Impact of Gestational Age and Birth Weight on Amikacin Clearance on Day 1 of Life

Schreuder, Michiel F.; Wilhelm, Andrew; Bökenkamp, Arend; Timmermans, S.M.H.; Waal, Henriëtte A. Delemarre-van de; Wijk, J. A. E. van

doi:10.2215/cjn.02230409

Cited by 40 publications

(35 citation statements)

References 41 publications

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“…Indeed, GFR extrapolated from Amikacin clearance on day 1 of life, preceding any compensatory adaptation, was significantly reduced in premature and LBW infants compared to term controls 67 . GFR measured by inulin clearance was significantly lower at age 7.6 years in children who had been premature and had severe growth restriction compared to non growth restricted controls 41 .…”

Section: Renal Function Birth Weight and Nephron Massmentioning

confidence: 92%

Effect of fetal and child health on kidney development and long-term risk of hypertension and kidney disease

et al. 2013

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Developmental programming of non-communicable diseases is now an established paradigm. With respect to hypertension and chronic kidney disease, adverse events experienced in utero can affect development of the fetal kidney and reduce final nephron number. Low birth weight and prematurity are the most consistent clinical surrogates for a low nephron number, and are associated with increased risk of hypertension, proteinuria and kidney disease in later life. Rapid weight gain in childhood or adolescence further compounds these risks. Low birth weight, prematurity and rapid childhood weight gain should alert clinicians to an individual's life-long risk of hypertension and kidney disease, prompting education to minimize additional risk factors and ensuring follow-up. Birth weight and prematurity are significantly impacted by maternal nutrition and health during pregnancy. Optimization of maternal health and early childhood nutrition could therefore attenuate this programming cycle and reduce the global burden of hypertension and kidney disease in the future.

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Section: Renal Function Birth Weight and Nephron Massmentioning

confidence: 92%

Effect of fetal and child health on kidney development and long-term risk of hypertension and kidney disease

et al. 2013

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“…119 In longer term follow-up of children with very low birth weight (VLBW; Ͻ1000 g), serum creatinine was higher and GFR lower compared with age-matched NBW children at 6 to 12 years. 120 A stronger association was found using cystatin C in children, suggesting that creatinine-based formulas underestimate the impact of birth weight on GFR.…”

Section: Measures Of Renal Functionmentioning

confidence: 98%

The Clinical Importance of Nephron Mass

Luyckx

Brenner²

2010

Journal of the American Society of Nephrology

277

243

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“…Previous studies indicated that amikacin CL was in the range of 31.3 -91 ml/h·kg, while half-life (t 1/2 ) was in the range of 4 -9.3 h (8, 11 -13, 21). High interindividual variability in amikacin pharmacokinetics was previously observed, and it was described in detail in pre-term neonates (9,11,22). In pre-term neonates, weight and gestational and/or neonatal age significantly contributed to amikacin pharmacokinetic variability (9,10,23).…”

Section: Introductionmentioning

confidence: 82%

Pharmacokinetic Variability of Amikacin After Once-Daily and Twice-Daily Dosing Regimen in Full-Term Neonates

Vučićević¹,

Rakonjac

Miljković³

et al. 2014

J Pharmacol Sci

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Abstract. The purpose of the study was to compare peak (C peak ) and trough (C trough ) amikacin levels after twice-daily (TD) or once-daily dosing (OD) in full-term neonates. Additionally, the study aimed to address amikacin pharmacokinetics and its variability. Data included 31 patients born on term. Amikacin daily dose was 15 or 20 mg/kg depending on the neonate's age. Patients randomly received amikacin every 12 or 24 h. In all patients corresponding C peak and C trough were taken. Volume of distribution (Vd), clearance (CL) and half-life (t 1/2 ) were calculated. Mean C peak of 21.79 mg/ml in the TD group was statistically different from C peak of 36.39 mg/ml in the OD group. Average C trough in TD (5.67 mg/ml) was statistically different from the corresponding 3.99 mg/ml in the OD group. Mean amikacin Vd, CL, and t 1/2 were 0.78 ± 0.38 l/kg, 86.99 ± 48.22 ml/h•kg, and 6.81 ± 2.51 h, respectively. High interindividual pharmacokinetic variability was observed. Further analysis showed that neonatal age contributed to the pharmacokinetic parameters' values. Statistically significant difference in CL and t 1/2 was observed between patients age ≤ 2 and > 2 days on therapy initiation. As expected, amikacin given OD achieved higher C peak and lower C trough than TD. Based on the results, observed variability in amikacin pharmacokinetics was possibly due to the renal maturation process.

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Impact of Gestational Age and Birth Weight on Amikacin Clearance on Day 1 of Life

Cited by 40 publications

References 41 publications

Effect of fetal and child health on kidney development and long-term risk of hypertension and kidney disease

Effect of fetal and child health on kidney development and long-term risk of hypertension and kidney disease

The Clinical Importance of Nephron Mass

Pharmacokinetic Variability of Amikacin After Once-Daily and Twice-Daily Dosing Regimen in Full-Term Neonates

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