Control variables of serum ferritin concentrations in hospitalized newborn infants: an observational study

Both iron excess and deficiency are deleterious to cellular and organ homeostasis. Serum ferritin levels serve as a biomarker of iron storage; however, their distribution and determinants in sick newborn infants remain unclear. This study aimed to investigate the reference range and independent variables of serum ferritin in hospitalized newborn infants. All newborn infants who were hospitalized at a tertiary neonatal center within 24 h of birth were retrospectively reviewed for the period of April 2015 through March 2017. Serum ferritin levels were assessed using venous blood samples obtained at admission and their independent variables were explored. The study population comprised 368 infants (36.2 ± 2.8 weeks gestation and 2319 ± 623 g at birth), whose median serum ferritin level was 149 µg/L (inter-quartile range: 81–236). The multivariable model used to explain serum ferritin values comprised hemoglobin, lactate dehydrogenase, blood pH, and maternal hypertensive disorders in pregnancy (all p < 0.01, adjusted for sex and birth weight). Serum ferritin values in hospitalized newborn infants were comparable to those previously reported using umbilical cord blood. Our novel findings indicated the association between blood pH, lactate dehydrogenase, and ferritin levels, suggesting the influence of antenatal hypoxia–ischemia and stress to serum ferritin levels.


Scientific Reports
| (2023) 13:8424 | https://doi.org/10.1038/s41598-023-35404-0 www.nature.com/scientificreports/ within an important part of the disease mechanism 23,31 . Although these clinical conditions cause a wide range of morbidities 32 , the timing and level of altered iron metabolism and related ferritin levels largely remain unknown. Adverse consequences related to impaired iron metabolism might be identified and ameliorated by monitoring ferritin levels shortly after birth. However, thus far, reference ranges of serum ferritin levels in newborn infants have not been established based on a large sample size. Reference ranges of serum ferritin levels are ethically difficult to establish in healthy newborn infants. However, in hospitalized newborn infants, serum ferritin levels can be assessed as a routine or additional test using residual blood samples. If the reference ranges can be established in hospitalized infants, they may help design and conduct future studies to explore covert relationships between altered iron metabolism and pathological clinical conditions. In addition, despite the dynamic change in serum ferritin levels in newborn infants under both physiological and pathological conditions, clinical factors associated with ferritin levels in newborn infants remain largely unknown.
This study aimed to clarify the reference range of serum ferritin levels in a relatively large cohort of hospitalized newborn infants and to elucidate their independent variables.

Results
Values are presented as mean ± standard deviation unless otherwise described.

Discussion
In a relatively larger population of hospitalized newborn infants, we demonstrated that ferritin levels of venous blood samples assessed shortly after birth were comparable to those measured using umbilical cord blood in term and preterm newborn infants 33 . Consistent with previous studies 33,34 , high serum ferritin levels were observed in newborn infants with greater gestational age and birth weight, and clinical conditions suggestive of placental dysfunction, infection, and inflammation. We newly identified hemoglobin levels, Apgar scores, and blood acid-base status as potential independent variables of ferritin levels. In the multivariable model, higher serum ferritin levels within the first 24 h of age were determined by a greater z-score of the birth weight, lower hemoglobin levels, lower blood pH, higher serum lactate dehydrogenase values, and absence of pregnancy-induced hypertension, suggesting that elevated serum ferritin levels in newborn infants might be associated with fetal growth and maturation, and with acute and chronic perinatal hypoxia-ischemia. With further validation, serum ferritin levels shortly after birth might be used as a predictive biomarker to estimate the impact of hypoxia-ischemia at birth.
Based on a mixed but relatively large population of hospitalized newborn infants, we first defined the reference value of serum ferritin levels. We found that ferritin levels were comparable but slightly lower than 171-200 µg/L, which were reported previously using umbilical cord blood 33,35 . Considering that our study population had a relatively younger mean gestational age of 36.2 weeks as opposed to 41 weeks in the aforementioned study, the slight difference in the ferritin values in these studies might reflect the maturation-related increase in ferritin www.nature.com/scientificreports/ levels, and our findings might be consistent with the previous understanding that serum ferritin levels increase during the fetal period and exceeds the level of healthy adults by term birth, followed by temporal declines from and recovery to the baseline levels during the first years of life 33,36 .
Using the same dataset, we further delineated clinical independent variables of serum ferritin levels at birth. Consistent with previous reports 33, 34 , the gestational age, birth weight, lactate dehydrogenase, and inflammatory biomarkers, including white blood cell count and C-reactive protein, have positive correlations with serum ferritin levels, suggesting that serum ferritin levels at birth are influenced by intrauterine growth and maturation, as well as antenatal infection and inflammation. Similarly, maternal age and the presence of pregnancy-induced hypertension appeared to be inversely correlated with serum ferritin levels.
In addition to established independent variables, we identified several novel control variables of serum ferritin in newborn infants. Regarding the relationship between ferritin and hemoglobin levels in newborn infants, www.nature.com/scientificreports/ positive and negative relationships have been reported 37,38 . In our study, we demonstrated that ferritin levels were inversely correlated with hemoglobin levels at birth according to a relatively large cohort of hospitalized newborn infants. This finding appears to be controversial considering that iron deficiency theoretically results in reduced serum ferritin and hemoglobin levels 12 . However, prolonged intrauterine hypoxia and ischemia might have upregulated fetal erythropoiesis with lower ferritin levels, similar with placental deficiency and intrauterine growth restriction 26 . Similar inverse relationships between serum ferritin and hemoglobin were reported in association with fetal growth restriction, maternal diabetes mellitus, and maternal smoking 33,39,40 . Since incomplete erythropoiesis leads to improper use of iron and destruction of immature erythrocytes and raises serum ferritin levels under anemic conditions 41 , immature response to erythropoietin in newborn infants might explain the observed inverse correlation between hemoglobin and ferritin levels. In addition, in cases when infection and inflammation coincide with anemia, elevated hepcidin expression may restrict iron supply and erythropoiesis, as shown in a rat model of anemia coincided with chronic inflammation 42 . We observed increases in ferritin levels in association with clinical events suggestive of the presence of fetal hypoxia-ischemia and acidosis, as well as birth asphyxia, represented by elevated lactate dehydrogenase levels, www.nature.com/scientificreports/ low blood pH and base excess, and low Apgar scores. These findings are consistent with studies that reported marked elevation of serum ferritin levels after the onset of stroke [43][44][45] and with a preclinical study in rodents, which showed that temporary occlusion of the middle cerebral artery resulted in the upregulation of ferritin synthesis at both mRNA and protein levels 44 . There were several limitations to our current study. First, because the dataset used for the current study was based on the information obtained for clinical reasons, we were not able to assess serum biomarkers of iron metabolism other than ferritin. Future studies may need to assess comprehensive markers involved in iron homeostasis, such as hepcidin, transferrin receptors, erythropoietin, and erythroferrone, as well as serum iron levels. Second, we were unable to recruit healthy newborn infants to establish the reference ranges of ferritin concentrations because of ethical and practical reasons. Consequently, the clinical backgrounds of the hospitalized newborn infants were highly heterogeneous, including extremely preterm birth, hypoxic-ischemic encephalopathy, severe systemic infection, and other clinical conditions, which need to be considered when interpreting our findings to the practice in healthy newborn infants. Such variations in the clinical backgrounds helped identify patient types and clinical conditions associated with ferritin levels shortly after birth. However, despite the moderate size of the study cohort, there were insufficient number of infants with specific diseases, such as septicemia, necrotizing enterocolitis, chronic lung disease, and retinopathy of prematurity, to investigate the relationship between altered iron metabolism and the development of the diseases. Third, although all blood samples were obtained within 24 h of birth, we were unable to incorporate the time of sampling after birth within the model, which might be an additional independent variable of serum ferritin levels considering the drastic changes in oxygen metabolism from intrauterine to the extrauterine environment.

Conclusions
We clarified a reference value for serum ferritin levels in sick newborns within 24 h of age, which was comparable to previous studies that used cord blood and included healthy adults. We also confirmed the relationship between ferritin levels and established control variables of gestational age, birth weight and its z-score, and those associated with infection and inflammation. Furthermore, hemoglobin levels, Apgar scores, lactate dehydrogenase levels, and blood acid-base status were newly identified as potential independent variables of ferritin levels in newborn infants. Our findings suggested that intrauterine growth and maturation, inflammation, anemia, and acute and chronic hypoxia-ischemia are key factors in determining serum ferritin levels in hospitalized newborn infants.

Methods
This retrospective observational study was conducted in compliance with the Declaration of Helsinki under the approval of the Ethics Committee of St Mary's Hospital. The Ethics Committee waived the requirement for informed consent because the study only used anonymized data obtained for clinical reasons. Newborn infants who were hospitalized at a tertiary neonatal intensive care unit (NICU) of St Mary's Hospital within 24 h of age and assessed serum ferritin values using peripheral venous blood samples obtained at admission were reviewed. In this NICU, serum ferritin is measured as a routine blood test for newborn infants who are admitted during the daytime or weekdays using the latex immunoturbidimetric assay (LABOSPECT 008, HITACHI, Tokyo, Japan). A total of 927 newborn infants were admitted to the NICU between April 2015 and March 2017. Of these, 348 newborn infants were hospitalized 24 h after birth, and 211 newborn infants were hospitalized within 24 h of age but during the night-time, weekend, and holidays, when the assay of serum ferritin values was unavailable. Finally, 368 newborn infants were included in the study cohort (Fig. 1). Physiological variables were obtained from the medical record of newborn infants and their mothers, including maternal complications, gestational age at birth, birth weight, sex, birth location, delivery mode, findings from blood tests, types of treatments, and clinical morbidities during hospitalization. variable linear regression analysis was first performed to estimate the crude effects of the clinical background on serum ferritin values, excluding those with the incidence of less than 10. Findings from the univariable analysis were shown without correcting for multiple comparisons because of its exploratory nature. Statistical significance was set at p-value < 0.01. We created a multivariable linear regression model to explain the ferritin level, which was adjusted for sex, gestational age at birth, and the z-score of birth weight. Up to four independent variables were chosen based on the findings from the univariate analysis when theoretically relevant.

Data availability
The datasets generated during and/or analyzed during the current study are available from the corresponding author on reasonable request. Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons licence, and indicate if changes were made. The images or other third party material in this article are included in the article's Creative Commons licence, unless indicated otherwise in a credit line to the material. If material is not included in the article's Creative Commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this licence, visit http:// creat iveco mmons. org/ licen ses/ by/4. 0/.