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首页> 外文期刊>Pediatric Research >The Influence of Gestation and Mechanical Ventilation on Serum Clara Cell Secretory Protein (CC10) Concentrations in Ventilated and Nonventilated Newborn Infants
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The Influence of Gestation and Mechanical Ventilation on Serum Clara Cell Secretory Protein (CC10) Concentrations in Ventilated and Nonventilated Newborn Infants

机译:妊娠和机械通气对通气和不通气新生儿的血清克拉拉细胞分泌蛋白(CC10)浓度的影响

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Clara cell secretory protein (CC10) is an important anti-inflammatory mediator in the adult lung, but its role in newborn pulmonary protection is uncertain. We examined the early postnatal behavior of CC10 in newborn serum and tracheal fluid and hypothesized that CC10 production is positively influenced by gestation. Blood from 165 infants from the first, third/fourth, and seventh days of life (gestational ages: 23–29 wk, 30–36 wk, >36 wk) and tracheal fluid (TF) from the first day of life from 32 ventilated infants were analyzed for CC10. Surfactant proteins A (SPA) and B (SPB) were also analyzed from the blood of a subgroup of infants. Serum CC10 on day 1 was highest in term infants (69.4 ng/mL), followed by moderately preterm (55.8 ng/mL), and then extremely preterm infants (median 42.1 ng/mL). Term infants also had higher tracheal fluid CC10 than preterm infants. (20.152 ng/mL versus 882 ng/mL). Mechanical ventilation increased serum CC10 only in moderately preterm infants, and only on d 1 [68.4 ng/mL versus 42.1 ng/mL (nonventilated moderately preterm infants)]. Serum CC10 decreased progressively by the end of the first week in all infants, in contrast to SPA and SPB, which increased. Our results show that CC10 is detectable in the blood of newborn infants and that a production surge occurs at birth. This surge is more pronounced in term infants and may confer them with superior extrauterine pulmonary protection compared with preterm infants.Abbreviations: CC10, Clara cell secretory protein; CLD, chronic lung disease; RDS, respiratory distress syndrome; SP, surfactant protein; TF, tracheal fluid; TTN, transient tachypnea of the newborn
机译:克拉拉细胞分泌蛋白(CC10)是成人肺中重要的抗炎介质,但其在新生儿肺保护中的作用尚不确定。我们检查了新生儿血清和气管液中CC10的早期产后行为,并假设CC10的产生受到妊娠的积极影响。出生后第一,第三/第四和第七天(胎龄:23-29 wk,30-36 wk,> 36 wk)的165名婴儿的血液和出生后第一天从32通风的气管液(TF)对婴儿进行了CC10分析。还从一个婴儿亚组的血液中分析了表面活性剂蛋白A(SPA)和B(SPB)。第一天的血清CC10在足月婴儿中最高(69.4 ng / mL),其次是中度早产(55.8 ng / mL),然后是极早产儿(中位数42.1 ng / mL)。足月儿的气管液CC10也比早产儿高。 (20.152 ng / mL对882 ng / mL)。机械通气仅在中度早产儿中增加血清CC10,仅在d 1时才升高[68.4 ng / mL对42.1 ng / mL(未通气的中度早产儿)]。与SPA和SPB升高相比,所有婴儿的血清CC10到第一周末逐渐降低。我们的结果表明,在新生儿的血液中可检测到CC10,并且出生时会出现生产激增。与早产儿相比,这种高潮在足月儿中更为明显,并且可能赋予他们优越的宫腔外肺部保护作用。 CLD,慢性肺病; RDS,呼吸窘迫综合征; SP,表面活性剂蛋白; TF,气管液; TTN,新生儿的短暂性呼吸急促

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