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先天性心脏病新生儿的红细胞生成改变。

Altered erythropoiesis in newborns with congenital heart disease.

机构信息

The Heart Institute, Cincinnati Children's Hospital Medical Center, Cincinnati, OH, USA.

Division of Hematology, Cincinnati Children's Hospital Medical Center, Cincinnati, OH, USA.

出版信息

Pediatr Res. 2022 Feb;91(3):606-611. doi: 10.1038/s41390-021-01370-4. Epub 2021 Feb 2.

Abstract

BACKGROUND

Fetal hypoxia has been implicated in fetal growth restriction in congenital heart disease (CHD) and leads to stress erythropoiesis in utero. The objective is to assess erythropoiesis and its association with growth in newborns with CHD.

METHODS

Fetuses with prenatally diagnosed CHD from 2013 to 2018 were retrospectively reviewed. Pregnancies with multiple gestation, genetic abnormalities, major extra-cardiac anomalies, and placental abruption were excluded. Complete blood count tests at birth were compared to published normative values. Spearman correlation assessed associations of red blood cell (RBC) indices with birth anthropometrics and prenatal Doppler measures.

RESULTS

A total of 160 newborns were included. Median gestational age was 38.3 (37.3, 39.0) weeks. Infants ≥37 weeks gestation had lower hemoglobin (Hgb), hematocrit, and elevated nucleated RBC (nRBC), mean corpuscular volume, and mean corpuscular hemoglobin compared to reference. No differences in RBC indices were observed in infants <34 and 34-37 weeks gestation. There was no difference in Hgb and nRBC between CHD subgroups. Neither Hgb nor nRBC were associated with birth anthropometrics or Doppler patterns.

CONCLUSIONS

Term infants with CHD demonstrated multiple alterations in erythrocyte indices suggesting ineffective stress erythropoiesis in late gestation resulting in lower Hgb at birth. Altered erythropoiesis was not correlated to growth or Doppler patterns.

IMPACT

Newborns with congenital heart disease (CHD) born at term gestation demonstrated altered erythropoiesis. Term newborns with CHD have decreased hemoglobin levels despite having red blood cell indices consistent with stress erythropoiesis, suggesting an incomplete compensatory response to in utero physiologic disturbances associated with CHD. The etiology is unknown; however, it may be influenced by multiple risk factors during pregnancy in the maternal-fetal dyad. Alterations in red blood cell indices were not associated with outcomes of fetal growth.

摘要

背景

胎儿缺氧与先天性心脏病(CHD)中的胎儿生长受限有关,并导致宫内应激性红细胞生成。目的是评估 CHD 新生儿的红细胞生成及其与生长的关系。

方法

回顾性分析 2013 年至 2018 年间产前诊断为 CHD 的胎儿。排除多胎妊娠、遗传异常、主要心脏外异常和胎盘早剥的妊娠。出生时的全血细胞计数检测与已发表的正常参考值进行比较。Spearman 相关分析评估 RBC 指数与出生人体测量学和产前多普勒测量值的相关性。

结果

共纳入 160 例新生儿。中位孕龄为 38.3(37.3,39.0)周。≥37 周的婴儿血红蛋白(Hgb)、血细胞比容和核红细胞(nRBC)升高,平均红细胞体积和平均红细胞血红蛋白均低于参考值。<34 周和 34-37 周的婴儿的 RBC 指数无差异。不同 CHD 亚组的 Hgb 和 nRBC 无差异。Hgb 和 nRBC 均与出生人体测量和多普勒模式无关。

结论

足月 CHD 婴儿的红细胞指数发生多种改变,提示晚期妊娠时无效的应激性红细胞生成导致出生时 Hgb 降低。红细胞生成的改变与生长或多普勒模式无关。

影响

足月出生的 CHD 新生儿表现出红细胞生成改变。尽管 CHD 新生儿的 RBC 指数与应激性红细胞生成一致,但血红蛋白水平降低,提示对与 CHD 相关的宫内生理紊乱的不完全代偿反应。其病因不明;然而,它可能受到母婴对子代中多种妊娠风险因素的影响。红细胞指数的改变与胎儿生长的结局无关。

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