Portability of paddle motif function and pharmacology in voltage sensors

Alabi, AbdulRasheed A.; Bahamonde, María Isabel; Jung, Hahn Chul; Kim, Jae Il; Swartz, Kenton J.

doi:10.1038/nature06266

Cited by 205 publications

(299 citation statements)

References 49 publications

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“…Only small portions of the two domains, e.g. the "paddle" motif of the VS domain and the P loop with most of the transmembrane domains of the pore, could be exchanged between K + channels (Lu et al, 2001;Alabi et al, 2007). These results led to the conclusion that membrane modules have coevolved so intimately in Kv proteins that it is impossible to exchange them entirely without losing the function of the chimeric channels.…”

Section: Viral K + Channels Are Ideal For Building More Complex and Mmentioning

confidence: 99%

Potassium Ion Channels: Could They Have Evolved from Viruses?

et al. 2013

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Section: Viral K + Channels Are Ideal For Building More Complex and Mmentioning

confidence: 99%

Potassium Ion Channels: Could They Have Evolved from Viruses?

et al. 2013

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“…[9][10][11] In fact, VSDs exist as independent gene products, coupled to other kinds of proteins, as demonstrated by the voltage-sensitive phosphatases 12 and can even mediate proton transport, as shown in the voltage-sensitive proton channels. 13,14 As diverse as the functions of VSDs may be, they all work by converting electrostatic energy into conformation changes and it seems that the basic mechanism of voltage sensing is the same.…”

Section: Introductionmentioning

confidence: 99%

Functional diversity of potassium channel voltage-sensing domains

Islas¹

2016

Channels

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Voltage-gated potassium channels or Kv's are membrane proteins with fundamental physiological roles. They are composed of 2 main functional protein domains, the pore domain, which regulates ion permeation, and the voltage-sensing domain, which is in charge of sensing voltage and undergoing a conformational change that is later transduced into pore opening. The voltagesensing domain or VSD is a highly conserved structural motif found in all voltage-gated ion channels and can also exist as an independent feature, giving rise to voltage sensitive enzymes and also sustaining proton fluxes in proton-permeable channels. In spite of the structural conservation of VSDs in potassium channels, there are several differences in the details of VSD function found across variants of Kvs. These differences are mainly reflected in variations in the electrostatic energy needed to open different potassium channels. In turn, the differences in detailed VSD functioning among voltage-gated potassium channels might have physiological consequences that have not been explored and which might reflect evolutionary adaptations to the different roles played by Kv channels in cell physiology.

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“…S4 of both mVSOP and Hv1 contain three arginines (R201, R204, and R207 in mVSOP, which are equivalent to R205, R208, and R211 in Hv1) that correspond to positively charged amino acids in S4 of voltagegated ion channels. Moreover, the area called the "paddle region," which is comprised of parts of S3 and S4 in Hv1, can replace the corresponding region in voltage-gated potassium channels without affecting voltage-dependent ion channel activity, indicating that a paddle motif-like structure is conserved among Hv and voltagegated potassium channels (20).Earlier studies by ourselves and others showed that Hv channels form dimers via their cytoplasmic regions (21−23), although monomeric Hv channels lacking their cytoplasmic regions remain functional and exhibit robust Hv channel activity (21,22). This motivated us to further define the minimum unit for Hv channel activity.…”

mentioning

confidence: 99%

Functionality of the voltage-gated proton channel truncated in S4

Sakata

Kurokawa

Nørholm

et al. 2009

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

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The voltage sensor domain (VSD) is the key module for voltage sensing in voltage-gated ion channels and voltage-sensing phosphatases. Structurally, both the VSD and the recently discovered voltage-gated proton channels (Hv channels) voltage sensor only protein (VSOP) and Hv1 contain four transmembrane segments. The fourth transmembrane segment (S4) of Hv channels contains three periodically aligned arginines (R1, R2, R3). It remains unknown where protons permeate or how voltage sensing is coupled to ion permeation in Hv channels. Here we report that Hv channels truncated just downstream of R2 in the S4 segment retain most channel properties. Two assays, site-directed cysteinescanning using accessibility of maleimide-reagent as detected by Western blotting and insertion into dog pancreas microsomes, both showed that S4 inserts into the membrane, even if it is truncated between the R2 and R3 positions. These findings provide important clues to the molecular mechanism underlying voltage sensing and proton permeation in Hv channels.ion conduction | membrane topology | membrane insertion | voltage sensor V oltage sensor domain (VSD) is a protein module that senses transmembrane voltage and regulates ion permeation through the pore (1-3) and phosphoinositide turnover by the phosphatase (4). The fourth transmembrane segment (S4) of VSD contains periodically aligned positively charged residues (arginine and lysine), which play a critical role in voltage sensing (1, 2). Recent analyses of the crystal structures of voltage-gated potassium channels (5, 6) showed that basic residues in S4 form salt bridges with negatively charged residues from other helices, and these salt bridges are formed at both sides of a hydrophobic residue such as phenylalanine. This suggests a focused electric field within a crevice surrounded by transmembrane helices (6), which would enable extracellular and intracellular aqueous environments to enter deeply into the membrane through a narrow crevice. One line of functional evidence for this narrow crevice is that mutation within the VSD creates an ion permeation pathway that is activated upon hyperpolarization (7−9). Such ion conduction is called an "omegacurrent" (9) or "gating pore current" (10). Similar conductances through the VSD are elicited in a mutated form of human voltagegated sodium channels (SCN4a) found in patients with periodic paralysis (11, 12) and in flatworm potassium channels (13).Recently, the protein, which consists solely of a VSD, was identified in tunicate, mouse (14) and human (15) and called voltage sensor only protein (VSOP) or Hv1. Mouse VSOP (mVSOP) is found within the phagosomes of white blood cells, and is essential for robust production of superoxide anions (16, 17) and maintenance of intracellular pH (18) in phagocytes. Despite the lack of a pore domain, these proteins function as voltage-gated proton channels (Hv channels) in heterologous expression systems (14,15) and when reconstituted into artificial membranes (19). S4 of both mVSOP and Hv1 contain three argini...

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Portability of paddle motif function and pharmacology in voltage sensors

Cited by 205 publications

References 49 publications

Potassium Ion Channels: Could They Have Evolved from Viruses?

Potassium Ion Channels: Could They Have Evolved from Viruses?

Functional diversity of potassium channel voltage-sensing domains

Functionality of the voltage-gated proton channel truncated in S4

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