Urinary S100B Protein Concentrations Are Increased in Intrauterine Growth-Retarded Newborns

Author:

Florio Pasquale1,Marinoni Emanuela2,Di Iorio Romolo2,Bashir Moataza3,Ciotti Sabina4,Sacchi Renata4,Bruschettini Matteo4,Lituania Mario4,Serra Giovanni4,Michetti Fabrizio5,Petraglia Felice1,Gazzolo Diego46

Affiliation:

1. Department of Pediatrics, Obstetrics, and Reproductive Medicine, University of Siena, Siena, Italy

2. Laboratory of Perinatal Medicine and Molecular Biology, Department of Obstetrics and Neonatal Health, “La Sapienza” University, Rome, Italy

3. Department of Neonatology, University Hospital, Cairo, Egypt

4. Department of Pediatrics, Obstetrics and Gynecology, and Neuroscience, Giannina Gaslini Children's University Hospital, Genoa, Italy

5. Institute of Anatomy and Cell Biology, Catholic University, Rome, Italy

6. Department of Fetal and Neonatal Medicine, G. Garibuldi Hospital, Catania, Italy

Abstract

BACKGROUND. Intrauterine growth retardation is one of the major causes of perinatal mortality and morbidity. To date, there are no reliable methods to detect brain damage in these patients. METHODS. We conducted a case-control study in tertiary NICUs from December 2001 to December 2003 with 42 intrauterine growth retardation infants and 84 controls. Routine laboratory variables, neurologic outcome at 7-day follow-up, ultrasound imaging, and urine concentrations of S100B protein were determined at 5 time points. Urine S100B levels were measured by an immunoluminometric assay at first urination, 24, 48, and 72 hours, and 7 days after birth. Routine laboratory parameters and neurologic patterns were assessed at the same time as urine sampling. RESULTS. S100B protein was significantly higher at all of the monitoring time points in urine taken from intrauterine growth retardation newborns than in control infants. When intrauterine growth retardation infants were corrected for the presence of abnormal (group A) or normal (group B) neurologic examination 7 days after birth, S100B was significantly higher at all of the predetermined monitoring time points in group A infants than in group B or controls. At a cutoff of 7.37 multiples of median at first urination, S100B achieved a sensitivity of 95% and a specificity of 99.1% as a single marker for predicting an adverse neurologic outcome. Twenty of 126 patients had neurologic abnormalities, making an overall prevalence of the disease in our population of 15.9% (pretest probability). With respect to the performance of S100B in predicting brain damage, its positive and negative predictive values were 91.0% and 99.0%, respectively. CONCLUSIONS. Increased urine S100B protein levels in intrauterine growth retardation newborns in the first week after birth suggest the presence of brain damage reasonably because of intrauterine hypoxia. Longitudinal S100B protein measurements soon after birth are a useful tool to identify which intrauterine growth retardation infants are at risk of possible neurologic sequelae.

Publisher

American Academy of Pediatrics (AAP)

Subject

Pediatrics, Perinatology, and Child Health

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