Abstract
Gain-of-function mutations of the voltage-gated sodium channel (VGSC) Nav1.7 have been linked to human pain disorders. The mutation F1449V, located at the intracellular end of transmembrane helix S6 of domain III, induces the inherited pain syndrome erythromelalgia. A kinetic model of wild-type (WT) and F1449V Nav1.7 may provide a basis for predicting putative intraprotein interactions. We semiautomatically constrained a Markov model using stochastic search algorithms and whole cell patch-clamp recordings from human embryonic kidney cells transfected with Nav1.7 and its F1449V mutation. The best models obtained simulated known differences in action potential thresholds and firing patterns in spinal sensory neurons expressing WT and F1449V. The most suitable Markov model consisted of three closed, one open, and two inactivated states. The model predicted that the F1449V mutation shifts occupancy of the closed states closer to the open state, making it easier for the channel pore to open. It also predicted that F1449V's second inactivated state is more than four times more likely to be occupied than the equivalent state in WT at hyperpolarized potentials, although the mutation still lowered the firing threshold of action potentials. The differences between WT and F1449V were not limited to a single transition. Thus a point mutation in position F1449, while phenotypically most probably affecting the activation gate, may also modify channel functions mediated by structures in more distant areas of the channel protein.
Original language | English |
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Pages (from-to) | 1546-1557 |
Number of pages | 12 |
Journal | Journal of Neurophysiology |
Volume | 105 |
Issue number | 4 |
Early online date | 2 Feb 2011 |
DOIs | |
State | Published - Apr 2011 |
Keywords
- Computer modeling
- Markov model
- Neuron
- Patch clamp
- Voltage-gated sodium channels
All Science Journal Classification (ASJC) codes
- General Neuroscience
- Physiology