2020
DOI: 10.3389/fphar.2020.00587
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A Physiology-Based Pharmacokinetic Framework to Support Drug Development and Dose Precision During Therapeutic Hypothermia in Neonates

Abstract: undergoing hypothermia are under investigation, all in need for dosing guidance. Furthermore, the hypothermia PBPK framework can be used to develop temperaturedriven PBPK models for other populations or indications. The applicability of the proposed workflow and the challenges in the development of the PBPK framework are illustrated for midazolam as model drug.

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Cited by 32 publications
(46 citation statements)
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References 129 publications
(192 reference statements)
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“…However, such findings need to be integrated with isoenzyme-specific ontogeny in neonates. 12 The sum of excretion in the urine of both the intact substance and metabolites that have been produced by the liver, further metabolisation and excretion into bile, sweat, saliva or milk make up the C L . 12 If, for example, a substance is primarily cleared by excretion in the urine, renal function is the principal determinate of clearance.…”
Section: Open Accessmentioning
confidence: 99%
See 3 more Smart Citations
“…However, such findings need to be integrated with isoenzyme-specific ontogeny in neonates. 12 The sum of excretion in the urine of both the intact substance and metabolites that have been produced by the liver, further metabolisation and excretion into bile, sweat, saliva or milk make up the C L . 12 If, for example, a substance is primarily cleared by excretion in the urine, renal function is the principal determinate of clearance.…”
Section: Open Accessmentioning
confidence: 99%
“…12 The sum of excretion in the urine of both the intact substance and metabolites that have been produced by the liver, further metabolisation and excretion into bile, sweat, saliva or milk make up the C L . 12 If, for example, a substance is primarily cleared by excretion in the urine, renal function is the principal determinate of clearance. The Cochrane systematic review on TH could not observe any significant differences in urine output in neonates who underwent TH compared with those who did not.…”
Section: Open Accessmentioning
confidence: 99%
See 2 more Smart Citations
“…This S cr variability is partly explained by maturational changes (e.g., birth weight, gestational age [GA], postnatal age) and non-maturational changes related to pathophysiology, e.g., perinatal asphyxia, co-medication, congenital anomalies of the kidney and urinary track (CAKUT), cardiac surgery with bypass, or extra-corporeal membrane oxygenation ( 4 , 5 ). Postnatal kidney adaptation is proportional to the nephron number (GA driven) and renal perfusion (postnatal adaptation, mean arterial blood pressure) ( 6 , 7 ). Nephrogenesis evolves as branching morphogenesis, similar to lung, pancreas, vascular tree, or retina.…”
Section: Introductionmentioning
confidence: 99%