Human voltage-gated sodium channel mutations that cause inherited neuronal and muscle channelopathies increase resurgent sodium currents
Brian W. Jarecki, … , James O. Jackson II, Theodore R. Cummins
Brian W. Jarecki, … , James O. Jackson II, Theodore R. Cummins
Published December 28, 2009
Citation Information: J Clin Invest. 2010;120(1):369-378. https://doi.org/10.1172/JCI40801.
View: Text | PDF
Research Article

Human voltage-gated sodium channel mutations that cause inherited neuronal and muscle channelopathies increase resurgent sodium currents

Abstract

Inherited mutations in voltage-gated sodium channels (VGSCs; or Nav) cause many disorders of excitability, including epilepsy, chronic pain, myotonia, and cardiac arrhythmias. Understanding the functional consequences of the disease-causing mutations is likely to provide invaluable insight into the roles that VGSCs play in normal and abnormal excitability. Here, we sought to test the hypothesis that disease-causing mutations lead to increased resurgent currents, unusual sodium currents that have not previously been implicated in disorders of excitability. We demonstrated that a paroxysmal extreme pain disorder (PEPD) mutation in the human peripheral neuronal sodium channel Nav1.7, a paramyotonia congenita (PMC) mutation in the human skeletal muscle sodium channel Nav1.4, and a long-QT3/SIDS mutation in the human cardiac sodium channel Nav1.5 all substantially increased the amplitude of resurgent sodium currents in an optimized adult rat–derived dorsal root ganglion neuronal expression system. Computer simulations indicated that resurgent currents associated with the Nav1.7 mutation could induce high-frequency action potential firing in nociceptive neurons and that resurgent currents associated with the Nav1.5 mutation could broaden the action potential in cardiac myocytes. These effects are consistent with the pathophysiology associated with the respective channelopathies. Our results indicate that resurgent currents are associated with multiple channelopathies and are likely to be important contributors to neuronal and muscle disorders of excitability.

Authors

Brian W. Jarecki, Andrew D. Piekarz, James O. Jackson II, Theodore R. Cummins

×

Figure 2

Resurgent currents are produced by recombinant Nav1.7 channels expressed in DRG neurons.

Options: View larger image (or click on image) Download as PowerPoint
Resurgent currents are produced by recombinant Nav1.7 channels expressed...
(A and B) Representative current traces recorded from DRG neurons expressing Nav1.7r that did not (A) and that did (B) generate resurgent currents. (C and D) Representative current traces recorded from DRG neurons expressing Nav1.7r-I1461T channels that did not (C) and that did (D) generate resurgent currents. Resurgent currents were larger on average for Nav1.7r-I1461T than for Nav1.7 channels. Currents are magnified ×30 relative to the peak transient current (elicited with a pulse to –10 mV) to emphasize the resurgent current components. (E) Resurgent current voltage protocol. (F) Voltage dependence of resurgent current shown in D.