TY - JOUR
T1 - General anesthetics directly inhibit electron mobility
T2 - dipole dispersion theory of anesthetic action.
AU - Hameroff, S. R.
AU - Watt, R. C.
AU - Borel, J. D.
AU - Carlson, G.
PY - 1982
Y1 - 1982
N2 - A model system of gaseous electron mobility, excitation, and plasma activity was used to study direct effects of six gases, including four general anesthetics, in oxygen. Helium increased, and nitrogen had minimal effects on gaseous excitation. Nitrous oxide, as well as the potent anesthetics halothane, enflurane, and isoflurane, inhibited gaseous excitation, nitrous oxide having the weakest anesthetic effect. The data are compatible with the view that anesthetic inhibition is mediated by Van der Waals dipole dispersion interactions among anesthetic molecules (e.g., halogenated hydrocarbons) and electrons accelerated by the applied field. Dipole dispersion interactions may also mediate anesthetic effects on synaptic protein conformational control.
AB - A model system of gaseous electron mobility, excitation, and plasma activity was used to study direct effects of six gases, including four general anesthetics, in oxygen. Helium increased, and nitrogen had minimal effects on gaseous excitation. Nitrous oxide, as well as the potent anesthetics halothane, enflurane, and isoflurane, inhibited gaseous excitation, nitrous oxide having the weakest anesthetic effect. The data are compatible with the view that anesthetic inhibition is mediated by Van der Waals dipole dispersion interactions among anesthetic molecules (e.g., halogenated hydrocarbons) and electrons accelerated by the applied field. Dipole dispersion interactions may also mediate anesthetic effects on synaptic protein conformational control.
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M3 - Article
C2 - 7185051
AN - SCOPUS:0020407445
SN - 0031-9325
VL - 14
SP - 183
EP - 187
JO - Physiological chemistry and physics
JF - Physiological chemistry and physics
IS - 3
ER -