Published February 7, 2024
| Version v1
Journal article
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Photolipid excitation triggers depolarizing optocapacitive currents and action potentials
Creators
- 1. University of Chicago
- 2. Johannes Kepler University Linz
- 3. Karl-Franzens-University
Description
Optically-induced changes in membrane capacitance may regulate neuronal activity without requiring genetic modifications. Previously, they mainly relied on sudden temperature jumps due to light absorption by membrane-associated nanomaterials or water. Yet, nanomaterial targeting or the required high infrared light intensities obstruct broad applicability. Now, we propose a very versatile approach: photolipids (azobenzene-containing diacylglycerols) mediate light-triggered cellular de- or hyperpolarization. As planar bilayer experiments show, the respective currents emerge from millisecond-timescale changes in bilayer capacitance. UV light changes photolipid conformation, which awards embedding plasma membranes with increased capacitance and evokes depolarizing currents. They open voltage-gated sodium channels in cells, generating action potentials. Blue light reduces the area per photolipid, decreasing membrane capacitance and eliciting hyperpolarization. If present, mechanosensitive channels respond to the increased mechanical membrane tension, generating large depolarizing currents that elicit action potentials. Membrane self-insertion of administered photolipids and focused illumination allows cell excitation with high spatiotemporal control.
Data availability
The data that support this study are available from the corresponding authors upon request. A Source Data file pertaining to Figs. 1, 2, 3, 5 and Supplementary Figs. 1–3 is provided.Files
Photolipid-excitation-triggers-depolarizing-optocapacitive-currents-and-action-potentials.pdf
Additional details
Identifiers
- DOI
- 10.1038/s41467-024-45403-y
- Other
- oai:uchicago.tind.io:10937
Funding
- Austrian Science Fund (FWF)
- P34826
- National Institutes of Health
- R01GM030376
- National Science Foundation
- QuBBE QLCI
- National Science Foundation
- OMA-2121044