Author
Listed:
- Young-Woo Nam
(Chapman University School of Pharmacy)
- Dohyun Im
(Kyoto University)
- Ana Santa Cruz Garcia
(Northeastern University School of Pharmacy and Pharmaceutical Sciences)
- Marios L. Tringides
(Case Western Reserve University School of Medicine)
- Hai Minh Nguyen
(University of California Davis)
- Yan Liu
(Stanford University)
- Razan Orfali
(Chapman University School of Pharmacy)
- Alena Ramanishka
(Chapman University School of Pharmacy)
- Grigore Pintilie
(Stanford University)
- Chih-Chia Su
(Case Western Reserve University School of Medicine)
- Meng Cui
(Northeastern University School of Pharmacy and Pharmaceutical Sciences)
- Diomedes E. Logothetis
(Northeastern University School of Pharmacy and Pharmaceutical Sciences)
- Edward W. Yu
(Case Western Reserve University School of Medicine)
- Heike Wulff
(University of California Davis)
- K. George Chandy
(Nanyang Technological University)
- Miao Zhang
(Chapman University School of Pharmacy)
Abstract
Small-conductance Ca2+-activated K+ (KCa2.1-KCa2.3) channels modulate neuronal and cardiac excitability. We report cryo-electron microscopy structures of the KCa2.2 channel in complex with calmodulin and Ca2+, alone or bound to two small molecule inhibitors, at 3.18, 3.50, 2.99 and 2.97 angstrom resolution, respectively. Extracellular S3-S4 loops in β-hairpin configuration form an outer canopy over the pore with an aromatic box at the canopy’s center. Each S3-S4 β-hairpin is tethered to the selectivity filter in the neighboring subunit by inter-subunit hydrogen bonds. This hydrogen bond network flips the aromatic residue (Tyr362) in the filter’s GYG signature by 180°, causing the outer selectivity filter to widen and water to enter the filter. Disruption of the tether by a mutation narrows the outer selectivity filter, realigns Tyr362 to the position seen in other K+ channels, and significantly increases unitary conductance. UCL1684, a mimetic of the bee venom peptide apamin, sits atop the canopy and occludes the opening in the aromatic box. AP14145, an analogue of a therapeutic for atrial fibrillation, binds in the central cavity below the selectivity filter and induces closure of the inner gate. These structures provide a basis for understanding the small unitary conductance and pharmacology of KCa2.x channels.
Suggested Citation
Young-Woo Nam & Dohyun Im & Ana Santa Cruz Garcia & Marios L. Tringides & Hai Minh Nguyen & Yan Liu & Razan Orfali & Alena Ramanishka & Grigore Pintilie & Chih-Chia Su & Meng Cui & Diomedes E. Logothe, 2025.
"Cryo-EM structures of the small-conductance Ca2+-activated KCa2.2 channel,"
Nature Communications, Nature, vol. 16(1), pages 1-13, December.
Handle:
RePEc:nat:natcom:v:16:y:2025:i:1:d:10.1038_s41467-025-59061-1
DOI: 10.1038/s41467-025-59061-1
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