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Vol. 289, Issue 1, 8-13, April 1999
Temple University School of Medicine (R.J.T., J.D.M.) and
School of
Pharmacy (D.J.S., R.B.R.), Philadelphia, Pennsylvania
Graded doses of morphine sulfate and clonidine hydrochloride
were administered intrathecally to mice that were then tested for
antinociception in the 55°C tail immersion test. The dose-effect relations of each compound were used in calculations that permitted the
construction of a three-dimensional plot of the expected additive effect (vertical scale) against the planar domain of dose pairs representing combinations administered simultaneously. This additive response surface became the reference surface for viewing the actual
effects produced by three different fixed-ratio combinations of the
drugs that were used in our tests. Each combination produced effects
significantly greater than indicated by the additive surface, thereby
illustrating marked synergism and a method for quantifying the
synergism. This quantification, measured by the value of the interaction index (
), was found to be dependent on the fixed-ratio combination; accordingly, the actual response surface could not be
described by a single value of the index
. Furthermore, we found
that application of the common method of isoboles gave estimates of the
index that agreed well with those obtained from the more extensive
surface analysis. These results confirm earlier studies, which found
synergism for these drugs while also providing surface views of
additivity and synergism that form the basis of isobolographic analysis.
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