早产儿粪便钙保护蛋白水平的变化趋势及其与早期生活经历的关系。

Wanli Xu, Yiming Zhang, Wenxiao Zhao, Jie Chen, Kendra Maas, Naveed Hussain, Wendy A Henderson, Xiaomei Cong
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引用次数: 3

摘要

背景:由于早产儿免疫系统不成熟,他们有严重感染的风险。早期生活中的疼痛/压力经历和喂养等因素可能影响免疫系统的激活和成熟。然而,其潜在机制尚不清楚。粪钙保护蛋白(FCP)是胃肠道粘膜炎症的一种无创替代生物标志物,已被用于检测特定儿科胃肠道疾病的肠道炎症。目的:描述早产儿FCP水平的纵向轨迹,并探讨与FCP水平相关的影响因素。设计:采用纵向研究设计。环境:从美国东北部儿童医疗中心的2个新生儿重症监护病房(NICU)招募早产儿。方法:对新生儿重症监护病房前4周早产儿进行随访。每周收集两次粪便样本以量化FCP水平。每天测量累积疼痛/应激体验和喂养类型。使用线性混合效应模型来检查FCP水平与人口统计学和临床特征、累积疼痛/压力和喂养之间的关系。结果:49例早产儿纳入研究。婴儿的FCP水平变化很大,平均为268.7±261.3µg/g,并随着时间的推移而增加。在新生儿重症监护病房期间,早产儿平均每天经历7.5±5.0个急性疼痛过程和15.3±20.8个慢性疼痛过程。自出生后第1周(57.1±36.5%)至第4周(60.7±38.9%),母乳平均百分比有所增加。FCP浓度升高与急性和累积(慢性)疼痛/压力水平、母乳、非白种人和较高的疾病严重程度评分有关。结论:早产儿FCP水平升高具有广泛的个体间和个体内差异。NICU住院期间的累积疼痛/应激、喂养、种族和健康状况可能影响生命早期FCP浓度,这可能与炎症性肠道过程有关。
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Trends of fecal calprotectin levels and associations with early life experience in preterm infants.

Background: Preterm infants are at risk for severe infections due to their immature immune systems. Factors such as early life pain/stress experiences and feeding may influence immune activation and maturation of immune systems. However, the underlying mechanism remains unclear. Fecal calprotectin (FCP) is a noninvasive surrogate biomarker of mucosal inflammation in the gastrointestinal tract and has been used in detecting intestinal inflammation in specific pediatric gastrointestinal disorders.

Objective: To describe the longitudinal trajectory of FCP levels in preterm infants and investigate the contributing factors that are associated with FCP levels.

Design: A longitudinal study design was used.

Settings: Preterm infants were recruited from 2 neonatal intensive care units (NICU) of a children's medical center in the North-eastern US.

Methods: Preterm infants were followed during their first 4 weeks of NICU hospitalization. Stool samples were collected twice per week to quantify the FCP levels. Cumulative pain/stress experiences and feeding types were measured daily. A linear mixed-effect model was used to examine the associations between FCP levels and demographic and clinical characteristics, cumulative pain/stress, and feeding over time.

Results: Forty-nine preterm infants were included in the study. Infants' FCP levels varied largely with a mean of 268.7±261.3 µg/g and increased over time. Preterm infants experienced an average of 7.5±5.0 acute painful procedures and 15.3±20.8 hours of chronic painful procedures per day during their NICU stay. The mean percentage of mother's own milk increased from the first week (57.1±36.5%) to the fourth week (60.7±38.9%) after birth. Elevated FCP concentration was associated with acute and cumulative (chronic) pain/stress levels, mother's own milk, non-White race, and higher severity of illness score.

Conclusions: FCP levels were elevated in preterm infants with wide interindividual and intraindividual variations. Cumulative pain/stress during the NICU hospitalization, feeding, race, and health status may influence FCP concentrations in early life that may be associated with inflammatory gut processes.

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