Modeling the human Nav1.5 sodium channel: structural and mechanistic insights of ion permeation and drug blockade

Marawan Ahmed; Horia Jalily Hasani; Aravindhan Ganesan; Michael Houghton; Khaled Barakat

doi:10.2147/DDDT.S133944

Modeling the human Na_v1.5 sodium channel: structural and mechanistic insights of ion permeation and drug blockade

Drug Des Devel Ther. 2017 Aug 4:11:2301-2324. doi: 10.2147/DDDT.S133944. eCollection 2017.

Authors

Marawan Ahmed¹, Horia Jalily Hasani¹, Aravindhan Ganesan¹, Michael Houghton^{2

3

4}, Khaled Barakat^{1

2

3}

Affiliations

¹ Faculty of Pharmacy and Pharmaceutical Sciences.
² Li Ka Shing Institute of Virology.
³ Li Ka Shing Applied Virology Institute.
⁴ Department of Medical Microbiology and Immunology, Katz Centre for Health Research, University of Alberta, Edmonton, AB, Canada.

Abstract

Abnormalities in the human Na_v1.5 (hNa_v1.5) voltage-gated sodium ion channel (VGSC) are associated with a wide range of cardiac problems and diseases in humans. Current structural models of hNa_v1.5 are still far from complete and, consequently, their ability to study atomistic interactions of this channel is very limited. Here, we report a comprehensive atomistic model of the hNa_v1.5 ion channel, constructed using homology modeling technique and refined through long molecular dynamics simulations (680 ns) in the lipid membrane bilayer. Our model was comprehensively validated by using reported mutagenesis data, comparisons with previous models, and binding to a panel of known hNa_v1.5 blockers. The relatively long classical MD simulation was sufficient to observe a natural sodium permeation event across the channel's selectivity filters to reach the channel's central cavity, together with the identification of a unique role of the lysine residue. Electrostatic potential calculations revealed the existence of two potential binding sites for the sodium ion at the outer selectivity filters. To obtain further mechanistic insight into the permeation event from the central cavity to the intracellular region of the channel, we further employed "state-of-the-art" steered molecular dynamics (SMD) simulations. Our SMD simulations revealed two different pathways through which a sodium ion can be expelled from the channel. Further, the SMD simulations identified the key residues that are likely to control these processes. Finally, we discuss the potential binding modes of a panel of known hNa_v1.5 blockers to our structural model of hNa_v1.5. We believe that the data presented here will enhance our understanding of the structure-property relationships of the hNa_v1.5 ion channel and the underlying molecular mechanisms in sodium ion permeation and drug interactions. The results presented here could be useful for designing safer drugs that do not block the hNa_v1.5 channel.

Keywords: cardiotoxicity; channel blockers; hNav1.5; sodium ion channel; steered molecular dynamics; voltage-gated sodium channel.

MeSH terms

Binding Sites
Drug Design
Humans
Models, Anatomic*
Molecular Dynamics Simulation*
NAV1.5 Voltage-Gated Sodium Channel / chemistry
NAV1.5 Voltage-Gated Sodium Channel / metabolism*
Permeability
Sodium / metabolism
Static Electricity

Substances

NAV1.5 Voltage-Gated Sodium Channel
SCN5A protein, human
Sodium