西亚试剂:Portability of paddle motif function and pharmacology in vo
发布时间:2025-09-20
Portability of paddle motif function and pharmacology in voltage sensors
AbdulRasheed A. Alabi1,3, Maria Isabel Bahamonde1,3, Hoi Jong Jung2, Jae Il Kim2 & Kenton J. Swartz1
- Molecular Physiology and Biophysics Section, Porter Neuroscience Research Center, National Institute of Neurological Disorders and Stroke, National Institutes of Health, Bethesda, Maryland 20892, USA
- Department of Life Sciences, Gwangju Institute of Science and Technology, Gwangju, 500-712, Korea
- These authors contributed equally to this work.
Correspondence to: Kenton J. Swartz1 Correspondence and requests for materials should be addressed to K.J.S. (Email: swartzk@ninds.nih.gov).
Voltage-sensing domains enable membrane proteins to sense and react to changes in membrane voltage. Although identifiable S1–S4 voltage-sensing domains are found in an array of conventional ion channels and in other membrane proteins that lack pore domains, the extent to which their voltage-sensing mechanisms are conserved is unknown. Here we show that the voltage-sensor paddle, a motif composed of S3b and S4 helices, can drive channel opening with membrane depolarization when transplanted from an archaebacterial voltage-activated potassium channel (KvAP) or voltage-sensing domain proteins (Hv1 and Ci-VSP) into eukaryotic voltage-activated potassium channels. Tarantula toxins that partition into membranes can interact with these paddle motifs at the protein–lipid interface and similarly perturb voltage-sensor activation in both ion channels and proteins with a voltage-sensing domain. Our results show that paddle motifs are modular, that their functions are conserved in voltage sensors, and that they move in the relatively unconstrained environment of the lipid membrane. The widespread targeting of voltage-sensor paddles by toxins demonstrates that this modular structural motif is an important pharmacological target.
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