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| Título : | Population pharmacokinetics of cyclosporine in mexican pediatric patients with renal transplants |
| Autor: | Zaruma Torres, Fausto Leonardo |
| Palabras clave : | Formulation
Tacrolimus
Renal transplant
Population pharmacokinetics
Paediatric |
| Área de conocimiento FRASCATI amplio: | 3. Ciencias Médicas y de la Salud |
| Área de conocimiento FRASCATI detallado: | 3.1.5 Farmacología y Farmacia |
| Área de conocimiento FRASCATI específico: | 3.1 Medicina Básica |
| Área de conocimiento UNESCO amplio: | 09 - Salud y Bienestar |
| ÁArea de conocimiento UNESCO detallado: | 0916 - Farmacia |
| Área de conocimiento UNESCO específico: | 091 - Salud |
| Fecha de publicación : | 2013 |
| Volumen: | Volumen 80, número 4 |
| Fuente: | Clinical Pharmacology in Drug Development |
| metadata.dc.identifier.doi: | 10.1111/bcp.12649 |
| Editor: | Wiley |
| Ciudad: | Maryland |
| Tipo: | ARTÍCULO DE CONFERENCIA |
| Abstract: | Statement of Purpose, Innovation or Hypothesis: The purpose of
the study was to determine the population pharmacokinetic (PPK) of
cyclosporine (CsA) in children subjected to renal transplant.
Description of Methods and Materials: The study was conducted
from 1948 retrospective drug monitoring data points were collected
from 54 renal pediatric patients receiving CsA. For the structural model
(PPK) the MONOLIX 1 MLXTRANS program was used, the data were
fitted using a two-compartment model with first order kinetics. The
structural model was selected according to the best fit, according to
criteria of-2Log likelihood, Akaike and Bayesian models.
Data and Results: To assess the effect of covariates on the response
we carried out PPK correlation between parameters: Ka, Vd, K12, K21
and Ke with the variables of interest: age (months), sex, body mass index
(BMI, kg/m2), current weight (kg), comprising postoperative days
(POD), creatinine clearance (CrCl, mL/min), transplant rejection, and
nutritional status (NS). Population values obtained were Ka/F ¼ 0.157
0.049(h-1); Vd/F ¼ 0.323 0.064 (Vd/F/70Kg) (L); Ke/F ¼ 0.145
0.03 (h-1); K12 ¼ 7.58 23 (h-1) and K21 ¼ 26.3 79 (h-1). In
assessing the influence of covariates of interest on the PPK of CsA, it
was determined that the actual weight, the CrCl, the (RT) and (NS),
showed significant correlation with Vd, and consequently with the
CsACL, which determines interindividual variability. In order to
correct for the influence of variables over response, we used the
following equation: Vd/F/70 ¼ 0323-0508
(CrCl-74) -0539(WT-37.5)-0562 0566 POD-NS-0456
RT (L/70Kg).
Interpretation, Conclusion or Significance: In summary, the
population pharmacokinetics model developed for CsA after administration in pediatric renal transplant patients was validated. The model
obtained for CsA PPK can be useful for dose adjustment in pediatric
Mexican patients, aimed at achieving therapeutic optimization of CsA |
| URI : | https://dspace.ucuenca.edu.ec/handle/123456789/46214
https://accp1.onlinelibrary.wiley.com/doi/pdfdirect/10.1002/cpdd.62 |
| URI Fuente: | https://accp1.onlinelibrary.wiley.com/doi/10.1002/cpdd.62/abstract |
| ISBN : | 000-000-000-0 |
| ISSN : | 2160-763X, e 2160-7648 |
| Aparece en las colecciones: | Artículos
|
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