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You may include any references to papers as in: the use of JSmol in Proteopedia ^[1] or to the article describing Jmol ^[2] to the rescue.

Introduction

Ion channels are transmembrane proteins which allow ions to pass through biological membranes. Some of these channels are very selective, others have a low level of selectivity. The NaK channel is a non-selective one : It conduits cations more than anions but it let pass several cations : Na+, K+, Rb+, and Ca2+ [1.1].

Understanding how these channels work is important because in the organism a lot of messages are transmitted through electric currents (which are ionic currents across the membrane) : nerves impulse, photoreceptors, etc. Thus, these not very selective NaK channels are very interesting for the inhibition of intercellular messages for instance.

Structure

General Description

The NaK channel is like an intracellular gate.

The NaK channel have the same general architecture as the K+ channels. In fact, the NaK channel has 4 subunits which are symmetric with respect to the central axis of the pore. Each subunit is composed of 3 alpha-helices. One of them is a short pore helix which is oblique to the channel axis. The others are the outer and the inner helices and they extend across the lipid membrane.

Structure of the open or closed complex

In response to a external stimuli, the structure of the NaK channel is different. In fact, after some inter- and intra-subunit rearrangements, the NaK channel can be open or closed.

Closed Conformation

In the closed conformation, inner helices are near and straight. There is a subsequent bundle crossing formed by interactions between C-terminal residues. In the region just above the bundle crossing, Phe92 from each inner helix forms contacts with a hydrophobic patch on the opposite face of Phe92 from the neighboring inner helix formed by Val91, Phe94, Ile95 and Leu98. [2]

Open Conformation

Channel opening is a conserved mechanism.The inner helix twist and bend thanks to a conserved glycine residue which is considered as the gating hinge. After this bending, the inner helices twist of 45° around their helical helix and the outer helix tilt tangentially in the same direction by 11° without any twisting motion. As all of helix twist or move inside of a subunit, intra-subunit interactions between inner and outer helix don’t differ a lot. On the contrary, inter-subunit interactions between neighboring inner helix change. In fact, Phe92 swings away and points its side chain towards the central ion conduction pathway due to inner helix bending and the hydrophobic patch slides along the neighboring inner helix by two helical turns and forms new van der Waals contacts with Phe85. This resulted in a disruption of the bundle crossing and so intra- and inter- subunits interactions in the open state become less important than in the close state. [2]

Active Site & Ions Passing

We will see for every binding site how his structure allows the passage of one or several ions.

External Site

We may notice the presence of a glycine (Gly67) which brings four carbonyl oxygen atoms, more inward oriented, able to bind with water molecules. This create an environement which can chelate K+ and Rb+ ions, but avoid the binding of Na+.

Moreover, thanks to a space intercation between Asp 66 and Gly67, the external site has a higher affinity for divalent cations such as Ca2+ and Ba2+ rather than monovalent such as K+ and Rb+[3].

The nature of the ligands is carbonyl-water.

Vestibule

In the case of the vestibule, there are too four carbonyl oxygen atom which brings by a valine (Val64). For instance, Na+ is neared to the ligand by this way: distance Na+-ligand=2,9 Ä. Moreover, ions are partially hydrated by four water molecules( they are along with the carboxyl oxygene atoms) : distance ions-H2O=4 Ä. The presence of water allows a greater flexibility in the ion binding so the vestibule may adapt to monovalent cations such as Na+, K+ and Rb+. However, this structure has a greater selectivity for K+ than Na+ : water molecules help to create a selectivity filter thanks to ligand geometry: octahedral arrangement which is impossible with Na+ because of a smaller radius and a hydratation by 5-6 molecules of water [4,5].

The nature of the ligands is carbonyl-water.

Site 3

He is the most non selective ion binding site which let pass mono and divalent cations, so a contamination can occur : presence of unkonwn species of ion at this site.

Moreover we may underscore a higher affinity for K+ than Na+ because of several reason :

  - First, we can find 4 backbone carbonyl oxygen from Val64 which participate in K+ and Rb+ ions chelation because of the formation of an octahedral ligand: an octahedral arrangement oxygen ligands in the channel pore is more favorable for K+ than Na+.
  - The lack of selectivity is due to the fact that the NaK channel have an almost identical structure when it is in complex with Na+, K+ or Rb+ : there is no big rearrangement in the structure of the protein depending on the bound ion. So the structure is stable with any ions, so it is non selective. Moreover, it could have a heavy atom contamination but it happens in a smaller extent with K+ than with Na+.

The amino-acids of the site 3 participate a lot in the transfert of Na+. In this case, Na+ binds because of an H-bonding interactions between Asp66 and the backbone amide of Asn68 which stabilize the structure. Furthermore, Val64 and Thr65 form a ion binding cage where Na+ ions tend bind at upper or lower ends (not in the center).

The nature of the ligands are carbonyl-carbonyl.

Site 4

We find again a ion binding cage made by carbonyl oxygen atoms from Thr63. Na+ ions have almost a planar conformation with respect to its ligands : distance of 2,4 Ä with the four hydroxyl oxygen atoms. There is also a coordination with water molecule in the central cavity : distance of 2,7 Ä between H2O and Na+.

The nature of the ligands is carbonyl-hydroxyl.

Regulation

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Structural highlights

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References

1. ↑ Hanson, R. M., Prilusky, J., Renjian, Z., Nakane, T. and Sussman, J. L. (2013), JSmol and the Next-Generation Web-Based Representation of 3D Molecular Structure as Applied to Proteopedia. Isr. J. Chem., 53:207-216. doi:http://dx.doi.org/10.1002/ijch.201300024
2. ↑ Herraez A. Biomolecules in the computer: Jmol to the rescue. Biochem Mol Biol Educ. 2006 Jul;34(4):255-61. doi: 10.1002/bmb.2006.494034042644. PMID:21638687 doi:10.1002/bmb.2006.494034042644

Contributors

Camille Noblet & Lola Welsch