TY - JOUR
T1 - Intestinal fatty-acid binding protein and metronidazole response in premature infants
AU - Best Pharmaceuticals for Children Act - Pediatric Trials Network Administrative Core Committee
AU - Sampson, M. R.
AU - Bloom, B. T.
AU - Arrieta, A.
AU - Capparelli, E.
AU - Benjamin, D. K.
AU - Smith, P. B.
AU - Kearns, G. L.
AU - Van Den Anker, J.
AU - Cohen-Wolkowiez, Michael
AU - Berezny, Katherine Y.
AU - Barrett, Jeffrey
AU - Laughon, Matthew
AU - Muelenaer, Andre
AU - O'Shea, T. Michael
AU - Paul, Ian M.
AU - Wade, Kelly
AU - Walsh, Thomas J.
AU - Siegel, David
AU - Taylor-Zapata, Perdita
AU - Zajicek, Anne
AU - Pagan, Alice
AU - Anand, Ravinder
AU - Clemons, Traci
AU - Simone, Gina
N1 - Publisher Copyright:
© 2014 - IOS Press and the authors. All rights reserved.
PY - 2014
Y1 - 2014
N2 - OBJECTIVES: In premature infants with suspected intra-abdominal infection, biomarkers for treatment response to antimicrobial therapy are lacking. Intestinal fatty acid-binding protein (I-FABP) is specific to the enterocyte and is released in response to intestinal mucosal injury. I-FABP has not been evaluated as a surrogate marker of disease response to antimicrobial therapy. We examined the relationship between metronidazole exposure and urinary I-FABP concentrations in premature infants with suspected intra-abdominal infection. STUDY DESIGN: We conducted an intravenous metronidazole pharmacokinetic study, collecting ≤3 urine samples per infant for I-FABP concentration measurements. We analyzed the relationship between I-FABP concentrations and measures of metronidazole exposure and pharmacokinetics, maturational factors, and other covariates. RESULTS: Twenty-six samples from 19 premature infants were obtained during metronidazole treatment. When analyzed without regard to presence of necrotic gastrointestinal disease, there were no significant associations between predictor variables and I-FABP concentrations. However, when the sample was limited to premature infants with necrotic gastrointestinal disease, an association was found between average predicted metronidazole concentration and I-FABP concentration (p = 0.006). CONCLUSION: While a predictive association between urinary I-FABP and metronidazole systemic exposure was not observed, the data suggest the potential of this endogenous biomarker to serve as a pharmacodynamic surrogate for antimicrobial treatment of serious abdominal infections in neonates and infants.
AB - OBJECTIVES: In premature infants with suspected intra-abdominal infection, biomarkers for treatment response to antimicrobial therapy are lacking. Intestinal fatty acid-binding protein (I-FABP) is specific to the enterocyte and is released in response to intestinal mucosal injury. I-FABP has not been evaluated as a surrogate marker of disease response to antimicrobial therapy. We examined the relationship between metronidazole exposure and urinary I-FABP concentrations in premature infants with suspected intra-abdominal infection. STUDY DESIGN: We conducted an intravenous metronidazole pharmacokinetic study, collecting ≤3 urine samples per infant for I-FABP concentration measurements. We analyzed the relationship between I-FABP concentrations and measures of metronidazole exposure and pharmacokinetics, maturational factors, and other covariates. RESULTS: Twenty-six samples from 19 premature infants were obtained during metronidazole treatment. When analyzed without regard to presence of necrotic gastrointestinal disease, there were no significant associations between predictor variables and I-FABP concentrations. However, when the sample was limited to premature infants with necrotic gastrointestinal disease, an association was found between average predicted metronidazole concentration and I-FABP concentration (p = 0.006). CONCLUSION: While a predictive association between urinary I-FABP and metronidazole systemic exposure was not observed, the data suggest the potential of this endogenous biomarker to serve as a pharmacodynamic surrogate for antimicrobial treatment of serious abdominal infections in neonates and infants.
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U2 - 10.3233/NPM-1477013
DO - 10.3233/NPM-1477013
M3 - Article
C2 - 25318626
AN - SCOPUS:84909961897
SN - 1934-5798
VL - 7
SP - 223
EP - 228
JO - Journal of Neonatal-Perinatal Medicine
JF - Journal of Neonatal-Perinatal Medicine
IS - 3
ER -