AI Article Synopsis
- HCN channels are essential for controlling how neurons behave, and inhibiting HCN1 could help in treating neurological issues, but the details of how this inhibition happens weren't clear.
- Researchers used cryo-electron microscopy to show how the drug ivabradine binds to a specific site on the human HCN1 channel, revealing new structural details of this interaction.
- Additionally, they identified two existing FDA-approved drugs that can also target this binding site, paving the way for new treatments aimed at regulating HCN1 activity in neurological disorders.
Article Abstract
The hyperpolarization-activated cyclic nucleotide-gated (HCN) channels play a crucial role in regulating neuronal excitability. Despite growing evidence supporting the therapeutic potential of HCN1 inhibition in treating neurological disorders, the structural basis of channel inhibition by inhibitor has remained elusive. Here, we present the cryo-electron microscopy structure of human HCN1 channel in complex with inhibitor ivabradine, the drug on the market that acts on HCN channels. Combining electrophysiology, mutagenesis, and molecular dynamics simulations, our findings reveal that ivabradine binds to a previously unidentified pocket formed between the S4, S1, and HCN domain. Furthermore, through structure-based virtual screening, we identify two Food and Drug Administration-approved drugs that can inhibit the HCN1 channel by interacting with the ivabradine-binding site. Our results not only provide insights into the structural intricacies of ivabradine-mediated inhibition, but also offer a potential pharmacological framework for developing novel drugs targeting the HCN1 channel. The elucidation of these molecular interactions serves as a foundational step in advancing therapeutic strategies for modulating HCN1 activity, contributing to the broader landscape of drug discovery and development in this area.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11530593 | PMC |
| http://dx.doi.org/10.1016/j.jbc.2024.107798 | DOI Listing |
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