Aditi Agrawal
Modelling the effect of experimental conditions that influence rundown of L-type calcium current [version 1; peer review: awaiting peer review]
Agrawal, Aditi; Clerx, Michael; Wang, Ken; Polonchuk, Liudmila; R. Mirams, Gary; J. Gavaghan, David; Aditi, Agrawal; David J., Gavaghan
Authors
Dr MICHAEL CLERX MICHAEL.CLERX@NOTTINGHAM.AC.UK
SENIOR RESEARCH FELLOW
Ken Wang
Liudmila Polonchuk
Professor GARY MIRAMS GARY.MIRAMS@NOTTINGHAM.AC.UK
PROFESSOR OF MATHEMATICAL BIOLOGY
David J. Gavaghan
Agrawal Aditi
Gavaghan David J.
Abstract
Background
L-type calcium channels (LCCs) are macro-molecular complexes that conduct ICaL and are involved in several critical functions in cardiac, skeletal, neuronal, smooth muscle, and endocrine cells. In common with other ionic channels they can be studied by isolating and overexpressing in a cell line, and the current through them can be measured using patch-clamp experiments. However, LCC current recordings are known to be contaminated with attenuation of current, known as ‘rundown’. Previous work has shown that increased accumulation of intracellular calcium is likely associated with increased rundown.
Methods
We built a mathematical model of ICaL conducted by LCCs overexpressed in CHO cells and systematically investigated the qualitative impact of both user-defined as well as experimental parameters within the typical patch-clamp setup on ICaL rundown.
Results
Simulations show that calcium-dependent inactivation (CDI) of LCCs modestly contributes towards experimentally observed rundown. The underlying reason for the experimental rundown due to CDI (RCDI) was found to be the non-instantaneous diffusion and reactions of calcium and the calcium-chelating buffer inside the cell. In this study we show that RCDI occurs when the buffer does not have sufficient time to diffuse into the cell; both after patching before the LCCs are activated, and also during the experiment progression. This finding was validated by showing that rundown due to accumulation of Ca2+ can be reduced by increasing the concentration of the calcium-chelating buffer in the intracellular solution.
Conclusions
To minimise rundown due to CDI, we suggest optimising independent experimental parameters such as buffer concentration and the time scales for diffusion to enable buffer equilibration into the cell. Additionally, we suggest that use of large cells should be avoided since they are more prone to RCDI.
Citation
Agrawal, A., Clerx, M., Wang, K., Polonchuk, L., R. Mirams, G., J. Gavaghan, D., Aditi, A., & David J., G. (2025). Modelling the effect of experimental conditions that influence rundown of L-type calcium current [version 1; peer review: awaiting peer review]
| Working Paper Type | Preprint |
|---|---|
| Publication Date | Mar 20, 2025 |
| Deposit Date | Apr 24, 2025 |
| Publicly Available Date | Apr 29, 2025 |
| DOI | https://doi.org/10.12688/wellcomeopenres.23558.1 |
| Public URL | https://nottingham-repository.worktribe.com/output/46850671 |
| Publisher URL | https://wellcomeopenresearch.org/articles/10-157/v1 |
Files
Modelling the effect of experimental conditions that influence rundown of L-type calcium current
(6.8 Mb)
PDF
Publisher Licence URL
https://creativecommons.org/licenses/by/4.0/
You might also like
Model-driven optimal experimental design for calibrating cardiac electrophysiology models
(2023)
Journal Article
Model-driven optimal experimental design for calibrating cardiac electrophysiology models
(2023)
Journal Article
Downloadable Citations
About Repository@Nottingham
Administrator e-mail: discovery-access-systems@nottingham.ac.uk
This application uses the following open-source libraries:
SheetJS Community Edition
Apache License Version 2.0 (http://www.apache.org/licenses/)
PDF.js
Apache License Version 2.0 (http://www.apache.org/licenses/)
Font Awesome
SIL OFL 1.1 (http://scripts.sil.org/OFL)
MIT License (http://opensource.org/licenses/mit-license.html)
CC BY 3.0 ( http://creativecommons.org/licenses/by/3.0/)
Powered by Worktribe © 2025
Advanced Search