Abstract
A physiologic pharmacodynamic model was developed to jointly characterize the effects of corticosteroid treatment on adrenal suppression and T-helper cell trafficking during single and multiple dosing in asthmatic patients Methylprednisolone (MP), cortisol, and T-helper cell concentrations obtained from a previously published study during single day and 6 days of multiple dosing MP treatment were examined. The formation and disposition kinetics of MP were described with a compartmental model. The biorhythmic profile of basal cortisol secretion rate was analyzed using a recent Fourier approach based on circadian harmonics. A three-compartment loop model was proposed to represent three major T-helper cell pools blood, extravascular site, and lymph nodes T-helper cell synthesis and degradation rate constants were obtained from the literature. The suppressive effects of cortisol and MP on T-helper cell concentrations were described with a joint additive inhibition function altering the cell migration rate from lymph nodes to blood. The model adequately described both plasma cortisol profiles and T-helper cells in blood after single and multiple doses of MP The potency of MP for suppression of cortisol secretion was estimated as IC50 = 0 8 ng/ml. The biorhythmic nature of the basal T-helper cells in blood was well described as under the influence of basal circadian cortisol concentrations with IC50 = 79 ng/ml. The model fitted potency of MP for suppression of T-helper cells was IC50 = 4 6 ng/ml The observed rebound of T-helper cells in blood can also be described by the proposed model The rhythm and suppression of plasma cortisol and T-helper cells before and during single and multiple dose MP treatment were adequately described by these extended indirect response models.
| Original language | English |
|---|---|
| Pages (from-to) | 559-575 |
| Number of pages | 17 |
| Journal | Journal of Pharmacokinetics and Biopharmaceutics |
| Volume | 27 |
| Issue number | 6 |
| DOIs | |
| State | Published - 1999 |
Keywords
- Circadian rhythm
- Corticosteroids
- Drug interactions
- Methylprednisolone
- Pharmacodynamics
- Pharmacokinetics
- Rebound
- T-helper cells
- Trafficking
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