Axon voltage-clamp simulations. A multicellular preparation.

F Ramón, N Anderson, R W Joyner and J W Moore

ABSTRACT

In this paper we extend the simulation of the voltage clampof a single nerve fiber to a bundle of axons. These simulationsincluded not only the description of the voltage clamp circuitand a single unidimensional cable to represent the preparationin the "node" region of a double sucrose gap used previouslybut also a series resistance and a shunt pathway. The outputof the voltage control amplifier is applied across the membraneplus the series resistance, producing a voltage drop acrossthe series resistance due to the current generated by the membranein response to a depolarizing voltage step. Since the membranecurrent has an inward and an outward phase, voltage drops ofopposite sign are produced across the series resistance. Duringthe transient current and at all points along an axon, the potentialdeviation produced by the series resistance is opposite to thedeviation produced by the longitudinal gradient. Only at a commandpotential equal to the sodium equilibrium potential, the membranepotential transiently matches the command potential. For theattempted voltage clamp of an axon, values of series resistancelarger than 50 omega-cm2 allowed propagated action potentialsin the membrane. In spite of the presence of propagated actionpotentials at the calbe membrane, the recorded current doesnot show "notches" and it has a phase of inward current anda phase of outward current. It is concluded that, in a multicellularpreparation with series resistance, the recording of a squarevoltage pulse does not indicate voltage control of the transmembranepotential. The presence of a shunt pathway produces inaccuratevalues of current density. Neither series or shunt resistanceproduce "notches" in the current records.

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