Characterization of a hERG Screen Using the IonWorks HT: Comparison to a hERG Rubidium Efflux Screen

Sorota, Steve; Zhang, Xue Song; Margulis, Michael; Tucker, Kristal R.; Priestley, Tony

doi:10.1089/adt.2005.3.47

Cited by 76 publications

(44 citation statements)

References 25 publications

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“…A better correlation was observed with the values obtained in the present study than with the previously reported values, which is probably due to the differences in experimental conditions such as recording solutions and voltage protocols. The underestimated IC 50 values previously often observed due to the limited time for solution exchange and the adsorption of lipophilic test compounds (Guo and Guthrie 2005;Sorota et al 2005) were not observed in the present work. Also, the range of the IC 50 values extends over six orders of magnitude of concentrations with a slope of 0.96 determined by a linear regression, close to the unity line, indicating that the dynamic range of this method is broad enough for most of the test compounds to fall into this range.…”

contrasting

confidence: 70%

Pharmacological studies of Cav3.1 T-type calcium channels using automated patch-clamp techniques

Choi

Song²,

Cheong³

et al. 2011

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Abstract. T-type calcium channels are involved in a variety of physiological and pathophysiological processes, and thus could be therapeutic targets. However, there is no T-type channel selective blocker for use in clinical practice, demanding a need for the development of novel drugs where a higher-throughput screening system is required. Here we present pharmacological studies on Ca v 3.1 T-type channels using automated patch-clamp. The IC 50 values obtained from automated patch-clamp and conventional one showed a good correlation (correlation coefficient of 0.82), suggesting that the automated patch-clamp is an efficient and reliable method for ranking the drug potencies for T-type channels.

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contrasting

confidence: 70%

Pharmacological studies of Cav3.1 T-type calcium channels using automated patch-clamp techniques

Choi

Song²,

Cheong³

et al. 2011

gpb

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“…Typically, hERG potencies measured by automated and manual electrophysiology are in good agreement; however, some compounds are known to appear less potent when tested by automated electrophysiology. [23][24][25][26] Discrepancies typically arise from hydrophobic compounds being adsorbed to the surface of the plate used to hold the compound or to the patch plate itself. Glass-coated compound plates can help to minimize the nonspecific binding to the compound plate but come at a significant cost.…”

Section: Medium and High Throughput Herg Assaysmentioning

confidence: 99%

Role of hERG potassium channel assays in drug development

Priest¹,

Bell²,

García³

2008

Channels

118

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“…Using CHO cells that stably express hERG channels, IonWorks allows for assessment of approximately 200 data points per Patch plate and about 80 concentration-response curves per day [21][22][23][24]. A good pharmacological correlation with conventional MPC data was observed in terms of rank-order of compounds with hERG activity although the concentration-response curves were shifted to the right (within 3-to 5-fold).…”

Section: Automated Planar Patch-clamp Methodsmentioning

confidence: 98%

Preclinical Drug Safety and Cardiac Ion Channel Screening

Gintant

2011

Heart Rate and Rhythm

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A new chemical entity must demonstrate efficacy and safety in order to be considered a successful therapeutic agent. Towards that goal, it is best to discover drugs demonstrating a wide concentration range between (lower) preclinical efficacious plasma concentrations and (higher) plasma concentrations eliciting preclinical off-target adverse effects. Drugs possessing such characteristics provide greater flexibility in clinical trials and explorations into alternative indications. Thus, preclinical studies related to both efficacy and safety must be considered equally important during drug discovery efforts. Cardiac safety plays a key role in defining the safety of novel therapeutics, and defining a drug's therapeutic window/safety margin.Much emphasis has been placed in the past decade on detecting (and avoiding) the ability of non-cardiovascular drugs to delay or alter ventricular repolarization (acquired long QT syndrome [1]). This focus arises in part from the association of delayed repolarization to the rare but potentially life-threatening arrhythmia torsades de pointes. As torsades is a rare event, surrogate markers are employed to detect and avoid this potential proarrhythmic risk. Preclinically, the most recognized in vitro marker for delayed repolarization is drug block of I Kr (an outward repolarizing current that initiates and defines terminal ventricular repolarization). In humans, the a-subunit of the I Kr channel is encoded by the human ether-a-go-go related gene (hERG) gene. Block of hERG/I Kr along with prolongation of the QT interval (an interval on the ECG that generally represents the onset of ventricular depolarization and the termination of ventricular repolarization) form the presentday cornerstone for cardiac electrophysiologic safety testing. Due to the importance of testing hERG current as a surrogate marker of proarrhythmia, great strides have been made in developing and streamlining testing protocols/procedures to evaluate

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Characterization of a hERG Screen Using the IonWorks HT: Comparison to a hERG Rubidium Efflux Screen

Cited by 76 publications

References 25 publications

Pharmacological studies of Cav3.1 T-type calcium channels using automated patch-clamp techniques

Pharmacological studies of Cav3.1 T-type calcium channels using automated patch-clamp techniques

Role of hERG potassium channel assays in drug development

Preclinical Drug Safety and Cardiac Ion Channel Screening

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