足月和早产儿尿S-100B浓度有脑损伤风险。

Biology of the neonate Pub Date : 2006-01-01 Epub Date: 2005-12-06 DOI:10.1159/000090120
Katharina Ruetzler, Christoph Bührer, Ingrid Grimmer, Christian Müller, Nicole Nagdyman, Michael Obladen
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引用次数: 8

摘要

S-100B是星形胶质细胞中表达的一种21 kda蛋白,其血清浓度升高已被用于评估头部外伤、感染、缺血和围产期窒息后的脑损伤。目的:由于S-100B被肾脏清除,我们探讨了在严重围产期窒息新生儿和极低出生体重(VLBW)有神经发育障碍风险的早产儿尿液中检测S-100B的可行性。方法:首先对8例无重大医学问题的足月或近期新生儿进行尿样分析,然后对2例重度出生窒息的足月新生儿进行尿样分析,最后对8例VLBW(胎龄24-28周)新生儿每4 h采集一次尿样,为期10天。结果:8名没有重大医学问题的足月或近期新生儿的尿液S-100B浓度在出生第一天获得的样本中一致为微克/升(范围1.2-44.9微克/升,中位数为6.8微克/升)。出生后12 h尿液s - 100b峰值与胎龄呈负相关(R(s)=-0.882, p=0.009)。8名早产儿中有3名尿浓度峰值>0微克/升,但在1岁矫正年龄时没有脑损伤的超声迹象,也没有神经发育迟缓。结论:尿S-100B浓度的测定可能对重度窒息的足月儿有帮助,而早产儿尿S-100B浓度高可能是由于不成熟所致。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Urinary S-100B concentrations in term and preterm infants at risk for brain damage.

Background: Elevated serum concentrations of S-100B, a 21-kDa protein expressed in astroglial cells, has been used to assess cerebral damage after head trauma, infection, ischemia, and perinatal asphyxia.

Objective: As S-100B is eliminated by the kidneys, we investigated the feasibility of measuring S-100B in urine of newborns with severe perinatal asphyxia, and in very low birth weight (VLBW) preterm infants at risk for neurodevelopmental impairment.

Methods: We first analyzed urine samples of 8 term or near-term newborns without major medical problems, followed by urine samples of 2 term newborns with severe birth asphyxia, and finally urine samples of 8 VLBW (gestational age 24-28 weeks) infants collected every 4 h for up to 10 days.

Results: Urinary S-100B concentrations in 8 term or near-term newborns without major medical problems were consistently <1 microg/l. In 2 term newborns with severe asphyxia (Apgar 0/0/0 and 0/2/4) who subsequently had widespread cerebral damage on magnetic resonance imaging, peak urinary S-100B concentrations on the first day of life were 28.1 and 28.4 microg/l, respectively. In 5/8 VLBW infants, urinary S-100B was> microg/l in samples obtained on the first day of life (range 1.2-44.9 microg/l, median 6.8 microg/l). Peak S-100B in urine samples collected during the first 12 h of life were negatively related to gestational age (R(s)=-0.882, p=0.009). Three of the 8 preterm infants had peak urinary concentrations>0 microg/l but neither ultrasound signs of brain damage nor neurodevelopmental delay at 1 year corrected age.

Conclusions: The determination of urinary S-100B concentrations might be helpful in term infants with severe asphyxia, while high urinary S-100B concentrations in preterm infants are to be attributed to immaturity.

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