Ion conduction and conformational flexibility of a bacterial voltage-gated sodium channel

Boiteux, Céline; Vorobyov, Igor; Allen, Toby W.

doi:10.1073/pnas.1320907111

Cited by 101 publications

(219 citation statements)

References 52 publications

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“…The rotameric change in conformation of the Glu66 side chains herein observed is reminiscent of the mobility recently reported for Na + bacterial channels, where the conformational isomerization of a ring of four glutamate side chains lining the selectivity filter is coupled to ionic coordination (24,25,48). We propose that this flexibility, together with the number of equivalent and contiguous ion binding sites in the filter (26,34,49), underscores the poor ionic selectivity of CNG channels and reveals a conduction mode that differs substantially from that of classical K + channels, which are highly selective and have a fairly rigid molecular structure.…”

Section: Discussionsupporting

confidence: 69%

“…We demonstrate that the extracellular entrance of the selectivity filter and the filter itself exhibit a dynamic structure capable of structural rearrangements, which can be partially captured by X-ray crystallography and are best visualized and understood through MD simulations. Our results indicate that the pore of CNG channels is highly flexible, with a liquidlike energy landscape (24,25). This flexibility underlies the poor selectivity of CNG channels and their strong coupling between gating and permeation.…”

mentioning

confidence: 83%

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A structural, functional, and computational analysis suggests pore flexibility as the base for the poor selectivity of CNG channels

Napolitano

Bisha

March

et al. 2015

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

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Cyclic nucleotide-gated (CNG) ion channels, despite a significant homology with the highly selective K + channels, do not discriminate among monovalent alkali cations and are permeable also to several organic cations. We combined electrophysiology, molecular dynamics (MD) simulations, and X-ray crystallography to demonstrate that the pore of CNG channels is highly flexible. When a CNG mimic is crystallized in the presence of a variety of monovalent cations, including Na + , Cs + , and dimethylammonium (DMA + ), the side chain of Glu66 in the selectivity filter shows multiple conformations and the diameter of the pore changes significantly. MD simulations indicate that Glu66 and the prolines in the outer vestibule undergo large fluctuations, which are modulated by the ionic species and the voltage. This flexibility underlies the coupling between gating and permeation and the poor ionic selectivity of CNG channels.CNG channels | pore flexibility | X-ray crystallography | MD simulations I n K + selective channels, the opening and closing of the ion channel pore (gating) and the translocation of ions through the pore (permeation) are considered independent processes with distinct structural basis (1). Gating is controlled by the bundle crossing at the intracellular side, whereas permeation reflects ion-ion and ion-pore interactions within the selectivity filter (1-5). Based on these experimental observations, the current paradigm assumes that the 3D structure of the selectivity filter is relatively rigid during ion translocation and the mechanisms of ionic permeation can be deduced in essence from its crystal structure. This paradigm has been successfully applied to several K + channels (4, 6, 7). Cyclic nucleotide-gated (CNG) channels underlie sensory transduction in the retina and olfactory epithelium and share a high degree of homology with K + channels (8-10). In contrast to K + channels, CNG channels' primary gate is located at the selectivity filter (11), suggesting that the same protein region controls ion permeation and gating. In CNG channels the ionic species present inside the pore influences channel gating; however, the nature of this coupling is not well understood (12-16). In the presence of large cations, such as Rb + and Cs + , channel conductance and gating are also controlled by membrane voltage, and current-voltage relationships activated by 1 mM cGMP depend on the radius of the permeating ion (17, 18) (Fig. S1).Structural information on CNG channels is limited to a lowresolution electron microscopy map (19), partial crystal structures of the intracellular cyclic nucleotide-binding domains (20)(21)(22), and the crystal structure of a chimeric channel in which the CNG selectivity-filter sequence is engineered into a bacterial NaK channel, creating a CNG mimic (NaK2CNG; Fig. 1 A and B) that shares several properties of CNG channels (23). This CNG mimic provides a suitable model for understanding the properties of the pore underlying the low ionic selectivity and the coupling between gating and perme...

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Section: Discussionsupporting

confidence: 69%

mentioning

confidence: 83%

A structural, functional, and computational analysis suggests pore flexibility as the base for the poor selectivity of CNG channels

Napolitano

Bisha

March

et al. 2015

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

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“…Similar conclusions were reached from long scale MD simulations (Boiteux et al, 2014), suggesting an essentially barrierless (~1.5 kcal/mol maximum barrier to conduction) multi ion 'knock-on' or 'pass-by' mechanism is more likely in the fully charged state, promoted by repulsive interactions between charged side-chains. The presence of one protonated glutamate, similarly, leads to a reduced charged density at the mouth of the selectivity filter.…”

Section: Protonation State Of Glu177supporting

confidence: 70%

“…Restriction of the selectivity filter, in a singly protonated system, seemingly adjusts the cavity shape and the orientation of S6 (Boiteux et al, 2014). The observed bent conformation in S6, on the level of P200-T206, is parallel to that of an inactivated structure suggested by Payandah et al (Payandeh et al 2012).…”

Section: Protonation State Of Glu177mentioning

confidence: 55%

“…Subsequently, Boiteux and coworkers identified a double potential well at S HFS in PMF profiles, corresponding to available conformers of Glu177, reducing the barrier between selectivity filter sites (Boiteux, Vorobyov, & Allen, 2014). An average occupancy of 2.3 ions is reported in the selectivity filter, lending further evidence to a three-ion conduction mechanism in which the selectivity filter switches between one, two and three-ion configurations facilitated by the isomerization of Glu177.…”

Section: S Hfs /S Cen S Hfs /S In S Hfs /Intracellular (Figure 5)mentioning

confidence: 99%

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Voltage-Gated Sodium Channels

Oakes

Furini

Domene

2016

Na Channels From Phyla to Function

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Simulating ion channel activation mechanisms using swarms of trajectories

Lev

Allen

2019

J Comput Chem

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Atomic-level studies of protein activity represent a significant challenge as a result of the complexity of conformational changes occurring on wide-ranging timescales, often greatly exceeding that of even the longest simulations. A prime example is the elucidation of protein allosteric mechanisms, where localized perturbations transmit throughout a large macromolecule to generate a response signal. For example, the conversion of chemical to electrical signals during synaptic neurotransmission in the brain is achieved by specialized membrane proteins called pentameric ligand-gated ion channels. Here, the binding of a neurotransmitter results in a global conformational change to open an ion-conducting pore across the nerve cell membrane. X-ray crystallography has produced static structures of the open and closed states of the proton-gated GLIC pentameric ligand-gated ion channel protein, allowing for atomistic simulations that can uncover changes related to activation. We discuss a range of enhanced sampling approaches that could be used to explore activation mechanisms. In particular, we describe recent application of an atomistic string method, based on Roux's "swarms of trajectories" approach, to elucidate the sequence and interdependence of conformational changes during activation. We illustrate how this can be combined with transition analysis and Brownian dynamics to extract thermodynamic and kinetic information, leading to understanding of what controls ion channel function.

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Ion conduction and conformational flexibility of a bacterial voltage-gated sodium channel

Cited by 101 publications

References 52 publications

A structural, functional, and computational analysis suggests pore flexibility as the base for the poor selectivity of CNG channels

A structural, functional, and computational analysis suggests pore flexibility as the base for the poor selectivity of CNG channels

Voltage-Gated Sodium Channels

Simulating ion channel activation mechanisms using swarms of trajectories

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