Fredrik Elinder scite author profile

Voltage-gated ion channels open and close in response to changes in membrane potential, thereby enabling electrical signaling in excitable cells. The voltage sensitivity is conferred through four voltage-sensor domains (VSDs) where positively charged residues in the fourth transmembrane segment (S4) sense the potential. While an open state is known from the Kv1.2/2.1 X-ray structure, the conformational changes underlying voltage sensing have not been resolved. We present 20 additional interactions in one open and four different closed conformations based on metal-ion bridges between all four segments of the VSD in the voltage-gated Shaker K channel. A subset of the experimental constraints was used to generate Rosetta models of the conformations that were subjected to molecular simulation and tested against the remaining constraints. This achieves a detailed model of intermediate conformations during VSD gating. The results provide molecular insight into the transition, suggesting that S4 slides at least 12 Å along its axis to open the channel with a 3 10 helix region present that moves in sequence in S4 in order to occupy the same position in space opposite F290 from open through the three first closed states. V oltage-gated ion channels are critical for biological signaling, and they are able to regulate ion flux on a millisecond time scale. To sense changes in membrane voltage, each ion channel is equipped with four voltage-sensor domains (VSDs) connected to a central ion-conducting pore domain. The fourth transmembrane segment (S4) of each VSD carries several positively charged amino-acid residues responsible for VSD gating (1). At least three elementary charges per VSD must traverse outwards through the membrane electric field to open a channel that corresponds to a considerable displacement of the S4 helix ( Fig. 1A) (2-4). The positive charges in S4 make salt bridges with negative countercharges on their move through the VSD (4-8). It has even been proposed that the VSD undergoes a conformational alteration following the opening, when the channel relaxes to an inactivated, that is closed, state (9). In addition to conferring voltage dependence to ion channels, VSDs also regulate enzymes (10), act as voltage-gated proton channels (11,12), are susceptible to disease-causing mutations (13,14), and serve as targets for drugs and toxins (1,(15)(16)(17)(18). Therefore, it is of crucial interest to understand the details underlying voltage sensing by VSDs.Few, if any, segments of membrane proteins have received more attention than the S4 helix of voltage sensors. In addition to their paramount biological importance, they can help us understand fundamental biophysical problems such as why some membrane protein segments can be hydrophilic (19), how charges effectively move through a membrane, or how a potential triggers structural changes on a microsecond time scale. These questions are inherently linked to transient conformations and contacts that can be difficult to capture in a single structure. Although active...

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Polyunsaturated fatty acid analogs act antiarrhythmically on the cardiac I _Ks channel

Liin

Ejneby

Barro-Soria

et al. 2015

Proc. Natl. Acad. Sci. U.S.A.

238

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Polyunsaturated fatty acids (PUFAs) affect cardiac excitability. Kv7.1 and the β-subunit KCNE1 form the cardiac IKs channel that is central for cardiac repolarization. In this study, we explore the prospects of PUFAs as IKs channel modulators. We report that PUFAs open Kv7.1 via an electrostatic mechanism. Both the polyunsaturated acyl tail and the negatively charged carboxyl head group are required for PUFAs to open Kv7.1. We further show that KCNE1 coexpression abolishes the PUFA effect on Kv7.1 by promoting PUFA protonation. PUFA analogs with a decreased pKa value, to preserve their negative charge at neutral pH, restore the sensitivity to open IKs channels. PUFA analogs with a positively charged head group inhibit IKs channels. These different PUFA analogs could be developed into drugs to treat cardiac arrhythmias. In support of this possibility, we show that PUFA analogs act antiarrhythmically in embryonic rat cardiomyocytes and in isolated perfused hearts from guinea pig.

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Voltage-sensing mechanism is conserved among ion channels gated by opposite voltages

Männikkö

Elinder

Larsson

2002

Nature

187

208

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Hyperpolarization-activated cyclic-nucleotide-gated (HCN) ion channels are found in rhythmically firing cells in the brain and in the heart, where the cation current through HCN channels (called I(h) or I(f)) causes these cells to fire repeatedly. These channels are also found in non-pacing cells, where they control resting membrane properties, modulate synaptic transmission, mediate long-term potentiation, and limit extreme hyperpolarizations. HCN channels share sequence motifs with depolarization-activated potassium (Kv) channels, such as the fourth transmembrane segment S4. S4 is the main voltage sensor of Kv channels, in which transmembrane movement of S4 charges triggers the opening of the activation gate. Here, using cysteine accessibility methods, we investigate whether S4 moves in an HCN channel. We show that S4 movement is conserved between Kv and HCN channels, which indicates that S4 is also the voltage sensor in HCN channels. Our results suggest that a conserved voltage-sensing mechanism operates in the oppositely voltage-gated Kv and HCN channels, but that there are different coupling mechanisms between the voltage sensor and activation gate in the two different channels.

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Lipoelectric Modification of Ion Channel Voltage Gating by Polyunsaturated Fatty Acids

Börjesson

Hammarström

Elinder

2008

Biophysical Journal

194

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Polyunsaturated fatty acids (PUFAs) have beneficial effects on epileptic seizures and cardiac arrhythmia. We report that omega-3 and omega-6 all-cis-PUFAs affected the voltage dependence of the Shaker K channel by shifting the conductance versus voltage and the gating charge versus voltage curves in negative direction along the voltage axis. Uncharged methyl esters of the PUFAs did not affect the voltage dependence, whereas changes of pH and charge mutations on the channel surface affected the size of the shifts. This suggests an electrostatic effect on the channel's voltage sensors. Monounsaturated and saturated fatty acids, as well as trans-PUFAs did not affect the voltage dependence. This suggests that fatty acid tails with two or more cis double bonds are required to place the negative carboxylate charge of the PUFA in a position to affect the channel's voltage dependence. We propose that charged lipophilic compounds could play a role in regulating neuronal excitability by electrostatically affecting the channel's voltage sensor. We believe this provides a new approach for pharmacological treatment that is voltage sensor pharmacology.

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An electrostatic potassium channel opener targeting the final voltage sensor transition

Börjesson

Elinder

2011

150

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Free polyunsaturated fatty acids (PUFAs) modulate the voltage dependence of voltage-gated ion channels. As an important consequence thereof, PUFAs can suppress epileptic seizures and cardiac arrhythmia. However, molecular details for the interaction between PUFA and ion channels are not well understood. In this study, we have localized the site of action for PUFAs on the voltage-gated Shaker K channel by introducing positive charges on the channel surface, which potentiated the PUFA effect. Furthermore, we found that PUFA mainly affects the final voltage sensor movement, which is closely linked to channel opening, and that specific charges at the extracellular end of the voltage sensor are critical for the PUFA effect. Because different voltage-gated K channels have different charge profiles, this implies channel-specific PUFA effects. The identified site and the pharmacological mechanism will potentially be very useful in future drug design of small-molecule compounds specifically targeting neuronal and cardiac excitability.

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Fredrik Elinder

Tracking a complete voltage-sensor cycle with metal-ion bridges

Polyunsaturated fatty acid analogs act antiarrhythmically on the cardiac I _Ks channel

Voltage-sensing mechanism is conserved among ion channels gated by opposite voltages

Lipoelectric Modification of Ion Channel Voltage Gating by Polyunsaturated Fatty Acids

An electrostatic potassium channel opener targeting the final voltage sensor transition

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Product

Resources

About

Fredrik Elinder

Tracking a complete voltage-sensor cycle with metal-ion bridges

Polyunsaturated fatty acid analogs act antiarrhythmically on the cardiac I Ks channel

Voltage-sensing mechanism is conserved among ion channels gated by opposite voltages

Lipoelectric Modification of Ion Channel Voltage Gating by Polyunsaturated Fatty Acids

An electrostatic potassium channel opener targeting the final voltage sensor transition

Contact Info

Product

Resources

About

Polyunsaturated fatty acid analogs act antiarrhythmically on the cardiac I _Ks channel