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胎儿细胞因子平衡、促红细胞生成素和地中海贫血而非胎盘疟疾导致坦桑尼亚胎儿贫血风险增加。

Fetal Cytokine Balance, Erythropoietin and Thalassemia but Not Placental Malaria Contribute to Fetal Anemia Risk in Tanzania.

机构信息

Mother Offspring Malaria Studies (MOMS) Project, Seattle Biomedical Research Institute, Seattle, WA, United States.

School of Medicine, Muhimbili University of Health and Allied Sciences, Dar es Salaam, Tanzania.

出版信息

Front Immunol. 2021 Apr 30;12:624136. doi: 10.3389/fimmu.2021.624136. eCollection 2021.

Abstract

Fetal anemia is common in malaria-endemic areas and a risk factor for anemia as well as mortality during infancy. Placental malaria (PM) and red cell abnormalities have been proposed as possible etiologies, but the relationship between PM and fetal anemia has varied in earlier studies, and the role of red cell abnormalities has not been studied in malaria-endemic areas. In a Tanzanian birth cohort study designed to elucidate the pathogenesis of severe malaria in young infants, we performed a cross-sectional analysis of risk factors for fetal anemia. We determined PM status, newborn red cell abnormalities, and maternal and cord blood levels of iron regulatory proteins, erythropoietin (EPO), cytokines and cytokine receptors. We examined the relationship between these factors and fetal anemia. Fetal anemia was present in 46.2% of the neonates but was not related to PM. Maternal iron deficiency was common (81.6%), most frequent in multigravidae, and interacted with parity to modify risk of fetal anemia, but it was not directly related to risk. Among offspring of iron-deficient women, the odds of fetal anemia increased with fetal α-thalassemia, as well as these patterns of cord blood cytokines: increased cord IL-6, decreased TNF-RI, and decreased sTfR. The EPO response to fetal anemia was low or absent and EPO levels were significantly decreased in newborns with the most severe anemia. This study from an area of high malaria transmission provides evidence that 1) fetal α-thalassemia and cytokine balance, but not PM at delivery, are related to fetal anemia; 2) maternal iron deficiency increases the risk that other factors may cause fetal anemia; and 3) fetal anemia has a multifactorial etiology that may require a variety of interventions, although measures that reduce maternal iron deficiency may be generally beneficial.

摘要

胎儿贫血在疟疾流行地区很常见,也是婴儿期贫血和死亡的一个危险因素。胎盘疟疾(PM)和红细胞异常已被提出作为可能的病因,但 PM 与胎儿贫血之间的关系在早期研究中有所不同,并且红细胞异常在疟疾流行地区的作用尚未得到研究。在一项旨在阐明婴幼儿严重疟疾发病机制的坦桑尼亚出生队列研究中,我们对胎儿贫血的危险因素进行了横断面分析。我们确定了 PM 状况、新生儿红细胞异常以及母体和脐带血中铁调节蛋白、促红细胞生成素 (EPO)、细胞因子和细胞因子受体的水平。我们研究了这些因素与胎儿贫血之间的关系。胎儿贫血存在于 46.2%的新生儿中,但与 PM 无关。母体缺铁很常见(81.6%),在多产妇中最为常见,并且与产次相互作用,改变了胎儿贫血的风险,但与风险没有直接关系。在缺铁的妇女的后代中,胎儿贫血的风险随着胎儿α-地中海贫血的增加而增加,以及这些脐带血细胞因子的模式:脐带 IL-6 增加,TNF-RI 减少,sTfR 减少。胎儿贫血对 EPO 的反应较低或不存在,并且 EPO 水平在贫血最严重的新生儿中显著降低。这项来自疟疾高传播地区的研究提供了证据,表明 1)胎儿α-地中海贫血和细胞因子平衡,但不是分娩时的 PM,与胎儿贫血有关;2)母体缺铁增加了其他因素可能导致胎儿贫血的风险;3)胎儿贫血的病因复杂,可能需要多种干预措施,尽管减少母体缺铁的措施可能普遍有益。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/39f8/8120033/ee1e24525815/fimmu-12-624136-g001.jpg

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