AI Article Synopsis

  • Traditional patch-clamp methods have low throughput and require expert handling, while automated patch-clamp (APC) methods are easier but mostly suited for smaller cells.
  • Researchers developed a fixed-well APC plate format that works well with larger cells like cardiomyocytes from mammalian hearts, allowing for the reliable capture of various electrophysiological data.
  • This approach enhances drug screening efficacy and opens the door for detailed studies on human cardiac electrophysiology, ultimately supporting drug development and personalized treatments for heart diseases.

Article Abstract

Crucial conventional patch-clamp approaches to investigate cellular electrophysiology suffer from low-throughput and require considerable experimenter expertise. Automated patch-clamp (APC) approaches are more experimenter independent and offer high-throughput, but by design are predominantly limited to assays containing small, homogenous cells. In order to enable high-throughput APC assays on larger cells such as native cardiomyocytes isolated from mammalian hearts, we employed a fixed-well APC plate format. A broad range of detailed electrophysiological parameters including action potential, L-type calcium current and basal inward rectifier current were reliably acquired from isolated swine atrial and ventricular cardiomyocytes using APC. Effective pharmacological modulation also indicated that this technique is applicable for drug screening using native cardiomyocyte material. Furthermore, sequential acquisition of multiple parameters from a single cell was successful in a high throughput format, substantially increasing data richness and quantity per experimental run. When appropriately expanded, these protocols will provide a foundation for effective mechanistic and phenotyping studies of human cardiac electrophysiology. Utilizing scarce biopsy samples, regular high throughput characterization of primary cardiomyocytes using APC will facilitate drug development initiatives and personalized treatment strategies for a multitude of cardiac diseases.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9477872PMC
http://dx.doi.org/10.1038/s42003-022-03871-2DOI Listing

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