, Alessandra, Benfenati, Emilio, Mangiatordi, Giuseppe Felice, and Gadaleta, Domenico

Subjects

BOOSTING algorithms, DRUG side effects, MACHINE learning, CARDIOTOXICITY, DRUG discovery, POTASSIUM channels, FEATURE selection

Abstract

Drug-induced cardiotoxicity is a common side effect of drugs in clinical use or under postmarket surveillance and is commonly due to off-target interactions with the cardiac human-ether-a-go-go-related (hERG) potassium channel. Therefore, prioritizing drug candidates based on their hERG blocking potential is a mandatory step in the early preclinical stage of a drug discovery program. Herein, we trained and properly validated 30 ligandbased classifiers of hERG-related cardiotoxicity based on 7,963 curated compounds extracted by the freely accessible repository ChEMBL (version 25). Different machine learning algorithms were tested, namely, random forest, K-nearest neighbors, gradient boosting, extreme gradient boosting, multilayer perceptron, and support vector machine. The application of 1) the best practices for data curation, 2) the feature selection method VSURF, and 3) the synthetic minority oversampling technique (SMOTE) to properly handle the unbalanced data, allowed for the development of highly predictive models (BAMAX = 0.91, AUCMAX = 0.95). Remarkably, the undertaken temporal validation approach not only supported the predictivity of the herein presented classifiers but also suggested their ability to outperform those models commonly used in the literature. From a more methodological point of view, the study put forward a new computational workflow, freely available in the GitHub repository (https://github.com/PDelre93/hERG-QSAR), as valuable for building highly predictive models of hERG-mediated cardiotoxicity. [ABSTRACT FROM AUTHOR]

Published

2022

54. Clinical update of medications associated with QT prolongation among COVID-19 patients.

Author

Herbert, Ernest and Fournier, Dominique

Subjects

*COVID-19 pandemic, *CHLOROQUINE, *ANTIMALARIALS, *ELECTROCARDIOGRAPHY, *ARRHYTHMIA

Abstract

In the struggle against COVID-19 pandemic, chloroquine (CQ) (a 4-aminoquinoline) and its derivative hydroxychloroquine (HCQ) have both been used as a potential form of treatment among infected patients. Originally known as an antimalarial quinolone, many countries have adopted their use as an option to treat COVID-19 patients. In humans, dose-dependent chloroquine induces QT interval prolongation. It also blocks the human ether-a-go-go-related gene (hERG), which encodes the rapidly activating delayed rectifier K+ channel. The action potential duration is then prolonged, as the eventual QTc interval of the electrocardiogram (ECG), resulting in torsade de pointes and cardiac arrhythmias that could lead to sudden death. It is yet unknown whether COVID-19 itself has any effect on the QTc interval. The current review established what is new and different from other studies involving the use of chloroquine and hydroxychloroquine among COVID-19 patients plus the corresponding QT interval prolongation in affected individuals. [ABSTRACT FROM AUTHOR]

Published

2022

55. New Diarylamine K V 10.1 Inhibitors and Their Anticancer Potential.

Author

Gubič, Špela, Toplak, Žan, Shi, Xiaoyi, Dernovšek, Jaka, Hendrickx, Louise Antonia, Pinheiro-Junior, Ernesto Lopes, Peigneur, Steve, Tytgat, Jan, Pardo, Luis A., Peterlin Mašič, Lucija, and Tomašič, Tihomir

Subjects

*DRUG discovery, *POTASSIUM channels, *STRUCTURE-activity relationships, *DRUG design, *CELL lines, *CELL growth

Abstract

Expression of the voltage-gated potassium channel KV10.1 (Eag1) has been detected in over 70% of human cancers, making the channel a promising new target for new anticancer drug discovery. A new structural class of KV10.1 inhibitors was prepared by structural optimisation and exploration of the structure–activity relationship of the previously published hit compound ZVS-08 (1) and its optimised analogue 2. The potency and selectivity of the new inhibitors between KV10.1 and hERG were investigated using whole-cell patch-clamp experiments. We obtained two new optimised KV10.1 inhibitors, 17a and 18b, with improved nanomolar IC50 values of 568 nM and 214 nM, respectively. Compound 17a exhibited better ratio between IC50 values for hEAG1 and hERG than previously published diarylamine inhibitors. Compounds 17a and 18b moderately inhibited the growth of the KV10.1-expressing cell line MCF-7 in two independent assays. In addition, 17a and 18b also inhibited the growth of hERG-expressing Panc-1 cells with higher potency compared with MCF-7 cells. The main obstacle for newly developed diarylamine KV10.1 inhibitors remains the selectivity toward the hERG channel, which needs to be addressed with targeted drug design strategies in the future. [ABSTRACT FROM AUTHOR]

Published

2022

56. The Effect of Fungicide Ziram on the hERG Potassium Channel

Author

Kearney, Brian P

Subjects

Physiology, Neurosciences, Electrophysiology, hERG, Ion Channel, Parkinsons Disease, Potassium Channel, Ziram

Abstract

Pesticides have been extensively used in agriculture for over a century but concerns regarding their negative impact on human health persist. The relationship between pesticides and human pathogenesis is complex and poorly understood, with myriad factors influencing their effects. Among the health risks associated with pesticide exposure, the development of neurodegenerative diseases, including Parkinson's disease (PD), is of particular concern. The fungicide Ziram has been shown to cause neurotoxicity as well as an increased risk of PD in those who have been chronically exposed. However, the precise mechanism for this effect remains unclear. In the fruitfly Drosophila melanogaster, Ziram has been shown to increase neuronal excitability by blocking the ether-a-gogo (eag) family of potassium channels. Ziram also increases excitability in mammalian neurons, and we here test the hypothesis that Ziram directly blocks hERG (human eag related gene) potassium channels. Using a non-neuronal cell line expressing hERG we find that Ziram indeed does block this potassium channel. Our data suggest that Ziram acts directly on hERG rather than an accessory subunit.

Published

2023

57. Series of (([1,1′-Biphenyl]-2-yl)methyl)sulfinylalkyl Alicyclic Amines as Novel and High Affinity Atypical Dopamine Transporter Inhibitors with Reduced hERG Activity

Author

Ku, Therese C., Cao, Jianjing, Won, Sung Joon, Guo, Jiqing, Camacho-Hernandez, Gisela A., Okorom, Amarachi V., Salomon, Kristine Walloe, Lee, Kuo Hao, Loland, Claus J., Duff, Henry J., Shi, Lei, Newman, Amy Hauck, Ku, Therese C., Cao, Jianjing, Won, Sung Joon, Guo, Jiqing, Camacho-Hernandez, Gisela A., Okorom, Amarachi V., Salomon, Kristine Walloe, Lee, Kuo Hao, Loland, Claus J., Duff, Henry J., Shi, Lei, and Newman, Amy Hauck

Abstract

Currently, there are no FDA-approved medications for the treatment of psychostimulant use disorders (PSUD). We have previously discovered “atypical” dopamine transporter (DAT) inhibitors that do not display psychostimulant-like behaviors and may be useful as medications to treat PSUD. Lead candidates (e.g., JJC8-091, 1) have shown promising in vivo profiles in rodents; however, reducing hERG (human ether-à-go-go-related gene) activity, a predictor of cardiotoxicity, has remained a challenge. Herein, a series of 30 (([1,1′-biphenyl]-2-yl)methyl)sulfinylalkyl alicyclic amines was synthesized and evaluated for DAT and serotonin transporter (SERT) binding affinities. A subset of analogues was tested for hERG activity, and the IC50 values were compared to those predicted by our hERG QSAR models, which showed robust predictive power. Multiparameter optimization scores (MPO > 3) indicated central nervous system (CNS) penetrability. Finally, comparison of affinities in human DAT and its Y156F and Y335A mutants suggested that several compounds prefer an inward facing conformation indicating an atypical DAT inhibitor profile., Currently, there are no FDA-approved medications for the treatment of psychostimulant use disorders (PSUD). We have previously discovered “atypical” dopamine transporter (DAT) inhibitors that do not display psychostimulant-like behaviors and may be useful as medications to treat PSUD. Lead candidates (e.g., JJC8-091, 1) have shown promising in vivo profiles in rodents; however, reducing hERG (human ether-à-go-go-related gene) activity, a predictor of cardiotoxicity, has remained a challenge. Herein, a series of 30 (([1,1′-biphenyl]-2-yl)methyl)sulfinylalkyl alicyclic amines was synthesized and evaluated for DAT and serotonin transporter (SERT) binding affinities. A subset of analogues was tested for hERG activity, and the IC50 values were compared to those predicted by our hERG QSAR models, which showed robust predictive power. Multiparameter optimization scores (MPO > 3) indicated central nervous system (CNS) penetrability. Finally, comparison of affinities in human DAT and its Y156F and Y335A mutants suggested that several compounds prefer an inward facing conformation indicating an atypical DAT inhibitor profile.

Published

2024

58. Harnessing AlphaFold to reveal hERG channel conformational state secrets.

Author

Ngo K, Yang PC, Yarov-Yarovoy V, Clancy CE, and Vorobyov I

Abstract

To design safe, selective, and effective new therapies, there must be a deep understanding of the structure and function of the drug target. One of the most difficult problems to solve has been resolution of discrete conformational states of transmembrane ion channel proteins. An example is KV11.1 (hERG), comprising the primary cardiac repolarizing current, I . hERG is a notorious drug anti-target against which all promising drugs are screened to determine potential for arrhythmia. Drug interactions with the hERG inactivated state are linked to elevated arrhythmia risk, and drugs may become trapped during channel closure. However, the structural details of multiple conformational states have remained elusive. Here, we guided AlphaFold2 to predict plausible hERG inactivated and closed conformations, obtaining results consistent with multiple available experimental data. Drug docking simulations demonstrated hERG state-specific drug interactions in good agreement with experimental results, revealing that most drugs bind more effectively in the inactivated state and are trapped in the closed state. Molecular dynamics simulations demonstrated ion conduction for an open but not AlphaFold2 predicted inactivated state that aligned with earlier studies. Finally, we identified key molecular determinants of state transitions by analyzing interaction networks across closed, open, and inactivated states in agreement with earlier mutagenesis studies. Here, we demonstrate a readily generalizable application of AlphaFold2 as an effective and robust method to predict discrete protein conformations, reconcile seemingly disparate data and identify novel linkages from structure to function.Kr . hERG is a notorious drug anti-target against which all promising drugs are screened to determine potential for arrhythmia. Drug interactions with the hERG inactivated state are linked to elevated arrhythmia risk, and drugs may become trapped during channel closure. However, the structural details of multiple conformational states have remained elusive. Here, we guided AlphaFold2 to predict plausible hERG inactivated and closed conformations, obtaining results consistent with multiple available experimental data. Drug docking simulations demonstrated hERG state-specific drug interactions in good agreement with experimental results, revealing that most drugs bind more effectively in the inactivated state and are trapped in the closed state. Molecular dynamics simulations demonstrated ion conduction for an open but not AlphaFold2 predicted inactivated state that aligned with earlier studies. Finally, we identified key molecular determinants of state transitions by analyzing interaction networks across closed, open, and inactivated states in agreement with earlier mutagenesis studies. Here, we demonstrate a readily generalizable application of AlphaFold2 as an effective and robust method to predict discrete protein conformations, reconcile seemingly disparate data and identify novel linkages from structure to function., Competing Interests: Competing Interest Statement: The authors declare no competing interests.

Published

2024

59. Leukotriene B4 is elevated in diabetes and promotes ventricular arrhythmogenesis in guinea pig.

Author

Corbin A, Aromolaran KA, and Aromolaran AS

Abstract

Diabetes (DM) patients have an increased risk (~50%) for sudden cardiac death (SCD), mostly as a result of ventricular arrhythmias. The molecular mechanisms involved remain partially defined. The potent proinflammatory lipid mediator leukotriene (LT) B4, is pathologically elevated in DM compared to nondiabetic patients, resulting in increased LTB4 accumulation in heart, leading to an increased risk for life-threatening proarrhythmic signatures. We used electrophysiology, immunofluorescence, and confocal microscopy approaches to evaluate LTB4 cellular effects in guinea pig heart and ventricular myocytes. We have observed that LTB4 is increased in multiple mouse models (C57BL/6 J/Lep ob/ob and PANIC-ATTAC) of DM, promotes profound cellular arrhythmogenesis (spontaneous beats and early after depolarizations, EADs), and severely depresses the rapidly activating delayed rectifier K current (hERG1/I Kr ) density in HEK293 cells and guinea pig ventricular myocytes. We have further found that guinea pigs challenged with LTB4 displayed a significantly prolonged QT interval, and that this can be prevented with LTB4R inhibition, suggesting that preventing such LTB4R effects may be therapeutically beneficial in DM. Our data suggests that a further elucidation of LTB4 vulnerable substrates, and how this leads to ventricular arrhythmias, is likely to lead to continued improvements in management options, and the development of new therapies for prevention of SCD in DM patients., (© 2024 The Author(s). Journal of Cellular Physiology published by Wiley Periodicals LLC.)

Published

2024

60. Inhibition of hERG K channels by verapamil at physiological temperature: Implications for the CiPA initiative.

Author

Johnson AA and Trudeau MC

Abstract

The Comprehensive in vitro Proarrhythmia Assay (CiPA) initiative reassesses using the inhibition of hERG potassium channels by drugs as the major determinant for the potential to cause drug-induced Torsades de Pointes (TdP) cardiac arrhythmias. Here we report our findings on the next phase of CiPA: Determination of hERG inhibitory properties using the standard CiPA-defined data acquisition protocol, here called the standard protocol, at physiological temperature (37 degrees Celsius). To do this, we measured inhibition of hERG1a potassium channels stably expressed in HEK293 cells by the small molecule verapamil, using manual whole-cell patch-clamp electrophysiology recordings with the standard protocol, which is characterized, in part, by a series of 10 s duration voltage steps to 0 mV, ultimately leading to a cumulative recording time of approximately 30 min. Using the standard protocol, we measured an IC 50 for verapamil of 225 nM, a Hill coefficient of 1, and time constant of inhibition at 0 mV of 0.64 s. But, using the standard protocol resulted in a very low (5 %) experimental success rate per cell, which had low practicality for future experiments. To address the 5 % success rate, we generated a revised protocol characterized, in part, by a series of 3 s duration voltage steps to 0 mV, leading to a cumulative recording time of approximately 10 min. Using the revised protocol, we found an IC 50 for verapamil of 252 nM, a Hill coefficient of 0.8, and time constant of inhibition at 0 mV of 0.67 s. The values measured with the revised protocol were similar to those measured using the standard protocol and, furthermore, our success rate using the revised protocol rose to 25 %, an increase of 5-fold over the standard protocol, and more in line with the success rate for biophysical studies. In summary, we captured key pharmacological data for subsequent analysis in CiPA using a revised protocol with an increased success rate and an overall enhanced feasibility and practicality. We propose that the revised protocol may be more pragmatic for generation of some hERG channel drug inhibition data for CiPA and other regulatory sciences., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024. Published by Elsevier Inc.)

Published

2024

61. The role of the HERG channel in the secretion of glucagon-like peptide-1 (GLP-1) from murine intestinal L-cells

Author

Yuan, Ying-Chao, Liu, Chang, Xie, Rong-Rong, Zhang, Lin, Wang, Hao, and Yang, Jin-Kui

Published

2023

62. Chaperone Rer1 involves in transport of hERG potassium channel protein in cell line HEK293T

Author

CHEN Bang-sheng, YU Xiao-ling, MAO Fei-yan, LIAN Jiang-fang, YU Xu-yun

Subjects

chaperone, rer1, herg, lqts, Medicine

Abstract

Objective To investigate the role of Rer1 in hERG potassium channel protein transport,and to study the medicine Baf A1 that may restore abnormal hERG transport. Methods HEK293T cells were transiently transfected with constructed A561V mutant and WT plasmids, the wild-type,mutant and mixed transfection cell models were established.The expressions of hERG and Rer1 were detected by immunofluorescence and Western blot.siRNA was used to knockdown the expression of Rer1 and detect the expression of hERG;Bafilomycin A1,a V-ATPase inhibitor was incubated with 1 mmol/L for 6 hours.Western blot was used to detect the changes of hERG protein before and after the incubation.Patch clamp was used to measure the current of potential functional in mixed transfection cells. Results Compared with the WT group,A561V-mutation could cause trafficking deficient of hERG protein.The PM expression of hERG in mutant group was significantly reduced(P＜0.01).The expression of Rer1 in mutation and mixed transfection groups decreased significantly(P＜0.01).Knockdown of Rer1 promoted the forward transport of mature hERG.Besides,after incubation with Baf A1,the mature hERG protein in WT and mutant groups increased significantly(P＜0.05),while the immature hERG in the mixed transformation group was significantly increased(P＜0.05).Relative density of tail current was elevated following incubation with Baf A1 compared with control. Conclusions Rer1 is involved in the transport of hERG potassium channel and inhibits the forward transport of some abnormal hERG.Baf A1 significantly enhances the tail current density of mixed transfection cells.

Published

2021

63. Evolutionary coupling analysis guides identification of mistrafficking-sensitive variants in cardiac K+ channels: Validation with hERG

Author

Yihong Zhang, Amy L. Grimwood, Jules C. Hancox, Stephen C. Harmer, and Christopher E. Dempsey

Subjects

misfolding, long QT syndrome, ClinVar, pathogenic, evolutionary coupling, hERG, Therapeutics. Pharmacology, RM1-950

Abstract

Loss of function (LOF) mutations of voltage sensitive K+ channel proteins hERG (Kv11.1) and KCNQ1 (Kv7.1) account for the majority of instances of congenital Long QT Syndrome (cLQTS) with the dominant molecular phenotype being a mistrafficking one resulting from protein misfolding. We explored the use of Evolutionary Coupling (EC) analysis, which identifies evolutionarily conserved pairwise amino acid interactions that may contribute to protein structural stability, to identify regions of the channels susceptible to misfolding mutations. Comparison with published experimental trafficking data for hERG and KCNQ1 showed that the method strongly predicts “scaffolding” regions of the channel membrane domains and has useful predictive power for trafficking phenotypes of individual variants. We identified a region in and around the cytoplasmic S2-S3 loop of the hERG Voltage Sensor Domain (VSD) as susceptible to destabilising mutation, and this was confirmed using a quantitative LI-COR® based trafficking assay that showed severely attenuated trafficking in eight out of 10 natural hERG VSD variants selected using EC analysis. Our analysis highlights an equivalence in the scaffolding structures of the hERG and KCNQ1 membrane domains. Pathogenic variants of ion channels with an underlying mistrafficking phenotype are likely to be located within similar scaffolding structures that are identifiable by EC analysis.

Published

2022

64. Ligand-based prediction of hERG-mediated cardiotoxicity based on the integration of different machine learning techniques

Author

Pietro Delre, Giovanna J. Lavado, Giuseppe Lamanna, Michele Saviano, Alessandra Roncaglioni, Emilio Benfenati, Giuseppe Felice Mangiatordi, and Domenico Gadaleta

Subjects

hERG, cardiotoxicity, QSAR, ligand-based, consensus modeling, Therapeutics. Pharmacology, RM1-950

Abstract

Drug-induced cardiotoxicity is a common side effect of drugs in clinical use or under postmarket surveillance and is commonly due to off-target interactions with the cardiac human-ether-a-go-go-related (hERG) potassium channel. Therefore, prioritizing drug candidates based on their hERG blocking potential is a mandatory step in the early preclinical stage of a drug discovery program. Herein, we trained and properly validated 30 ligand-based classifiers of hERG-related cardiotoxicity based on 7,963 curated compounds extracted by the freely accessible repository ChEMBL (version 25). Different machine learning algorithms were tested, namely, random forest, K-nearest neighbors, gradient boosting, extreme gradient boosting, multilayer perceptron, and support vector machine. The application of 1) the best practices for data curation, 2) the feature selection method VSURF, and 3) the synthetic minority oversampling technique (SMOTE) to properly handle the unbalanced data, allowed for the development of highly predictive models (BAMAX = 0.91, AUCMAX = 0.95). Remarkably, the undertaken temporal validation approach not only supported the predictivity of the herein presented classifiers but also suggested their ability to outperform those models commonly used in the literature. From a more methodological point of view, the study put forward a new computational workflow, freely available in the GitHub repository (https://github.com/PDelre93/hERG-QSAR), as valuable for building highly predictive models of hERG-mediated cardiotoxicity.

Published

2022

65. Inhibition of the hERG Potassium Channel by a Methanesulphonate-Free E-4031 Analogue

Author

Matthew V. Helliwell, Yihong Zhang, Aziza El Harchi, Christopher E. Dempsey, and Jules C. Hancox

Subjects

E-4031, E-4031-17, heart, hERG, long QT, methanesulphonanilide, Medicine, Pharmacy and materia medica, RS1-441

Abstract

hERG (human Ether-à-go-go Related Gene)-encoded potassium channels underlie the cardiac rapid delayed rectifier (IKr) potassium current, which is a major target for antiarrhythmic agents and diverse non-cardiac drugs linked to the drug-induced form of long QT syndrome. E-4031 is a high potency hERG channel inhibitor from the methanesulphonanilide drug family. This study utilized a methanesulphonate-lacking E-4031 analogue, “E-4031-17”, to evaluate the role of the methanesulphonamide group in E-4031 inhibition of hERG. Whole-cell patch-clamp measurements of the hERG current (IhERG) were made at physiological temperature from HEK 293 cells expressing wild-type (WT) and mutant hERG constructs. For E-4031, WT IhERG was inhibited by a half-maximal inhibitory concentration (IC50) of 15.8 nM, whilst the comparable value for E-4031-17 was 40.3 nM. Both compounds exhibited voltage- and time-dependent inhibition, but they differed in their response to successive applications of a long (10 s) depolarisation protocol, consistent with greater dissociation of E-4031-17 than the parent compound between applied commands. Voltage-dependent inactivation was left-ward voltage shifted for E-4031 but not for E-4031-17; however, inhibition by both compounds was strongly reduced by attenuated-inactivation mutations. Mutations of S6 and S5 aromatic residues (F656V, Y652A, F557L) greatly attenuated actions of both drugs. The S624A mutation also reduced IhERG inhibition by both molecules. Overall, these results demonstrate that the lack of a methanesulphonate in E-4031-17 is not an impediment to high potency inhibition of IhERG.

Published

2023

66. The Strength of hERG Inhibition by Erythromycin at Different Temperatures Might Be Due to Its Interacting Features with the Channels

Author

Dongrong Cheng, Xiaofeng Wei, Yanting Zhang, Qian Zhang, Jianwei Xu, Jiaxin Yang, Junjie Yu, Antony Stalin, Huan Liu, Jintao Wang, Dian Zhong, Lanying Pan, Wei Zhao, and Yuan Chen

Subjects

erythromycin, temperature, hERG, steady-state activation, steady-state inactivation, Organic chemistry, QD241-441

Abstract

Erythromycin is one of the few compounds that remarkably increase ether-a-go-go-related gene (hERG) inhibition from room temperature (RT) to physiological temperature (PT). Understanding how erythromycin inhibits the hERG could help us to decide which compounds are needed for further studies. The whole-cell patch clamp technique was used to investigate the effects of erythromycin on hERG channels at different temperatures. While erythromycin caused a concentration-dependent inhibition of cardiac hERG channels, it also shifted the steady-state activation and steady-state inactivation of the channel to the left and significantly accelerated the onset of inactivation at both temperatures, although temperature itself caused a profound change in the dynamics of hERG channels. Our data also suggest that the binding pattern to S6 of the channels changes at PT. In contrast, cisapride, a well-known hERG blocker whose inhibition is not affected by temperature, does not change its critical binding sites after the temperature is raised to PT. Our data suggest that erythromycin is unique and that the shift in hERG inhibition may not apply to other compounds.

Published

2023

67. There is no F in APC: Using physiological fluoride-free solutions for high throughput automated patch clamp experiments.

Author

Rapedius, Markus, Obergrussberger, Alison, Humphries, Edward S. A., Scholz, Stephanie, Rinke-Weiss, Ilka, Goetze, Tom A., Brinkwirth, Nina, Rotordam, Maria Giustina, Strassmaier, Tim, Randolph, Aaron, Friis, Søren, Liutkute, Aiste, Seibertz, Fitzwilliam, Voigt, Niels, and Fertig, Niels

Subjects

CHO cell, VOLTAGE control, FLUORIDES, ION channels, UMBILICAL cord clamping

Abstract

Fluoride has been used in the internal recording solution for manual and automated patch clamp experiments for decades because it helps to improve the seal resistance and promotes longer lasting recordings. In manual patch clamp, fluoride has been used to record voltage-gated Na (NaV) channels where seal resistance and access resistance are critical for good voltage control. In automated patch clamp, suction is applied from underneath the patch clamp chip to attract a cell to the hole and obtain a good seal. Since the patch clamp aperture cannot be moved to improve the seal like the patch clamp pipette in manual patch clamp, automated patch clamp manufacturers use internal fluoride to improve the success rate for obtaining GΩ seals. However, internal fluoride can affect voltage-dependence of activation and inactivation, as well as affecting internal second messenger systems and therefore, it is desirable to have the option to perform experiments using physiological, fluoride-free internal solution. We have developed an approach for high throughput fluoride-free recordings on a 384-well based automated patch clamp system with success rates >40% for GΩ seals. We demonstrate this method using hERG expressed in HEK cells, as well as NaV1.5, NaV1.7, and KCa3.1 expressed in CHO cells. We describe the advantages and disadvantages of using fluoride and provide examples of where fluoride can be used, where caution should be exerted and where fluoride-free solutions provide an advantage over fluoride-containing solutions. [ABSTRACT FROM AUTHOR]

Published

2022

68. A Review of Computational Methods in Predicting hERG Channel Blockers.

Author

Shan, Mengyi, Jiang, Chen, Qin, Lu‐Ping, and Cheng, Gang

Subjects

*DRUG discovery, *VENTRICULAR arrhythmia, *DRUG development, *PREDICTION models, *CARDIOTOXICITY, *ION channels, *ARRHYTHMIA

Abstract

Inhibition of the human ether‐à‐go‐go‐related gene (hERG) ion channel may lead to prolonged QT interval and even fatal ventricular arrhythmia. Therefore, evaluating the hERG liability has become a mandatory requirement for drug development and drug safety process. However, standard experimental assays are complex, expensive and time‐consuming. Various in silico tools have been developed to identify potential hERG blockers and reduce in advance the risk of cardiotoxicity‐related attritions during the early drug discovery phase. In this review, we first outlined the structure and gating properties of the hERG channel briefly. Then analyzed the advantages of computational technology, and comprehensively summarized the in silico methods of hERG‐related cardiotoxicity, including ligand‐based and structure‐based methods. Additionally, the current predictive models in prediction of hERG blockage were emphatically reviewed. Finally, issues involved in the current computational methods, as well as the future direction for developing reliable models of hERG channel blockers, are discussed. [ABSTRACT FROM AUTHOR]

Published

2022

69. Multiple mechanisms underlie reduced potassium conductance in the p.T1019PfsX38 variant of hERG.

Author

Al Salmani, Majid K., Tavakoli, Rezvan, Zaman, Wajid, and Al Harrasi, Ahmed

Subjects

*LONG QT syndrome, *CARDIAC arrest, *BRUGADA syndrome, *GENETIC variation, *POTASSIUM, *DEEP learning

Abstract

Long QT syndrome type II (LQT2) is caused by loss‐of‐function mutations in the hERG K+ channel, leading to increased incidence of cardiac arrest and sudden death. Many genetic variants have been reported in the hERG gene with various consequences on channel expression, permeation, and gating. Only a small number of LQT2 causing variants has been characterized to define the underlying pathophysiological causes of the disease. We sought to determine the characteristics of the frameshift variant p.Thr1019ProfsX38 (T1019PfsX38) which affects the C‐terminus of the protein. This mutation was identified in an extended Omani family of LQT2. It replaces the last 140 amino acids of hERG with 37 unique amino acids. T1019 is positioned at a distinguished region of the C‐terminal tail of hERG, as predicted from the deep learning system AlphaFold v2.0. We employed the whole‐cell configuration of the patch‐clamp technique to study wild‐type and mutant channels that were transiently expressed in human embryonic kidney 293 (HEK293) cells. Depolarizing voltages elicited slowly deactivating tail currents that appeared upon repolarization of cells that express either wild‐type‐ or T1019PfsX38‐hERG. There were no differences in the voltage and time dependencies of activation between the two variants. However, the rates of hERG channel deactivation at hyperpolarizing potentials were accelerated by T1019PfsX38. In addition, the voltage dependence of inactivation of T1019PfsX38‐hERG was shifted by 20 mV in the negative direction when compared with wild‐type hERG. The rates of channel inactivation were increased in the mutant channel variant. Next, we employed a step‐ramp protocol to mimic membrane repolarization by the cardiac action potential. The amplitudes of outward currents and their integrals were reduced in the mutant variant when compared with the wild‐type variant during repolarization. Thus, changes in the gating dynamics of hERG by the T1019PfsX38 variant contribute to the pathology seen in affected LQT2 patients. [ABSTRACT FROM AUTHOR]

Published

2022

70. A massively parallel assay accurately discriminates between functionally normal and abnormal variants in a hotspot domain of KCNH2.

Author

Ng, Chai-Ann, Ullah, Rizwan, Farr, Jessica, Hill, Adam P., Kozek, Krystian A., Vanags, Loren R., Mitchell, Devyn W., Kroncke, Brett M., and Vandenberg, Jamie I.

Subjects

*BRUGADA syndrome, *LONG QT syndrome, *CARDIAC arrest, *FUNCTIONAL genomics

Abstract

Many genes, including KCNH2 , contain "hotspot" domains associated with a high density of variants associated with disease. This has led to the suggestion that variant location can be used as evidence supporting classification of clinical variants. However, it is not known what proportion of all potential variants in hotspot domains cause loss of function. Here, we have used a massively parallel trafficking assay to characterize all single-nucleotide variants in exon 2 of KCNH2 , a known hotspot for variants that cause long QT syndrome type 2 and an increased risk of sudden cardiac death. Forty-two percent of KCNH2 exon 2 variants caused at least 50% reduction in protein trafficking, and 65% of these trafficking-defective variants exerted a dominant-negative effect when co-expressed with a WT KCNH2 allele as assessed using a calibrated patch-clamp electrophysiology assay. The massively parallel trafficking assay was more accurate (AUC of 0.94) than bioinformatic prediction tools (REVEL and CardioBoost, AUC of 0.81) in discriminating between functionally normal and abnormal variants. Interestingly, over half of variants in exon 2 were found to be functionally normal, suggesting a nuanced interpretation of variants in this "hotspot" domain is necessary. Our massively parallel trafficking assay can provide this information prospectively. [ABSTRACT FROM AUTHOR]

Published

2022

71. Repurposing drugs as COVID-19 therapies: A toxicity evaluation.

Author

Ngan, Deborah K., Xu, Tuan, Xia, Menghang, Zheng, Wei, and Huang, Ruili

Subjects

*COVID-19, *COVID-19 treatment, *DRUG repositioning, *DRUG therapy, *TOXICITY testing, *DRUG interactions, *ANTIVIRAL agents

Abstract

• Drugs repurposed as anti-SARS-CoV-2 candidates may have undesirable side effects due to hERG inhibition and/or phospholipidosis induction. • Anti-SARS-CoV-2 drug candidates are categorized by their level of hERG liability. • Autophagy may play a central role in the antiviral mechanisms and toxic effects of anti-SARS-CoV-2 compounds. Drug repurposing is an appealing method to address the Coronavirus 2019 (COVID-19) pandemic because of the low cost and efficiency. We analyzed our in-house database of approved drug screens and compared their activity profiles with results from a severe acute respiratory syndrome-coronavirus 2 (SARS-CoV-2) cytopathic effect (CPE) assay. The activity profiles of the human ether-à-go-go-related gene (hERG), phospholipidosis (PLD), and many cytotoxicity screens were found significantly correlated with anti-SARS-CoV-2 activity. hERG inhibition is a nonspecific off-target effect that has contributed to promiscuous drug interactions, whereas drug-induced PLD is an undesirable effect linked to hERG blockers. Thus, this study identifies preferred drug candidates as well as chemical structures that should be avoided because of their potential to induce toxicity. Lastly, we highlight the hERG liability of anti-SARS-CoV-2 drugs currently enrolled in clinical trials. [ABSTRACT FROM AUTHOR]

Published

2022

72. The HERG K+ Channel increases Intracellular Calcium in myotubes by modulation of Calsequestrin.

Author

Pond, Amber, Guha, Shalini, LaVigne, Emily, McClure, Natalie, Koran, Jennifer, and Hockerman, Gregory H.

Subjects

*INTRACELLULAR calcium, *NUCLEOTIDE sequencing, *RYANODINE receptors, *CALCIUM channels, *SARCOPLASMIC reticulum

Abstract

The ERG1A K+ channel upregulates protein degradation in skeletal muscle atrophying in response to disuse1 and is found upregulated in muscle atrophying in response to cancer1 and denervation2. We have shown that overexpression of the HERG channel increases basal intracellular calcium concentration ([Ca2+]i) and calpain activity in C2C12 myotubes3; however, it is not known how HERG modulates [Ca2+]i. Indeed, we find that Ltype calcium current is not changed by HERG expression. Thus, to explore this mechanism, we increased [Ca2+]i by depolarization with 100 mM KCl and used Fura2 dyes and immunoblot to reveal that HERG does not alter myotube calcium levels by affecting L-type calcium channels. Instead, using the SERCA blocking agent thapsigargin with our Fura2 assay, we discovered that the HERG-mediated increase in calcium occurs through modulation of intracellular calcium stores4. Therefore, we hypothesized that HERG may be modulating[Ca2+]i by modulation of ryanodine receptor (RyR1) activity. To investigate this, we transduced myotubes in a 96-well plate with either a control or HERG-encoded adenovirus and after 48 hours loaded these with QBT Fura (Molecular Devices; San Jose, CA). At 1 hour post-loading, we treated the myotubes with either ryanodine (90 uM to block RyR1 receptors) or vehicle for 30 minutes. We then treated the cells with caffeine (5 mM) to activate ryanodine receptors and evaluated the [Ca2+]i over time by fluorescence (340 and 380 excitement; 508 nm emission). The 340/380 ratios were determined and normalized to baseline. The ratios were plotted over time, the area under the curve (AUC) was calculated, and these were analyzed by ANOVA with means separated by Tukey's test. Interestingly, in response to caffeine, the significant increase in [Ca2+]i was similar in control (73.3%, p<0.005) and HERGexpressing (71.7%, p<.001) myotubes. However, when the cells were treated with ryanodine to block RyR1, the [Ca2+]i increase was lower in the HERG-expressing (46.4%, p<0.02) relative to control (24.9%, p<0.8) myotubes. The data suggest that the increase in [Ca2+]i in the HERG-expressing cells is, at least in part, a result of RyR1 activation. Because calsequestrin 1 (CaSeq1) is an integral part of RyR1 modulation of [Ca2+]i and was reported mildly downregulated in HERG-expressing myotubes by Next Generation Sequencing, 5 we performed an immunoblot on control and HERGexpressing myotubes (n=8, 4 replicates each HERG and control), in which we detected a full length CaSeq ~63 kD protein along with ~50 kD and ~40 kD CaSeq proteins which appear to be CaSeq1 degradation products. Each protein was decreased in the HERGexpressing myotubes relative to control cells: ~63 kD decreased 47.2%, p<0.001; ~50 kD decreased 44.9%, p<0.01; and ~40 kD decreased 49.8%, p<0.01 (Student's t-test). CaSeq1 is known to function as a calcium buffer in skeletal muscle sarcoplasmic reticulum (SR), storing calcium when the concentration is high. Thus, we suggest that HERG expression produces a decrease in CaSeq protein, which removes this calcium binding protein and increases free calcium in intracellular calcium stores (Figure). Dysregulation of normal calcium buffering is known to contribute to pathologies in both skeletal muscle and heart. This is an exciting finding which merits further exploration. [ABSTRACT FROM AUTHOR]

Published

2023

73. There is no F in APC: Using physiological fluoride-free solutions for high throughput automated patch clamp experiments

Author

Markus Rapedius, Alison Obergrussberger, Edward S. A. Humphries, Stephanie Scholz, Ilka Rinke-Weiss, Tom A. Goetze, Nina Brinkwirth, Maria Giustina Rotordam, Tim Strassmaier, Aaron Randolph, Søren Friis, Aiste Liutkute, Fitzwilliam Seibertz, Niels Voigt, and Niels Fertig

Subjects

automated patch clamp, ion channels, hERG, NaV1.5, physiological solutions, KCa3.1, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Fluoride has been used in the internal recording solution for manual and automated patch clamp experiments for decades because it helps to improve the seal resistance and promotes longer lasting recordings. In manual patch clamp, fluoride has been used to record voltage-gated Na (NaV) channels where seal resistance and access resistance are critical for good voltage control. In automated patch clamp, suction is applied from underneath the patch clamp chip to attract a cell to the hole and obtain a good seal. Since the patch clamp aperture cannot be moved to improve the seal like the patch clamp pipette in manual patch clamp, automated patch clamp manufacturers use internal fluoride to improve the success rate for obtaining GΩ seals. However, internal fluoride can affect voltage-dependence of activation and inactivation, as well as affecting internal second messenger systems and therefore, it is desirable to have the option to perform experiments using physiological, fluoride-free internal solution. We have developed an approach for high throughput fluoride-free recordings on a 384-well based automated patch clamp system with success rates >40% for GΩ seals. We demonstrate this method using hERG expressed in HEK cells, as well as NaV1.5, NaV1.7, and KCa3.1 expressed in CHO cells. We describe the advantages and disadvantages of using fluoride and provide examples of where fluoride can be used, where caution should be exerted and where fluoride-free solutions provide an advantage over fluoride-containing solutions.

Published

2022

74. Multiple mechanisms underlie reduced potassium conductance in the p.T1019PfsX38 variant of hERG

Author

Majid K. Al Salmani, Rezvan Tavakoli, Wajid Zaman, and Ahmed Al Harrasi

Subjects

arrhythmia, hERG, long QT syndrome, potassium channels, Physiology, QP1-981

Abstract

Abstract Long QT syndrome type II (LQT2) is caused by loss‐of‐function mutations in the hERG K+ channel, leading to increased incidence of cardiac arrest and sudden death. Many genetic variants have been reported in the hERG gene with various consequences on channel expression, permeation, and gating. Only a small number of LQT2 causing variants has been characterized to define the underlying pathophysiological causes of the disease. We sought to determine the characteristics of the frameshift variant p.Thr1019ProfsX38 (T1019PfsX38) which affects the C‐terminus of the protein. This mutation was identified in an extended Omani family of LQT2. It replaces the last 140 amino acids of hERG with 37 unique amino acids. T1019 is positioned at a distinguished region of the C‐terminal tail of hERG, as predicted from the deep learning system AlphaFold v2.0. We employed the whole‐cell configuration of the patch‐clamp technique to study wild‐type and mutant channels that were transiently expressed in human embryonic kidney 293 (HEK293) cells. Depolarizing voltages elicited slowly deactivating tail currents that appeared upon repolarization of cells that express either wild‐type‐ or T1019PfsX38‐hERG. There were no differences in the voltage and time dependencies of activation between the two variants. However, the rates of hERG channel deactivation at hyperpolarizing potentials were accelerated by T1019PfsX38. In addition, the voltage dependence of inactivation of T1019PfsX38‐hERG was shifted by 20 mV in the negative direction when compared with wild‐type hERG. The rates of channel inactivation were increased in the mutant channel variant. Next, we employed a step‐ramp protocol to mimic membrane repolarization by the cardiac action potential. The amplitudes of outward currents and their integrals were reduced in the mutant variant when compared with the wild‐type variant during repolarization. Thus, changes in the gating dynamics of hERG by the T1019PfsX38 variant contribute to the pathology seen in affected LQT2 patients.

Published

2022

75. Supporting an integrated QTc risk assessment using the hERG margin distributions for three positive control agents derived from multiple laboratories and on multiple occasions.

Author

Leishman, Derek J., Brimecombe, Jessica, Crumb, William, Hebeisen, Simon, Jenkinson, Steve, Kilfoil, Peter J., Matsukawa, Hiroshi, Melliti, Karim, and Qu, Yusheng

Subjects

*RISK assessment, *BLOOD proteins, *LABORATORIES, *PROTEIN binding, *BEST practices, *RESEARCH personnel

Abstract

Determination of a drug's potency in blocking the hERG channel is an established safety pharmacology study. Best practice guidelines have been published for reliable assessment of hERG potency. In addition, a set of plasma concentration and plasma protein binding fraction data were provided as denominators for margin calculations. The aims of the current analysis were five-fold: provide data allowing creation of consistent denominators for the hERG margin distributions of the key reference agents, explore the variation in hERG margins within and across laboratories, provide a hERG margin to 10 ms QTc prolongation based on several newer studies, provide information to use these analyses for reference purposes, and provide recommended hERG margin 'cut-off' values. The analyses used 12 hERG IC 50 'best practice' data sets (for the 3 reference agents). A group of 5 data sets came from a single laboratory. The other 7 data sets were collected by 6 different laboratories. The denominator exposure distributions were consistent with the ICH E14/S7B Training Materials. The inter-occasion and inter-laboratory variability in hERG IC 50 values were comparable. Inter-drug differences were most important in determining the pooled margin variability. The combined data provided a robust hERG margin reference based on best practice guidelines and consistent exposure denominators. The sensitivity of hERG margin thresholds were consistent with the sensitivity described over the course of the last two decades. The current data provide further insight into the sensitivity of the 30-fold hERG margin 'cut-off' used for two decades. Using similar hERG assessments and these analyses, a future researcher can use a hERG margin threshold to support a negative QTc integrated risk assessment. [ABSTRACT FROM AUTHOR]

Published

2024

76. Macrocyclization strategy for improving candidate profiles in medicinal chemistry.

Author

Darlami, Om, Pun, Rabin, Ahn, Sung-Hoon, Kim, Seok-Ho, and Shin, Dongyun

Subjects

*PHARMACEUTICAL chemistry, *DRUG discovery, *CYCLIC peptides, *X-ray crystallography, *CYCLIC compounds, *MACROCYCLIC compounds

Abstract

Macrocycles are defined as cyclic compounds with 12 or more members. In medicinal chemistry, they are categorized based on their core chemistry into cyclic peptides and macrocycles. Macrocycles are advantageous because of their structural diversity and ability to achieve high affinity and selectivity towards challenging targets that are often not addressable by conventional small molecules. The potential of macrocyclization to optimize drug-like properties while maintaining adequate bioavailability and permeability has been emphasized as a key innovation in medicinal chemistry. This review provides a detailed case study of the application of macrocyclization over the past 5 years, starting from the initial analysis of acyclic active compounds to optimization of the resulting macrocycles for improved efficacy and drug-like properties. Additionally, it illustrates the strategic value of macrocyclization in contemporary drug discovery efforts. [Display omitted] • We summarized macrocyclization strategy from acyclic precursors aimed at improving candidate profile from 2019 to 2023. • We specifically emphasized rationale behind the design strategy of macrocyclization based on X-ray crystallography or molecular modelling. • Improvements or changes of activities or DMPK-Tox profiles of resulting macrocycles were compared with acyclic precursors. [ABSTRACT FROM AUTHOR]

Published

2024

77. Challenges of Predicting Drug-Induced QTc Prolongation in Humans.

Author

Valentin, Jean-Pierre, Hoffmann, Peter, Ortemann-Renon, Catherine, Koerner, John, Pierson, Jennifer, Gintant, Gary, Willard, James, Garnett, Christine, Skinner, Matthew, Vargas, Hugo M, Wisialowski, Todd, and Pugsley, Michael K

Subjects

*DRUG side effects, *ACTION potentials, *VENTRICULAR tachycardia, *HEART beat, *DRUG development

Abstract

The content of this article derives from a Health and Environmental Sciences Institute (HESI) consortium with a focus to improve cardiac safety during drug development. A detailed literature review was conducted to evaluate the concordance between nonclinical repolarization assays and the clinical thorough QT (TQT) study. Food and Drug Administration and HESI developed a joint database of nonclinical and clinical data, and a retrospective analysis of 150 anonymized drug candidates was reviewed to compare the performance of 3 standard nonclinical assays with clinical TQT study findings as well as investigate mechanism(s) potentially responsible for apparent discrepancies identified. The nonclinical assays were functional (I Kr) current block (Human ether-a-go-go related gene), action potential duration, and corrected QT interval in animals (in vivo corrected QT). Although these nonclinical assays demonstrated good specificity for predicting negative clinical QT prolongation, they had relatively poor sensitivity for predicting positive clinical QT prolongation. After review, 28 discordant TQT-positive drugs were identified. This article provides an overview of direct and indirect mechanisms responsible for QT prolongation and theoretical reasons for lack of concordance between clinical TQT studies and nonclinical assays. We examine 6 specific and discordant TQT-positive drugs as case examples. These were derived from the unique HESI/Food and Drug Administration database. We would like to emphasize some reasons for discordant data including, insufficient or inadequate nonclinical data, effects of the drug on other cardiac ion channels, and indirect and/or nonelectrophysiological effects of drugs, including altered heart rate. We also outline best practices that were developed based upon our evaluation. [ABSTRACT FROM AUTHOR]

Published

2022

78. Identification and New Indication of Melanin-Concentrating Hormone Receptor 1 (MCHR1) Antagonist Derived from Machine Learning and Transcriptome-Based Drug Repositioning Approaches.

Author

Lim, Gyutae, You, Ka Young, Lee, Jeong Hyun, Jeon, Moon Kook, Lee, Byung Ho, Ryu, Jae Yong, and Oh, Kwang-Seok

Subjects

*HORMONE receptors, *DRUG repositioning, *LIPOPROTEIN receptors, *APPETITE depressants, *NON-alcoholic fatty liver disease, *MACHINE learning

Abstract

Melanin-concentrating hormone receptor 1 (MCHR1) has been a target for appetite suppressants, which are helpful in treating obesity. However, it is challenging to develop an MCHR1 antagonist because its binding site is similar to that of the human Ether-à-go-go-Related Gene (hERG) channel, whose inhibition may cause cardiotoxicity. Most drugs developed as MCHR1 antagonists have failed in clinical development due to cardiotoxicity caused by hERG inhibition. Machine learning-based prediction models can overcome these difficulties and provide new opportunities for drug discovery. In this study, we identified KRX-104130 with potent MCHR1 antagonistic activity and no cardiotoxicity through virtual screening using two MCHR1 binding affinity prediction models and an hERG-induced cardiotoxicity prediction model. In addition, we explored other possibilities for expanding the new indications for KRX-104130 using a transcriptome-based drug repositioning approach. KRX-104130 increased the expression of low-density lipoprotein receptor (LDLR), which induced cholesterol reduction in the gene expression analysis. This was confirmed by comparison with gene expression in a nonalcoholic steatohepatitis (NASH) patient group. In a NASH mouse model, the administration of KRX-104130 showed a protective effect by reducing hepatic lipid accumulation, liver injury, and histopathological changes, indicating a promising prospect for the therapeutic effect of NASH as a new indication for MCHR1 antagonists. [ABSTRACT FROM AUTHOR]

Published

2022

79. Identification through action potential clamp of proarrhythmic consequences of the short QT syndrome T618I hERG 'hotspot' mutation.

Author

Du, Chunyun, Zhang, Henggui, Harmer, Stephen C., and Hancox, Jules C.

Subjects

*BRUGADA syndrome, *ARRHYTHMIA, *VENTRICULAR fibrillation, *GENETIC mutation, *POTASSIUM channels, *ATRIAL fibrillation, *SUDDEN death

Abstract

The T618I KCNH2 -encoded hERG mutation is the most frequently observed mutation in genotyped cases of the congenital short QT syndrome (SQTS), a cardiac condition associated with ventricular fibrillation and sudden death. Most T618I hERG carriers exhibit a pronounced U wave on the electrocardiogram and appear vulnerable to ventricular, but not atrial fibrillation (AF). The basis for these effects is unclear. This study used the action potential (AP) voltage clamp technique to determine effects of the T618I mutation on hERG current (I hERG) elicited by APs from different cardiac regions. Whole-cell patch-clamp recordings were made at 37 °C of I hERG from hERG-transfected HEK-293 cells. Maximal I hERG during a ventricular AP command was increased ∼4-fold for T618I I hERG and occurred much earlier during AP repolarization. The mutation also increased peak repolarizing currents elicited by Purkinje fibre (PF) APs. Maximal wild-type (WT) I hERG current during the PF waveform was 87.2 ± 4.5% of maximal ventricular repolarizing current whilst for the T618I mutant, the comparable value was 47.7 ± 2.7%. Thus, the T618I mutation exacerbated differences in repolarizing I hERG between PF and ventricular APs; this could contribute to heterogeneity of ventricular-PF repolarization and consequently to the U waves seen in T618I carriers. The comparatively shorter duration and lack of pronounced plateau of the atrial AP led to a smaller effect of the T618I mutation during the atrial AP, which may help account for the lack of reported AF in T618I carriers. Use of a paired ventricular AP protocol revealed an alteration to protective I hERG transients that affect susceptibility to premature excitation late in AP repolarization/early in diastole. These observations may help explain altered arrhythmia susceptibility in this form of the SQTS. • T618I is a 'hotspot' hERG potassium channel mutation in the congenital short QT syndrome. • Differences in hERG current during ventricular and Purkinje fibre action potentials are exacerbated by the T618I mutation. • T618I has more modest effects on current during atrial action potentials. • T618I modifies the protective response of hERG to premature ventricular excitation. • These alterations to hERG function help explain ECG changes reported in T618I-hERG carriers. [ABSTRACT FROM AUTHOR]

Published

2022

80. A Comprehensive Evaluation of Sdox, a Promising H2S-Releasing Doxorubicin for the Treatment of Chemoresistant Tumors.

Author

Alov, Petko, Al Sharif, Merilin, Aluani, Denitsa, Chegaev, Konstantin, Dinic, Jelena, Divac Rankov, Aleksandra, Fernandes, Miguel X., Fusi, Fabio, García-Sosa, Alfonso T., Juvonen, Risto, Kondeva-Burdina, Magdalena, Padrón, José M., Pajeva, Ilza, Pencheva, Tania, Puerta, Adrián, Raunio, Hannu, Riganti, Chiara, Tsakovska, Ivanka, Tzankova, Virginia, and Yordanov, Yordan

Subjects

TUMOR treatment, HYDROGEN sulfide, ANTHRACYCLINES, DOXORUBICIN, CYTOCHROME P-450 CYP3A, CYTOCHROME P-450, LIPOPHILICITY

Abstract

Sdox is a hydrogen sulfide (H2S)-releasing doxorubicin effective in P-glycoprotein-overexpressing/doxorubicin-resistant tumor models and not cytotoxic, as the parental drug, in H9c2 cardiomyocytes. The aim of this study was the assessment of Sdox drug-like features and its absorption, distribution, metabolism, and excretion (ADME)/toxicity properties, by a multi- and transdisciplinary in silico , in vitro , and in vivo approach. Doxorubicin was used as the reference compound. The in silico profiling suggested that Sdox possesses higher lipophilicity and lower solubility compared to doxorubicin, and the off-targets prediction revealed relevant differences between Dox and Sdox towards several cancer targets, suggesting different toxicological profiles. In vitro data showed that Sdox is a substrate with lower affinity for P-glycoprotein, less hepatotoxic, and causes less oxidative damage than doxorubicin. Both anthracyclines inhibited CYP3A4, but not hERG currents. Unlike doxorubicin, the percentage of zebrafish live embryos at 72 hpf was not affected by Sdox treatment. In conclusion, these findings demonstrate that Sdox displays a more favorable drug-like ADME/toxicity profile than doxorubicin, different selectivity towards cancer targets, along with a greater preclinical efficacy in resistant tumors. Therefore, Sdox represents a prototype of innovative anthracyclines, worthy of further investigations in clinical settings. [ABSTRACT FROM AUTHOR]

Published

2022

81. Open-Access Activity Prediction Tools for Natural Products. Case Study: hERG Blockers

Author

Mayr, Fabian, Vieider, Christian, Temml, Veronika, Stuppner, Hermann, Schuster, Daniela, Kinghorn, A. Douglas, Series Editor, Falk, Heinz, Series Editor, Gibbons, Simon, Series Editor, Kobayashi, Jun'ichi, Series Editor, Asakawa, Yoshinori, Series Editor, Liu, Ji-Kai, Series Editor, Appendino, Giovanni, Advisory Editor, Berlinck, Roberto G. S., Advisory Editor, Dirsch, Verena, Advisory Editor, Ludwiczuk, Agnieszka, Advisory Editor, Mata, Rachel, Advisory Editor, Oberlies, Nicholas H., Advisory Editor, Tasdemir, Deniz, Advisory Editor, Trauner, Dirk, Advisory Editor, Viljoen, Alvaro, Advisory Editor, and Ye, Yang, Advisory Editor

Published

2019

82. Exploiting the Diversity of Ion Channels: Modulation of Ion Channels for Therapeutic Indications

Author

Liu, Yani, Wang, KeWei, Barrett, James E., Editor-in-Chief, Flockerzi, Veit, Editorial Board Member, Frohman, Michael A., Editorial Board Member, Geppetti, Pierangelo, Editorial Board Member, Hofmann, Franz B., Editorial Board Member, Michel, Martin C., Editorial Board Member, Page, Clive P., Editorial Board Member, Rosenthal, Walter, Editorial Board Member, and Wang, KeWei, Editorial Board Member

Published

2019

83. Approaching Pharmacological Space: Events and Components.

Author

Vistoli G, Talarico C, Vittorio S, Lunghini F, Mazzolari A, Beccari A, and Pedretti A

Subjects

Ligands, Humans, Protein Binding, Proteins chemistry, Proteins metabolism, Drug Discovery methods, Binding Sites, Molecular Docking Simulation

Abstract

The pharmacological space comprises all the dynamic events that determine the bioactivity (and/or the metabolism and toxicity) of a given ligand. The pharmacological space accounts for the structural flexibility and property variability of the two interacting molecules as well as for the mutual adaptability characterizing their molecular recognition process. The dynamic behavior of all these events can be described by a set of possible states (e.g., conformations, binding modes, isomeric forms) that the simulated systems can assume. For each monitored state, a set of state-dependent ligand- and structure-based descriptors can be calculated. Instead of considering only the most probable state (as routinely done), the pharmacological space proposes to consider all the monitored states. For each state-dependent descriptor, the corresponding space can be evaluated by calculating various dynamic parameters such as mean and range values.The reviewed examples emphasize that the pharmacological space can find fruitful applications in structure-based virtual screening as well as in toxicity prediction. In detail, in all reported examples, the inclusion of the pharmacological space parameters enhances the resulting performances. Beneficial effects are obtained by combining both different binding modes to account for ligand mobility and different target structures to account for protein flexibility/adaptability.The proposed computational workflow that combines docking simulations and rescoring analyses to enrich the arsenal of docking-based descriptors revealed a general applicability regardless of the considered target and utilized docking engine. Finally, the EFO approach that generates consensus models by linearly combining various descriptors yielded highly performing models in all discussed virtual screening campaigns., (© 2025. The Author(s), under exclusive license to Springer Science+Business Media, LLC, part of Springer Nature.)

Published

2025

84. A Comprehensive Evaluation of Sdox, a Promising H2S-Releasing Doxorubicin for the Treatment of Chemoresistant Tumors

Author

Petko Alov, Merilin Al Sharif, Denitsa Aluani, Konstantin Chegaev, Jelena Dinic, Aleksandra Divac Rankov, Miguel X. Fernandes, Fabio Fusi, Alfonso T. García-Sosa, Risto Juvonen, Magdalena Kondeva-Burdina, José M. Padrón, Ilza Pajeva, Tania Pencheva, Adrián Puerta, Hannu Raunio, Chiara Riganti, Ivanka Tsakovska, Virginia Tzankova, Yordan Yordanov, and Simona Saponara

Subjects

cytochrome P450, doxorubicin, hepatotoxicity, hERG, in silico profiling, off-targets, Therapeutics. Pharmacology, RM1-950

Abstract

Sdox is a hydrogen sulfide (H2S)-releasing doxorubicin effective in P-glycoprotein-overexpressing/doxorubicin-resistant tumor models and not cytotoxic, as the parental drug, in H9c2 cardiomyocytes. The aim of this study was the assessment of Sdox drug-like features and its absorption, distribution, metabolism, and excretion (ADME)/toxicity properties, by a multi- and transdisciplinary in silico, in vitro, and in vivo approach. Doxorubicin was used as the reference compound. The in silico profiling suggested that Sdox possesses higher lipophilicity and lower solubility compared to doxorubicin, and the off-targets prediction revealed relevant differences between Dox and Sdox towards several cancer targets, suggesting different toxicological profiles. In vitro data showed that Sdox is a substrate with lower affinity for P-glycoprotein, less hepatotoxic, and causes less oxidative damage than doxorubicin. Both anthracyclines inhibited CYP3A4, but not hERG currents. Unlike doxorubicin, the percentage of zebrafish live embryos at 72 hpf was not affected by Sdox treatment. In conclusion, these findings demonstrate that Sdox displays a more favorable drug-like ADME/toxicity profile than doxorubicin, different selectivity towards cancer targets, along with a greater preclinical efficacy in resistant tumors. Therefore, Sdox represents a prototype of innovative anthracyclines, worthy of further investigations in clinical settings.

Published

2022

85. Inhibition of hERG by ESEE suppresses the progression of colorectal cancer.

Author

Wan J, Xu H, Ju J, Chen Y, Zhang H, Qi L, Zhang Y, Du Z, and Zhao X

Abstract

Colorectal cancer (CRC) is one of the most common malignant cancers. Emodin is a lipophilic anthraquinone commonly found in medicinal herbs and known for its antitumor properties. However, its clinical utility has been hampered by low druggability. We designed and synthesized a new compound named Emodin succinimidyl ethyl ester (ESEE), which improves the bioavailability and preserves the original pharmacological effects of Emodin. In vitro, we have confirmed that ESEE induces apoptosis in colon cancer cells, suppresses cell proliferation, migration, and invasion, and inhibits the growth of subcutaneous transplantation tumors associated with colon cancer. And, in vivo, ESEE robustly inhibited tumor growth. Human Ether-a-go-go Related Gene (hERG) is aberrantly expressed in various cancer cells, where they play an important role in cancer progression. Focal adhesion kinase (FAK) is a tyrosine kinase overexpressed in cancer cells and plays an important role in the progression of tumors to a malignant phenotype. Mechanistically, the anti-CRC properties of ESEE are exerted through direct binding with hERG, which impedes the FAK/PI3K/AKT signaling axis-dependent apoptotic cascade., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024. Published by Elsevier Inc.)

Published

2024

86. Metabolic and electrolyte abnormalities as risk factors in drug-induced long QT syndrome.

Author

TeBay, Clifford, Hill, Adam P., and Windley, Monique J.

Abstract

Drug-induced long QT syndrome (diLQTS) is the phenomenon by which the administration of drugs causes prolongation of cardiac repolarisation and leads to an increased risk of the ventricular tachycardia known as torsades de pointes (TdP). In most cases of diLQTS, the primary molecular target is the human ether-à-go-go-related gene protein (hERG) potassium channel, which carries the rapid delayed rectifier current (IKr) in the heart. However, the proarrhythmic risk associated with drugs that block hERG can be modified in patients by a range of environmental- and disease-related factors, such as febrile temperatures, alterations in pH, dyselectrolytaemias such as hypokalaemia and hypomagnesemia and coadministration with other drugs. In this review, we will discuss the clinical occurrence of drug-induced LQTS in the context of these modifying factors as well as the mechanisms by which they contribute to altered hERG potency and proarrhythmic risk. [ABSTRACT FROM AUTHOR]

Published

2022

87. Overcoming challenges of HERG potassium channel liability through rational design: Eag1 inhibitors for cancer treatment.

Author

Toplak, Žan, Hendrickx, Louise A., Abdelaziz, Reham, Shi, Xiaoyi, Peigneur, Steve, Tomašič, Tihomir, Tytgat, Jan, Peterlin‐Mašič, Lucija, and Pardo, Luis A.

Subjects

POTASSIUM channels, DRUG design, ION channels, POTASSIUM antagonists, CANCER treatment, VOLTAGE-gated ion channels, TUMOR growth

Abstract

Two decades of research have proven the relevance of ion channel expression for tumor progression in virtually every indication, and it has become clear that inhibition of specific ion channels will eventually become part of the oncology therapeutic arsenal. However, ion channels play relevant roles in all aspects of physiology, and specificity for the tumor tissue remains a challenge to avoid undesired effects. Eag1 (KV10.1) is a voltage‐gated potassium channel whose expression is very restricted in healthy tissues outside of the brain, while it is overexpressed in 70% of human tumors. Inhibition of Eag1 reduces tumor growth, but the search for potent inhibitors for tumor therapy suffers from the structural similarities with the cardiac HERG channel, a major off‐target. Existing inhibitors show low specificity between the two channels, and screenings for Eag1 binders are prone to enrichment in compounds that also bind HERG. Rational drug design requires knowledge of the structure of the target and the understanding of structure–function relationships. Recent studies have shown subtle structural differences between Eag1 and HERG channels with profound functional impact. Thus, although both targets' structure is likely too similar to identify leads that exclusively bind to one of the channels, the structural information combined with the new knowledge of the functional relevance of particular residues or areas suggests the possibility of selective targeting of Eag1 in cancer therapies. Further development of selective Eag1 inhibitors can lead to first‐in‐class compounds for the treatment of different cancers. [ABSTRACT FROM AUTHOR]

Published

2022

88. The Linkage Phase of the Polymorphism KCNH2-K897T Influences the Electrophysiological Phenotype in hiPSC Models of LQT2.

Author

van den Brink, Lettine, Brandão, Karina O., Yiangou, Loukia, Blanch-Asensio, Albert, Mol, Mervyn P. H., Mummery, Christine L., Verkerk, Arie O., and Davis, Richard P.

Subjects

PHENOTYPES, INDUCED pluripotent stem cells, GENETIC variation, GENETIC models, LONG QT syndrome, ARRHYTHMIA, BRUGADA syndrome

Abstract

While rare mutations in ion channel genes are primarily responsible for inherited cardiac arrhythmias, common genetic variants are also an important contributor to the clinical heterogeneity observed among mutation carriers. The common single nucleotide polymorphism (SNP) KCNH2-K897T is associated with QT interval duration, but its influence on the disease phenotype in patients with long QT syndrome type 2 (LQT2) remains unclear. Human induced pluripotent stem cells (hiPSCs), coupled with advances in gene editing technologies, are proving an invaluable tool for modeling cardiac genetic diseases and identifying variants responsible for variability in disease expressivity. In this study, we have used isogenic hiPSC-derived cardiomyocytes (hiPSC-CMs) to establish the functional consequences of having the KCNH2-K897T SNP in cis - or trans -orientation with LQT2-causing missense variants either within the pore-loop domain (KCNH2A561T/WT) or tail region (KCNH2N996I/WT) of the potassium ion channel, human ether-a-go-go-related gene (hERG). When KCNH2-K897T was on the same allele (cis) as the primary mutation, the hERG channel in hiPSC-CMs exhibited faster activation and deactivation kinetics compared to their trans -oriented counterparts. Consistent with this, hiPSC-CMs with KCNH2-K897T in cis orientation had longer action and field potential durations. Furthermore, there was an increased occurrence of arrhythmic events upon pharmacological blocking of hERG. Collectively, these results indicate that the common polymorphism KCNH2-K897T differs in its influence on LQT2-causing KCNH2 mutations depending on whether it is present in cis or trans. This study corroborates hiPSC-CMs as a powerful platform to investigate the modifying effects of common genetic variants on inherited cardiac arrhythmias and aids in unraveling their contribution to the variable expressivity of these diseases. [ABSTRACT FROM AUTHOR]

Published

2021

89. Endocannabinoid Degradation Enzyme Inhibitors as Potential Antipsychotics: A Medicinal Chemistry Perspective

Author

Giuseppe Felice Mangiatordi, Maria Maddalena Cavalluzzi, Pietro Delre, Giuseppe Lamanna, Maria Cristina Lumuscio, Michele Saviano, Jean-Pierre Majoral, Serge Mignani, Andrea Duranti, and Giovanni Lentini

Subjects

endocannabinoid system, FAAH inhibitors, MGL inhibitors, repositioning, drug-likeness, hERG, Biology (General), QH301-705.5

Abstract

The endocannabinoid system (ECS) plays a very important role in numerous physiological and pharmacological processes, such as those related to the central nervous system (CNS), including learning, memory, emotional processing, as well pain control, inflammatory and immune response, and as a biomarker in certain psychiatric disorders. Unfortunately, the half-life of the natural ligands responsible for these effects is very short. This perspective describes the potential role of the inhibitors of the enzymes fatty acid amide hydrolase (FAAH) and monoacylglycerol lipase (MGL), which are mainly responsible for the degradation of endogenous ligands in psychic disorders and related pathologies. The examination was carried out considering both the impact that the classical exogenous ligands such as Δ9-tetrahydrocannabinol (THC) and (−)-trans-cannabidiol (CBD) have on the ECS and through an analysis focused on the possibility of predicting the potential toxicity of the inhibitors before they are subjected to clinical studies. In particular, cardiotoxicity (hERG liability), probably the worst early adverse reaction studied during clinical studies focused on acute toxicity, was predicted, and some of the most used and robust metrics available were considered to select which of the analyzed compounds could be repositioned as possible oral antipsychotics.

Published

2023

90. Novel Bacterial Topoisomerase inhibitors (NBTIs) – A comprehensive review

Author

Jigar Desai, Sachchidanand S, Sanjay Kumar, and Rajiv Sharma

Subjects

DNA gyrase, hERG, MIC, NBTI, Topoisomerase, Pharmacy and materia medica, RS1-441, Other systems of medicine, RZ201-999

Abstract

Bacterial DNA gyrase and topoisomerase IV inhibition has emerged as a promising strategy for the cure of infections caused by antibiotic-resistant bacteria. Small molecule antibacterials inhibiting bacterial topoisomerases have been previously exploited by the successful fluoroquinolone class. The Novel Bacterial Topoisomerase Inhibitors (NBTIs) bind to a different site to that of the fluoroquinolones with novel mechanism of action to evade the existing target-mediated bacterial resistance associated with fluoroquinolones. This review comprehensively summarizes various efforts with respect to structural modifications of inhibitors and their impact on their general physicochemical and biological properties.

Published

2021

91. The proteostasis interactomes of trafficking-deficient variants of the voltage-gated potassium channel K V 11.1 associated with long QT syndrome.

Author

Egly CL, Barny LA, Do T, McDonald EF, Knollmann BC, and Plate L

Subjects

Humans, HEK293 Cells, Ether-A-Go-Go Potassium Channels metabolism, Ether-A-Go-Go Potassium Channels genetics, ERG1 Potassium Channel metabolism, ERG1 Potassium Channel genetics, Animals, Long QT Syndrome metabolism, Long QT Syndrome genetics, Proteostasis, Protein Transport

Abstract

The voltage-gated potassium ion channel K V 11.1 plays a critical role in cardiac repolarization. Genetic variants that render Kv11.1 dysfunctional cause long QT syndrome (LQTS), which is associated with fatal arrhythmias. Approximately 90% of LQTS-associated variants cause intracellular protein transport (trafficking) dysfunction, which pharmacological chaperones like E-4031 can rescue. Protein folding and trafficking decisions are regulated by chaperones, protein quality control factors, and trafficking machinery comprising the cellular proteostasis network. Here, we test whether trafficking dysfunction is associated with alterations in the proteostasis network of pathogenic Kv11.1 variants and whether pharmacological chaperones can normalize the proteostasis network of responsive variants. We used affinity-purification coupled with tandem mass tag-based quantitative mass spectrometry to assess protein interaction changes of WT K V 11.1 or trafficking-deficient channel variants in the presence or absence of E-4031. We identified 572 core K V 11.1 protein interactors. Trafficking-deficient variants K V 11.1-G601S and K V 11.1-G601S-G965 ∗ had significantly increased interactions with proteins responsible for folding, trafficking, and degradation compared to WT. We confirmed previous findings that the proteasome is critical for K V 11.1 degradation. Our report provides the first comprehensive characterization of protein quality control mechanisms of K V 11.1. We find extensive interactome remodeling associated with trafficking-deficient K V 11.1 variants and with pharmacological chaperone rescue of K V 11.1 cell surface expression. The identified protein interactions could be targeted therapeutically to improve K V 11.1 trafficking and treat LQTS., Competing Interests: Conflict of interest The authors declare that they have no conflicts of interest with the contents of this article., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

92. Structural Modeling of Voltage-Gated Ion Channel Interactions with Drugs Using Rosetta

Author

Cortez, Aiyana Margaret Emigh

Subjects

Biophysics, arrhythmia, hERG, ion channel, ligand docking, professional development, structural modeling

Abstract

Many different types of drugs–from antibiotics to blood pressure medication–tend to interfere with the body’s ability to control heart rhythm by disrupting the proteins in heart cells that control the movement of charged atoms (ions) across the cell membrane known as voltage-gated ion channels (VGICs). These drugs can cause dangerous arrhythmias (abnormal heart rhythms) that can increase risk for heart failure, stroke, or death. Early and efficient assessment of cardiotoxicity is essential to the drug development process and to reducing drug development costs. Current methods for assessing safety are sensitive but not specific and can often result in false identification of unsafe treatments and the failure of potentially life-saving treatments to reach the public. Structural characterization of VGICs and their modulating interactions are necessary for rational design of safe therapeutics. Human Ether-a-go-go-Related Gene (hERG) encodes a potassium-selective voltage-gated ion channel (KV11.1) essential for normal electrical activity in the heart. Genetic hERG mutations and blockage of the channel pore by drugs can cause long QT syndrome (LQTS). LQTS predisposes individuals to arrhythmia and puts them at risk for stroke or sudden cardiac arrest. A major problem in antiarrhythmic drug therapies is the proclivity for these drugs to promote fatal arrhythmias through hERG channel blockade. However, not all hERG channel blocking drugs are pro-arrhythmic, and their differential affinities to discrete channel conformational states and/or their state stability modulations have been suggested to contribute to arrhythmogenicity. Voltage-gated calcium (CaV) channels play a key role in muscular contraction, neuronal excitation, gene expression regulation, and release of hormones or neurotransmitters. Dysregulation of CaV channels and the associated intracellular calcium homeostasis have been associated with various types of cardiac and neurological disorders. Found throughout the body, often as part of large complexes and/or clusters, the L-type CaV1.2 channel mediates the influx of Ca2+ into the cell in response to membrane depolarization. Mutations or blockage of the channel by drug molecules leading to altered functions of human CaV1.2 have been linked to cardiac arrhythmias, autism, bipolar disorder, and immunodeficiency. Many CaV channel blockers targeting the alpha-1-subunit of CaV1.2 are used to treat hypertension, coronary artery disease and other cardiovascular medical conditions. However, only a few drugs have been approved for clinical use due to severe side effects (including cardiotoxicity) or limited efficacy.In this study, Rosetta electron density refinement and homology modeling protocols were used to build voltage sensing and pore domain structural models of wild-type hERG channel in open and closed states, open-state hERG mutant variants (Y652A, F656A, and Y652A/F656A double mutant) based on cryo-electron microscopy (cryo-EM) structures of hERG (PDBID: 5VA2) and EAG1 (PDBID: 5K7L) channels as well as open- and closed-state models of the wild-type CaV1.2 alpha-1-subunit using cryo-EM CaV1.1 (PDBID: 5GJV), and NaV1.4 (PDB ID: 6AGF) structures, respectively. The hERG channel models were developed as protein targets for Rosetta-based molecular docking studies of charged and neutral forms of amiodarone, nifekalant, dofetilide, d- and l-sotalol, flecainide, and moxifloxacin–a diverse set of pharmaceuticals chosen based on their different arrhythmogenic potentials and abilities to facilitate hERG current. The CaV1.2 models were used as targets for Rosetta docking studies with verapamil and amlodipine– representatives of two different calcium channel blocking classes: phenylalkylamines and dihydropyridines, respectively. We present here the results of our docking studies that provide structural insights into the molecular and state-dependent drug interactions with hERG and CaV1.2 channels that play a key role in differentiating safe and harmful ion channel blockers.Key Findings:1. Pattern of hERG-drug interactions with the hydrophobic pocket is consistent with experimental data suggesting facilitating drugs may act as a wedge to bias hERG channel equilibrium towards the open state and increase hERG current amplitude in response to low-voltage depolarization.2. Open-state WT hERG interface scores are lower than, or similar to, Y652A mutants suggesting that these poses are relevant for amiodarone, nifekalant, flecainide, moxifloxacin, d-sotalol, and dofetilide, based on comparison to existing experimental data. 3. Open-state WT hERG interface scores are not lower than the F656A mutants for nifekalant, neutral flecainide, neutral moxifloxacin, d-sotalol, l-sotalol, and dofetilide, suggesting limitations of our study using only two conformational states or limitations of Rosetta to model allosteric contributions of F656. 4. Percentage of poses remaining within the closed-state hERG channels suggest that closed channels can accommodate known trapped drugs (nifekalant, flecainide, d/l-sotalol, and dofetilide), but not amiodarone or moxifloxacin (non-trapped drugs). 5. Amlodipine and verapamil docked to rCaV1.2 models in open and closed states recapitulated known binding orientations and similar positioning within pore but did not reproduce known binding determinants necessitating revision of model development to include additional structural densities and increasing search radius in docking protocol in future studies.

Published

2022

93. Long QT syndrome type 2: mechanism-based therapies.

Author

Cox, Kofi Oliver and Wang, Brian Xiangzhi

Abstract

Long QT syndrome type 2 is a life-threatening disorder of cardiac electrophysiology. It can lead to sudden cardiac death as a result of QT prolongation and can remain undetected until it presents clinically in the form of life-threatening cardiac arrythmias. Current treatment relies on symptom management largely through the use of β-adrenergic blockade and presently no mechanism-based therapies exist to treat the dysfunction in the hERG channels responsible for the rapid delayed rectifier K+ current which is the pathological source of long QT syndrome type 2. We review the pathophysiology, diagnosis and current management of this life-threatening condition and also analyze some promising potential mechanism-based therapies. Long QT syndrome is a condition which is characterized by an abnormally lengthened time period of electrical activity in the heart. This abnormality can result in the initiation of heart rhythms which can cause the patient to lose consciousness or cause the patient to enter a heart rhythm which is not conducive to life resulting in sudden cardiac death. In this article we look more closely at a subtype of this disease known as long QT syndrome type 2. We look at how this disease can cause sudden cardiac death, how it is currently managed and how future treatments may be able to work at a genetic and cellular level to reverse the disease-causing mechanisms behind this life-threatening syndrome. [ABSTRACT FROM AUTHOR]

Published

2021

94. MOLECULAR IODINE CATALYZED SOLVENT FREE ONE POT SYNTHESIS, CHARACTERIZATION, INSILICO ADME, hERG ANALYSIS, MOLECULAR DOCKING STUDIES AND DFT ANALYSIS OF 2- SUBSTITUTED 4,5-DIPHENYL-1H-IMIDAZOLE DERIVATIVES.

Author

K., Pruthviraj, T. N., Lohith, M., Yeshwanth, G. H., Usha, H. V., Vanajakshi, K. B., Venugopal, G., Krishnaswamy, G., Shivaraja, Zohra, Fathima, M. A., Sridhar, and S., Sreenivasa

Subjects

*MOLECULAR docking, *IMIDAZOLES, *DIPHENYL

Abstract

In the present investigation, a series of 2-substituted 4,5-Diphenyl-1H-imidazoles (3a-f) were prepared via one pot Debus-Radziszwski multicomponent condensation reaction using molecular iodine as a catalyst. Synthesis involves one pot reaction of benzil and substituted aromatic aldehydes (2a-e) in the presence of ammonium acetate and molecular iodine as catalyst under the solvent free grinding technique. The structures of the compounds were established based on multi nuclear NMR (¹H &13C) spectral data and mass spectrometry. These compounds were subjected to in- silico ADMETox evaluation, hERG analysis, and molecular docking studies to evaluate their potency as antibacterial, antifungal, anti-inflammatory, and antimycobacterial. Molecular physicochemical properties were analyzed using density functional theory (DFT), molecular electrostatic potential (MEP) studies and reduced density gradient analysis. [ABSTRACT FROM AUTHOR]

Published

2021

95. Update on ICH E14/S7B Cardiac Safety Regulations: The Expanded Role of Preclinical Assays and the "Double‐Negative" Scenario.

Subjects

*SAFETY regulations, *DRUG development, *DATA integration, *DRUG design, *WEBINARS

Abstract

For nearly 2 decades, regulators have adopted a harmonized approach to drug development, which has succeeded in bringing new pharmaceuticals to market without significant cardiac liability. Ushered in by technological advancements and better understanding of cellular electrophysiology, the initial paradigm detailed in the 2005 International Conference for Harmonization E14 and S7B documents has undergone evolutionary changes designed to streamline drug development and improve regulatory decision‐making and product labeling. The intent of this review is to summarize the new US Food and Drug Administration (FDA) Question and Answer update from August 2020 and key messaging from a subsequent FDA webinar describing best practices for preclinical and clinical data integration into a QT risk prediction model. [ABSTRACT FROM AUTHOR]

Published

2021

96. Coupling the Cardiac Voltage-Gated Sodium Channel to Channelrhodopsin-2 Generates Novel Optical Switches for Action Potential Studies

Author

Christian vom Dahl, Christoph Emanuel Müller, Xhevat Berisha, Georg Nagel, and Thomas Zimmer

Subjects

optogenetics, channelrhodopsin, voltage-gated Na+ channel, action potential, delayed rectifier potassium channel, hERG, Chemical technology, TP1-1185, Chemical engineering, TP155-156

Abstract

Voltage-gated sodium (Na+) channels respond to short membrane depolarization with conformational changes leading to pore opening, Na+ influx, and action potential (AP) upstroke. In the present study, we coupled channelrhodopsin-2 (ChR2), the key ion channel in optogenetics, directly to the cardiac voltage-gated Na+ channel (Nav1.5). Fusion constructs were expressed in Xenopus laevis oocytes, and electrophysiological recordings were performed by the two-microelectrode technique. Heteromeric channels retained both typical Nav1.5 kinetics and light-sensitive ChR2 properties. Switching to the current-clamp mode and applying short blue-light pulses resulted either in subthreshold depolarization or in a rapid change of membrane polarity typically seen in APs of excitable cells. To study the effect of individual K+ channels on the AP shape, we co-expressed either Kv1.2 or hERG with one of the Nav1.5-ChR2 fusions. As expected, both delayed rectifier K+ channels shortened AP duration significantly. Kv1.2 currents remarkably accelerated initial repolarization, whereas hERG channel activity efficiently restored the resting membrane potential. Finally, we investigated the effect of the LQT3 deletion mutant ΔKPQ on the AP shape and noticed an extremely prolonged AP duration that was directly correlated to the size of the non-inactivating Na+ current fraction. In conclusion, coupling of ChR2 to a voltage-gated Na+ channel generates optical switches that are useful for studying the effect of individual ion channels on the AP shape. Moreover, our novel optogenetic approach provides the potential for an application in pharmacology and optogenetic tissue-engineering.

Published

2022

97. New Diarylamine KV10.1 Inhibitors and Their Anticancer Potential

Author

Špela Gubič, Žan Toplak, Xiaoyi Shi, Jaka Dernovšek, Louise Antonia Hendrickx, Ernesto Lopes Pinheiro-Junior, Steve Peigneur, Jan Tytgat, Luis A. Pardo, Lucija Peterlin Mašič, and Tihomir Tomašič

Subjects

KV10.1, ion channels, hERG, SAR, antiproliferative activity, Pharmacy and materia medica, RS1-441

Abstract

Expression of the voltage-gated potassium channel KV10.1 (Eag1) has been detected in over 70% of human cancers, making the channel a promising new target for new anticancer drug discovery. A new structural class of KV10.1 inhibitors was prepared by structural optimisation and exploration of the structure–activity relationship of the previously published hit compound ZVS-08 (1) and its optimised analogue 2. The potency and selectivity of the new inhibitors between KV10.1 and hERG were investigated using whole-cell patch-clamp experiments. We obtained two new optimised KV10.1 inhibitors, 17a and 18b, with improved nanomolar IC50 values of 568 nM and 214 nM, respectively. Compound 17a exhibited better ratio between IC50 values for hEAG1 and hERG than previously published diarylamine inhibitors. Compounds 17a and 18b moderately inhibited the growth of the KV10.1-expressing cell line MCF-7 in two independent assays. In addition, 17a and 18b also inhibited the growth of hERG-expressing Panc-1 cells with higher potency compared with MCF-7 cells. The main obstacle for newly developed diarylamine KV10.1 inhibitors remains the selectivity toward the hERG channel, which needs to be addressed with targeted drug design strategies in the future.

Published

2022

98. Huffing and twist: Fatal Torsade de pointes associated with Tetrafluoroethane Inhalation and amphetamine use

Author

Joseph Burke, Mark C. P. Haigney, Morteza Farasat, Philip S. Mehler, and Mori J. Krantz

Subjects

hERG, huffing, Ikr, sudden cardiac death, torsade de pointes, Medicine, Medicine (General), R5-920

Abstract

Abstract Many volatile chemicals inhaled for a recreational high have a chemical structure similar to chloroform and may lead to Ikr blockade and subsequent torsades de pointes. This is one potential mechanism of action for huffing‐associated sudden death.

Published

2021

99. Huffing and twist: Fatal Torsade de pointes associated with Tetrafluoroethane Inhalation and amphetamine use.

Author

Burke, Joseph, Haigney, Mark C. P., Farasat, Morteza, Mehler, Philip S., and Krantz, Mori J.

Subjects

*VENTRICULAR tachycardia, *SUDDEN death, *AMPHETAMINES, *CARDIAC arrest, *CHEMICAL structure

Abstract

Many volatile chemicals inhaled for a recreational high have a chemical structure similar to chloroform and may lead to Ikr blockade and subsequent torsades de pointes. This is one potential mechanism of action for huffing-associated sudden death. [ABSTRACT FROM AUTHOR]

Published

2021

100. Pharmacological corrections of the mutant hERG channels by posaconazole.

Author

Luo, Chaodi, Zheng, Xinglong, Li, Jing, Zhang, Yongjian, Shi, Tao, Yan, Yang, and Han, Dan

Subjects

*LONG QT syndrome, *ANTIFUNGAL agents, *PROTEIN expression, *WESTERN immunoblotting, *CONFOCAL microscopy

Abstract

Properties of mutant human ether‐à‐go‐go‐related gene (hERG) channels can be modified by some antibiotics. However, the pharmacological effects of posaconazole on cardiomyocyte hERG channels remain unclear. Whole‐cell patch clamping, western blotting and laser confocal scanning microscopy were used to evaluate the effects of posaconazole on wild‐type (WT)‐, A561V‐ and L539 fs/47‐hERG channels expressed in human embryonic kidney (HEK) 293 cells. In electrophysiological experiments, HEK 293 cells were transiently co‐transfected with equal amounts of WT‐hERG, WT+A561 V‐hERG and WT+L539 fs/47‐hERG plasmids to mimic a heterozygous genotype. Posaconazole (30 μM) increased tail currents in cells expressing WT‐hERG, WT+A561 V‐hERG and WT+L539 fs/47‐hERG by 82.65%, 147.72% and 134.73%, respectively, compared to controls. Posaconazole increased hERG protein expression in cells expressing WT‐hERG, WT+A561 V‐hERG and WT+L539 fs/47‐hERG compared to controls condition as well as their trafficking to the cell membrane. To our knowledge, this is the first study to show that antifungal agent posaconazole rescues the mutant A561 V‐hERG and L539 fs/47‐hERG channels by altering the gating kinetics, enhancing the expression and trafficking of hERG channels. The results demonstrate that posaconazole could be a promising candidate for the prevention and treatment of long QT syndrome and other arrhythmia‐related diseases. [ABSTRACT FROM AUTHOR]

Published

2021