Patterned cardiomyocytes on microelectrode arrays as a functional, high information content drug screening platform

Natarajan, Anupama; Stancescu, Maria; Dhir, Vipra; Armstrong, Christopher G.; Sommerhage, Frank; Hickman, James J.; Molnár, Péter

doi:10.1016/j.biomaterials.2010.12.022

Cited by 111 publications

(114 citation statements)

References 52 publications

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“…Amiodarone inhibited neuronal activity in rat cortical neurons [37]. Measuring effects on the beating rate or on the generation of action potentials as additional parameters, using for example multielectrode arrays [38], will most likely result in a more sensitive assay and might even result in an assay able to detect a wider range of neurotoxins. Ultimately, a model capable of detecting an extensive range of marine neurotoxins shall present a large variety of ion channels/pumps as well as neuronal receptors, the principal targets of such toxins.…”

Section: Discussionmentioning

confidence: 99%

In vitro detection of cardiotoxins or neurotoxins affecting ion channels or pumps using beating cardiomyocytes as alternative for animal testing

Nicolas

Hendriksen

Haan

et al. 2015

Toxicology in Vitro

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In vitro detection of cardiotoxins or neurotoxins affecting ion channels or pumps using beating cardiomyocytes as alternative for animal testing Nicolaas, J.; Hendriksen, P.J.M.; Haan, L.H.J. de; Koning, R.; Rietjens, I.M.C.M.; Bovee, T.F.H.This is a "Post-Print" accepted manuscript, which has been published in the "Toxicology in Vitro"This version is distributed under a non-commencial no derivatives Creative Commons (CC-BY-NC-ND) user license, which permits use, distribution, and reproduction in any medium, provided the original work is properly cited and not used for commercial purposes. Further, the restriction applies that if you remix, transform, or build upon the material, you may not distribute the modified material.Please cite this publication as follows:

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Section: Discussionmentioning

confidence: 99%

In vitro detection of cardiotoxins or neurotoxins affecting ion channels or pumps using beating cardiomyocytes as alternative for animal testing

Nicolas

Hendriksen

Haan

et al. 2015

Toxicology in Vitro

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“…In some cases, it can be valuable to electrically ‘pace’ CMs so that their beating rate (defined RR‐like interval because it reflects the analogue ECG parameter) is standardized and constant rather than irregular, as often occurs if beating is spontaneous. However, in contrast to isolated cells or neuronal networks, clusters of hPSC‐CMs seeded on MEA cannot efficiently be paced in all available devices, because the hardware is not suitable (Natarajan et al , 2011). Although methods for electrical stimulation have been implemented in some custom‐made MEAs (Kaneko et al , 2012) and impedance‐based systems (Xi et al , 2011), these are not yet widely used.…”

Section: Assays and Readoutsmentioning

confidence: 99%

Integrating cardiomyocytes from human pluripotent stem cells in safety pharmacology: has the time come?

Sala

Bellin

Mummery

2016

British J Pharmacology

107

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Cardiotoxicity is a severe side effect of drugs that induce structural or electrophysiological changes in heart muscle cells. As a result, the heart undergoes failure and potentially lethal arrhythmias. It is still a major reason for drug failure in preclinical and clinical phases of drug discovery. Current methods for predicting cardiotoxicity are based on guidelines that combine electrophysiological analysis of cell lines expressing ion channels ectopically in vitro with animal models and clinical trials. Although no new cases of drugs linked to lethal arrhythmias have been reported since the introduction of these guidelines in 2005, their limited predictive power likely means that potentially valuable drugs may not reach clinical practice. Human pluripotent stem cell‐derived cardiomyocytes (hPSC‐CMs) are now emerging as potentially more predictive alternatives, particularly for the early phases of preclinical research. However, these cells are phenotypically immature and culture and assay methods not standardized, which could be a hurdle to the development of predictive computational models and their implementation into the drug discovery pipeline, in contrast to the ambitions of the comprehensive pro‐arrhythmia in vitro assay (CiPA) initiative. Here, we review present and future preclinical cardiotoxicity screening and suggest possible hPSC‐CM‐based strategies that may help to move the field forward. Coordinated efforts by basic scientists, companies and hPSC banks to standardize experimental conditions for generating reliable and reproducible safety indices will be helpful not only for cardiotoxicity prediction but also for precision medicine.Linked ArticlesThis article is part of a themed section on New Insights into Cardiotoxicity Caused by Chemotherapeutic Agents. To view the other articles in this section visit http://onlinelibrary.wiley.com/doi/10.1111/bph.v174.21/issuetoc

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“…The current microCCA has >10,000 cells per compartment which provides sufficient material for diagnosis, but requires the sacrifice of the unit. On line analysis either optically 18 or electrically 15 allows readout without having to sacrifice the unit and is compatible with measurement of time course.…”

Section: Living Cell Models Of Humansmentioning

confidence: 99%

“…Also there are serum-free defined media that will support long-term culture of difficult to culture cell types. 15 Another constraint, but not a strong one with the development of a broad range of analytic devices, is analysis based on relatively few cells. The current microCCA has >10,000 cells per compartment which provides sufficient material for diagnosis, but requires the sacrifice of the unit.…”

Section: Living Cell Models Of Humansmentioning

confidence: 99%

Modeling Life

Shuler

2012

Ann Biomed Eng

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Abstract-We seek to construct physical and mathematical models of life. Such models allow us to test our understanding of how living systems function and how they respond to human imposed stimuli. One system is a genomically and chemically complete model of a minimal cell. This cell is a hypothetical bacterium with the fewest number of genes possible. Such a minimal cell provides a platform to ask about the essential features of a living cell and forms a platform to investigate ''synthetic biology.'' A second system is ''Body-on-a-Chip'' which is a microfabricated microfluidic system with cells or tissue constructs representing various organs in the body. It can be constructed from human or animal cells and used in drug discovery development. That model is a physical representation of a physiologically based pharmacokinetic model. Both the computer and the physical models provide insight into the underlying biology and provide new tools to make use of that understanding to provide benefits to society.

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Patterned cardiomyocytes on microelectrode arrays as a functional, high information content drug screening platform

Cited by 111 publications

References 52 publications

In vitro detection of cardiotoxins or neurotoxins affecting ion channels or pumps using beating cardiomyocytes as alternative for animal testing

In vitro detection of cardiotoxins or neurotoxins affecting ion channels or pumps using beating cardiomyocytes as alternative for animal testing

Integrating cardiomyocytes from human pluripotent stem cells in safety pharmacology: has the time come?

Modeling Life

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