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Determination of the MRI contrast agent concentration time course in vivo following bolus injection: Effect of equilibrium transcytolemmal water exchange
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Citations
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References
2000
Year
Bolus InjectionEngineeringImaging AgentBiomedical EngineeringPhysiologically-based Pharmacokinetic ModelingRat Thigh MuscleMagnetic Resonance ImagingTransport PhenomenaApplied PhysiologyClinical ChemistryFast ExchangeBiophysicsRadiologyPharmacokinetic ModelingMedical ImagingMedicineContrast AgentCerebral Blood FlowMri-guided Radiation TherapyPharmacologyPhysiologyBiomedical ImagingElectrophysiologyCr ConcentrationChemical KineticsPharmacokinetics
For bolus-tracking studies, it is commonly assumed that CR concentration bears a linear relationship with the measured (usually longitudinal) (1)H(2)O relaxation rate constant, R*(1) identical with(T(1) *)(-1). This requires that equilibrium transcytolemmal water exchange be in the fast exchange limit (FXL). However, though systems remain in fast exchange, the FXL will not usually obtain. Here, the consequences are considered: 1) the measurement of R(1) * itself can be affected, 2) the resultant non-linear [CR]-dependence causes significant error by assuming FXL, 3) the thermodynamic [CR] (based on the space in which CR is actually distributed) can be determined, 4) transcytolemmal water permeability may be estimated, and 5) the pharmacokinetic parameters can be factored. For a 30-sec, 0.17 mmol/kg dose of GdDTPA(2-), the FXL assumption underestimates the [CR] maximum in rat thigh muscle by a factor of almost two. Similar results are obtained for a rat brain GS-9L gliosarcoma tumor model.
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