1997
DOI: 10.1007/s002280050250
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Disopyramide concentrations in human plasma and saliva: Comparison of disopyramide concentrations in saliva and plasma unbound concentrations

Abstract: Disopyramide concentrations in saliva correlated well with plasma unbound concentrations on the elimination phase.

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Cited by 7 publications
(6 citation statements)
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“…However, actual bioavailability in vivo is less than this due to pharmacokinetic factors such as plasma protein binding. 1 and 2 μM of disopyramide and quinidine likely constitute realistic maximal unbound concentrations (Sagawa et al, 1997 ). To encompass likely total as well as unbound concentrations, we elected to simulate effects of a wide range of concentrations of both agents (0.2–20 μM) at the single cell level, and a narrower set of more “clinically-relevant” concentrations (1, 2, 5, 10 μM) at the tissue level (represented by light blue shaded regions on dose-response curves in Figures 1 , 2 ).…”
Section: Methodsmentioning
confidence: 99%
“…However, actual bioavailability in vivo is less than this due to pharmacokinetic factors such as plasma protein binding. 1 and 2 μM of disopyramide and quinidine likely constitute realistic maximal unbound concentrations (Sagawa et al, 1997 ). To encompass likely total as well as unbound concentrations, we elected to simulate effects of a wide range of concentrations of both agents (0.2–20 μM) at the single cell level, and a narrower set of more “clinically-relevant” concentrations (1, 2, 5, 10 μM) at the tissue level (represented by light blue shaded regions on dose-response curves in Figures 1 , 2 ).…”
Section: Methodsmentioning
confidence: 99%
“…The class I AADs investigated here included disopyramide, quinidine, and propafenone. Taking into account plasma protein binding, estimates of the most likely unbound concentrations of propafenone, disopyramide, and quinidine have been given as~0.15-1 µM [85][86][87], 1 µM, and 2 µM [88], respectively. To encompass the likely total as well as unbound concentrations, we chose to simulate the effects of a wide range of concentrations of propafenone (low dose Prop_L: 0.2, medium dose Prop_M: 0.5, and high dose Prop_H: 0.8 µM), disopyramide (Diso_L: 1.0, Diso_M: 2.0, and Diso_H: 5.0 µM), and quinidine (Quin_L: 1.0, Quin_M: 2.0, and Quin_H: 5.0 µM) [37,89].…”
Section: Antiarrhythmic Effects Of Class I Drugs On Dvdt Max and Apd mentioning
confidence: 99%
“…Class I AADs investigated here included disopyramide, quinidine and propafenone. Taking into account plasma protein binding, estimates of the most likely unbound concentrations of propafenone, disopyramide and quinidine have been given as ~0.15-1 μM [83][84][85], 1 μM and 2 μM [86], respectively. To encompass likely total as well as unbound concentrations, we selected to simulate effects of a wide range of concentration of propafenone (low dose Prop_L: 0.2, medium dose Prop_M: 0.5 and high dose Prop_H: 0.8 μM), disopyramide (Diso_L: 1.0, Diso_M: 2.0 and Diso_H: 5.0 μM) and quinidine (Quin_L: 1.0, Quin_M: 2.0 and Quin_H: 5.0 μM) [37,87].…”
Section: Antiarrhythmic Effects Of Class I Drugs On Dvdtmax and Apd90mentioning
confidence: 99%