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. 2015 Mar;47(3):117-24.
doi: 10.3109/00365548.2014.971053. Epub 2014 Dec 18.

Diagnostic utility of biomarkers for neonatal sepsis--a systematic review

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Diagnostic utility of biomarkers for neonatal sepsis--a systematic review

Sofie Sommer Hedegaard et al. Infect Dis (Lond). 2015 Mar.

Abstract

Neonatal sepsis is a major cause of morbidity and mortality. Early diagnosis and treatment of the neonate with suspected sepsis are essential to prevent life-threatening complications. Diagnosis of neonatal sepsis is a challenge due to non-specific clinical signs and the fact that infection markers are difficult to interpret in the first and critical phase of neonatal sepsis. The objective of the present study was to systematically evaluate existing evidence of the diagnostic utility of biomarkers for prediction of sepsis in neonates. We conducted a systematic literature search performed in PubMed and Embase. The study population was neonates with gestation age > 24 weeks in their first 28 days of life with suspected sepsis. The included manuscripts were rated due to criteria from a modified rating scale developed by Douglas Altman. Of 292 potentially relevant manuscripts, 77 fulfilled the inclusion and exclusion criteria; 16 (21%) were rated as high-quality studies. C-reactive protein (CRP) was the most extensively studied biomarker evaluated. The high-quality studies indicated that the acute phase protein serum amyloid A had high sensitivity, both at onset of symptoms and 2 days after. The studies evaluating serum amyloid A presented a variable positive predictive value (PPV, 0.67 and 0.92) with a high negative predictive value (NPV, 0.97 and 1.00). The existing evidence of the diagnostic value of serum amyloid A for neonatal sepsis showed promising results, and should be further investigated in clinical settings.

Keywords: C-reactive protein; CRP; Newborn; procalcitonin; serum amyloid A.

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Comment in

  • Ischemia modified albumin in early neonatal sepsis.
    Khashana A, Ayoub A, Younes S, Abdelrahman A. Khashana A, et al. Infect Dis (Lond). 2016;48(6):488-9. doi: 10.3109/23744235.2016.1153807. Epub 2016 Mar 1. Infect Dis (Lond). 2016. PMID: 27030922 No abstract available.

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