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W2084804585 abstract "Objectives To test the hypothesis that an exploratory proteomics analysis of urine proteins with subsequent development of validated urine biomarker panels would produce molecular classifiers for both the diagnosis and prognosis of infants with necrotizing enterocolitis (NEC). Study design Urine samples were collected from 119 premature infants (85 NEC, 17 sepsis, 17 control) at the time of initial clinical concern for disease. The urine from 59 infants was used for candidate biomarker discovery by liquid chromatography/mass spectrometry. The remaining 60 samples were subject to enzyme-linked immunosorbent assay for quantitative biomarker validation. Results A panel of 7 biomarkers (alpha-2-macroglobulin-like protein 1, cluster of differentiation protein 14, cystatin 3, fibrinogen alpha chain, pigment epithelium-derived factor, retinol binding protein 4, and vasolin) was identified by liquid chromatography/mass spectrometry and subsequently validated by enzyme-linked immunosorbent assay. These proteins were consistently found to be either up- or down-regulated depending on the presence, absence, or severity of disease. Biomarker panel validation resulted in a receiver-operator characteristic area under the curve of 98.2% for NEC vs sepsis and an area under the curve of 98.4% for medical NEC vs surgical NEC. Conclusions We identified 7 urine proteins capable of providing highly accurate diagnostic and prognostic information for infants with suspected NEC. This work represents a novel approach to improving the efficiency with which we diagnose early NEC and identify those at risk for developing severe, or surgical, disease. To test the hypothesis that an exploratory proteomics analysis of urine proteins with subsequent development of validated urine biomarker panels would produce molecular classifiers for both the diagnosis and prognosis of infants with necrotizing enterocolitis (NEC). Urine samples were collected from 119 premature infants (85 NEC, 17 sepsis, 17 control) at the time of initial clinical concern for disease. The urine from 59 infants was used for candidate biomarker discovery by liquid chromatography/mass spectrometry. The remaining 60 samples were subject to enzyme-linked immunosorbent assay for quantitative biomarker validation. A panel of 7 biomarkers (alpha-2-macroglobulin-like protein 1, cluster of differentiation protein 14, cystatin 3, fibrinogen alpha chain, pigment epithelium-derived factor, retinol binding protein 4, and vasolin) was identified by liquid chromatography/mass spectrometry and subsequently validated by enzyme-linked immunosorbent assay. These proteins were consistently found to be either up- or down-regulated depending on the presence, absence, or severity of disease. Biomarker panel validation resulted in a receiver-operator characteristic area under the curve of 98.2% for NEC vs sepsis and an area under the curve of 98.4% for medical NEC vs surgical NEC. We identified 7 urine proteins capable of providing highly accurate diagnostic and prognostic information for infants with suspected NEC. This work represents a novel approach to improving the efficiency with which we diagnose early NEC and identify those at risk for developing severe, or surgical, disease." @default.
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W2084804585 date "2014-03-01" @default.
W2084804585 modified "2023-10-16" @default.
W2084804585 title "Urine Protein Biomarkers for the Diagnosis and Prognosis of Necrotizing Enterocolitis in Infants" @default.
W2084804585 cites W130487724 @default.
W2084804585 cites W1963808434 @default.
W2084804585 cites W1966660127 @default.
W2084804585 cites W1973651409 @default.
W2084804585 cites W1975753137 @default.
W2084804585 cites W1994340698 @default.
W2084804585 cites W1999237504 @default.
W2084804585 cites W2001795292 @default.
W2084804585 cites W2007241626 @default.
W2084804585 cites W2010268287 @default.
W2084804585 cites W2012611711 @default.
W2084804585 cites W2013994985 @default.
W2084804585 cites W2015250987 @default.
W2084804585 cites W2019011307 @default.
W2084804585 cites W2019549525 @default.
W2084804585 cites W2023950153 @default.
W2084804585 cites W2025503906 @default.
W2084804585 cites W2033081843 @default.
W2084804585 cites W2035018358 @default.
W2084804585 cites W2035413290 @default.
W2084804585 cites W2039698305 @default.
W2084804585 cites W2040692501 @default.
W2084804585 cites W2044903961 @default.
W2084804585 cites W2050684827 @default.
W2084804585 cites W2067548751 @default.
W2084804585 cites W2074089196 @default.
W2084804585 cites W2075652947 @default.
W2084804585 cites W2076025706 @default.
W2084804585 cites W2080298716 @default.
W2084804585 cites W2080706671 @default.
W2084804585 cites W2090242046 @default.
W2084804585 cites W2090277531 @default.
W2084804585 cites W2104960492 @default.
W2084804585 cites W2106447783 @default.
W2084804585 cites W2108581239 @default.
W2084804585 cites W2109881724 @default.
W2084804585 cites W2110033245 @default.
W2084804585 cites W2116519404 @default.
W2084804585 cites W2118991879 @default.
W2084804585 cites W2124012609 @default.
W2084804585 cites W2134713747 @default.
W2084804585 cites W2145126338 @default.
W2084804585 cites W4322703183 @default.
W2084804585 doi "https://doi.org/10.1016/j.jpeds.2013.10.091" @default.
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