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血红蛋白和输血对早产儿肠道灌注及损伤的影响。

The effect of haemoglobin and blood transfusion on preterm infant gut perfusion and injury.

作者信息

Howarth Claire, Mifsud Christian, Banerjee Jayanta, Eaton Simon, Leung Terence, Fleming Paul, Morris Joan, Aladangady Narendra

机构信息

Neonatal Unit, Homerton Healthcare NHS Foundation Trust and Queen Mary University of London, London, England.

Great Ormond Street Institute of Child Health, University College London (UCL), London, England.

出版信息

Front Pediatr. 2024 Nov 22;12:1440537. doi: 10.3389/fped.2024.1440537. eCollection 2024.

Abstract

INTRODUCTION

There is significant uncertainty regarding the role that anaemia or red blood cell transfusion (RBCT) plays in the development of gut injury in preterm infants. This study evaluated Near Infrared Spectroscopy (NIRS) together with a range of known biomarkers of gut inflammation to identify their relationship with anaemia and RBCT.

METHOD

A prospective observational study of preterm infants born at <30 weeks gestation was conducted from birth until either 36 weeks post conceptional age or discharge home. Gut perfusion and biomarkers of gut injury were assessed weekly by: 60 min NIRS measurements (splanchnic tissue oxygenation index [sTOI] and fractional tissue oxygenation extraction [sFTOE]); stool calprotectin; urine intestinal and liver fatty acid binding proteins (I-FABPs and L-FABPs); and trefoil factor 3 (TFF-3). Exclusion criteria included Fetal Growth Restriction (FGR), and abnormal antenatal Dopplers. Haemoglobin (Hb) levels were measured in parallel with NIRS measurements. NIRS, together with urine and stool biomarkers of gut injury, were evaluated up to 72 h pre/post RBCT and pre/post measurements compared.

RESULTS

Forty-eight infants were studied. Median (range) gestational age was 26   (23   to 29  ) weeks and birthweight 883.5 g (460-1,600). Seven (14.6%) infants developed ≥ Bells stage 2 NEC. 28 (58.3%), 5 (10.4%) and 24 (50%) infants had ECHO confirmed PDA, haemorrhagic parenchymal infarct (HPI) and IVH respectively. There were 22 episodes of sepsis. Infants were in the study for a median of 7.3 (1-13) weeks. There was no significant association between Hb divided into three categories (<80 g/L, 80-111.9 g/L and ≥120 g/L) or continuous values and sTOI, sFTOE or any of the gut injury biomarkers measured ( > 0.05). 283 RBCTs were administered; 117 (41.3%) within the first two weeks of life. Pre and post blood transfusion changes in splanchnic NIRS oxygenation, urine and stool gut injury biomarkers were measured in 165, 195 and 175 episodes of RBCT respectively. There was no significant post RBCT changes in splanchnic NIRS or gut injury biomarker levels ( > 0.05). However, post RBCT calprotectin was significantly reduced during the first 14 days of life (mean difference -114%, CI -185 to -42 & 0.002).

CONCLUSION

There was no association between anaemia or RBCT with NIRS measurements of tissue oxygen saturation and biomarkers of intestinal inflammation or gut injury in preterm infants enrolled in this study. Further studies with standardised methods of examining the relationship between anaemia, RBCT and gut injury are needed.

摘要

引言

关于贫血或红细胞输血(RBCT)在早产儿肠道损伤发展中所起的作用,存在很大的不确定性。本研究评估了近红外光谱(NIRS)以及一系列已知的肠道炎症生物标志物,以确定它们与贫血和RBCT的关系。

方法

对孕周小于30周的早产儿进行了一项前瞻性观察研究,从出生开始直至孕龄36周或出院回家。每周通过以下方式评估肠道灌注和肠道损伤生物标志物:60分钟的NIRS测量(内脏组织氧合指数[sTOI]和组织氧合分数提取率[sFTOE]);粪便钙卫蛋白;尿液肠道和肝脏脂肪酸结合蛋白(I-FABP和L-FABP);以及三叶因子3(TFF-3)。排除标准包括胎儿生长受限(FGR)和产前多普勒检查异常。在进行NIRS测量的同时测量血红蛋白(Hb)水平。在RBCT前/后72小时内评估NIRS以及尿液和粪便肠道损伤生物标志物,并比较测量前后的结果。

结果

研究了48名婴儿。中位(范围)孕周为26(23至29)周,出生体重为883.5克(460 - 1600克)。7名(14.6%)婴儿发生了≥贝尔2期坏死性小肠结肠炎。28名(58.3%)、5名(10.4%)和24名(50%)婴儿分别经超声心动图证实患有动脉导管未闭、出血性实质梗死(HPI)和脑室内出血。发生了22次败血症发作。婴儿参与研究的中位时间为7.3(1 - 13)周。分为三类(<80克/升、80 - 111.9克/升和≥120克/升)或连续值的Hb与sTOI、sFTOE或所测量的任何肠道损伤生物标志物之间均无显著关联(>0.05)。共进行了283次RBCT;其中117次(41.3%)在出生后的头两周内进行。分别在165次、195次和175次RBCT过程中测量了输血前后内脏NIRS氧合、尿液和粪便肠道损伤生物标志物的变化。RBCT后内脏NIRS或肠道损伤生物标志物水平无显著变化(>0.05)。然而,在出生后的前14天内,RBCT后钙卫蛋白显著降低(平均差异 - 114%,CI - 185至 - 42,P = 0.002)。

结论

在本研究纳入的早产儿中,贫血或RBCT与组织氧饱和度的NIRS测量以及肠道炎症或肠道损伤生物标志物之间无关联。需要采用标准化方法进一步研究贫血、RBCT与肠道损伤之间的关系。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d13e/11620877/3d24bd8318c6/fped-12-1440537-g001.jpg

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