Simplified Dosing of Gentamicin for Treatment of Sepsis in Bangladeshi Neonates

Authors

  • M Monir Hossain Department of Neonatology, Bangladesh Institute of Child Health, Dhaka Shishu (Children?s) Hospital, Dhaka
  • Nazma A Chowdhury Department of Neonatology, Bangladesh Institute of Child Health, Dhaka Shishu (Children?s) Hospital, Dhaka
  • Mahfuza Shirin Department of Neonatology, Bangladesh Institute of Child Health, Dhaka Shishu (Children?s) Hospital, Dhaka
  • Samir K Saha Department of Microbiology, Bangladesh Institute of Child Health, Dhaka Shishu (Children?s) Hospital, Dhaka
  • Mary Miller-Bell Department of Pharmacology, Duke University, Durham, NC, USA
  • David Edwards Department of Pharmacy Practice, Wayne State University, Detroit, MI, USA, NIH/NICHD Pediatric Pharmacology Research Unit Network, Children?s Hospital of Michigan, Wayne State University, Detroit
  • Jacob Aranda NIH/NICHD Pediatric Pharmacology Research Unit Network, Children?s Hospital of Michigan, Wayne State University, Detroit
  • Patricia Coffey PATH, Seattle, WA, USA
  • Gary L Darmstadt International Center for Advancing Neonatal Health, Department of International Health, Bloomberg School of Medicine, Johns Hopkins University, Baltimore

DOI:

https://doi.org/10.3329/jhpn.v27i5.3640

Keywords:

Aminoglycoside, Antibiotics, Gentamicin, Infection, Newborns, Observational studies, Pharmacokinetics, Prospective studies, Sepsis, Bangladesh

Abstract

Extended-interval dosing of gentamicin has several advantages over conventional multiple-daily dosing for the treatment of sepsis. The study was conducted to evaluate the pharmacokinetics of gentamicin for the treatment of neonatal sepsis in predetermined doses at 24- or 48-hour intervals, according to weight category, and to develop a simplified protocol for use in peripheral healthcare settings in developing countries. This prospective observational study was conducted among 59 neonates admitted to the Special Care Nursery at Dhaka Shishu Hospital, Bangladesh, with suspected sepsis and treated with antibiotics, including gentamicin. Intravenous dosing of gentamicin according to weight category was: 10 mg every 48 hours if the infant weighed <2,000 g (n=23), 10 mg every 24 hours if the infant weighed 2,000-2,249 g (n=12), or 13.5 mg every 24 hours if the infant weighed 2,500-3,000 g (n=24). Peak and trough concentrations of gentamicin and the presence of signs of nephrotoxicity and ototoxicity were determined. The mean±standard deviation peak concentration of gentamicin was 12.3±3.7 ?g/mL in infants weighing <2,000 g, 9.6±3.1 ?g/mL in infants 2,000-2,249 g, and 10.0±3.4 ?g/mL in infants 2,500-3,000 g. Initial peak concentration of gentamicin was >12 ?g/mL in 28.8% and initial trough concentration was >2 ?g/mL in 6.8% of the subjects. No signs of nephrotoxicity or ototoxicity were detected. Favourable pharmacokinetic parameters found with the simplified dosing regimen suggest that it is safe for the treatment of neonatal sepsis.

J Health Popul Nutr 2009 Oct; 27(5):640-645

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Author Biography

Gary L Darmstadt, International Center for Advancing Neonatal Health, Department of International Health, Bloomberg School of Medicine, Johns Hopkins University, Baltimore

Dr. Gary L. Darmstadt
Director
International Center for Advancing Neonatal
Health
Department of International Health E-8153
Bloomberg School of Medicine
Johns Hopkins University
615 North Wolfe Street
Baltimore, MD 21205
USA
Email: gdarmsta@jhsph.edu
Fax: 410-614-1419

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How to Cite

Hossain, M. M., Chowdhury, N. A., Shirin, M., Saha, S. K., Miller-Bell, M., Edwards, D., Aranda, J., Coffey, P., & Darmstadt, G. L. (2009). Simplified Dosing of Gentamicin for Treatment of Sepsis in Bangladeshi Neonates. Journal of Health, Population and Nutrition, 27(5), 640–645. https://doi.org/10.3329/jhpn.v27i5.3640

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Original Papers