| Literature DB >> 30994929 |
Melissa F Young1, Brietta M Oaks2, Sonia Tandon1, Reynaldo Martorell1, Kathryn G Dewey3, Amanda S Wendt4.
Abstract
Maternal anemia is a well-recognized global health problem; however, there remain questions on specific hemoglobin (Hb) thresholds that predict health risk or protection for mother and child. We conducted a systematic review and meta-analysis to examine the associations of maternal Hb concentrations with a range of maternal and infant health outcomes, accounting for the timing of measurement (preconception, and first, second, and third trimesters), etiology of anemia, and cutoff category. The systematic review included 272 studies and the meta-analysis included 95 studies. Low maternal Hb (<110 g/L) was associated with poor birth outcomes (low birth weight, preterm birth, small-for-gestational-age (SGA), stillbirth, and perinatal and neonatal mortality) and adverse maternal outcomes (postpartum hemorrhage, preeclampsia, and blood transfusion). High maternal Hb (>130 g/L) was associated with increased odds of SGA, stillbirth, preeclampsia, and gestational diabetes. Relationships varied by the timing of measurement and cutoff category (stronger associations with lower cutoffs); limited data were available on anemia etiology. There were insufficient data for other maternal outcomes and long-term child health outcomes. Current data are insufficient for determining if revisions to current Hb cutoffs are required. Pooled high-quality individual-level data analyses, as well as prospective cohort studies, would be valuable to inform the reevaluation of Hb cutoffs.Entities:
Keywords: anemia; birth outcomes; hemoglobin; pregnancy; review
Year: 2019 PMID: 30994929 PMCID: PMC6767572 DOI: 10.1111/nyas.14093
Source DB: PubMed Journal: Ann N Y Acad Sci ISSN: 0077-8923 Impact factor: 5.691
Figure 1Flow of study selection.
Meta‐analysis of the association between low maternal Hb and child outcomes
| LBW OR (95% CI) | PTB OR (95% CI) | SGA OR (95% CI) | Stillbirth OR (95% CI) | Perinatal mortality OR (95% CI) | Neonatal mortality OR (95% CI) | |
|---|---|---|---|---|---|---|
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| Preconception |
| 1.04 (0.97−1.12) |
| 1.23 (0.39−3.86) | ||
| First trimester |
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| 1.08 (0.94−1.25) | 1.42 (0.39−5.25) | 1.61 (0.80−3.24) |
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| Second trimester | 1.14 (0.78−1.68) |
| 1.14 (0.96−1.37) |
| 1.38 (0.88−2.15) | |
| Third trimester |
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| 0.90 (0.73−1.10) | 1.82 (0.97−3.42) | 1.27 (0.97−1.67) | |
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| ≤70 g/L |
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| ≤80 g/L |
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| 1.10 (0.29−4.21) |
| ≤90 g/L |
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| 1.10 (0.29−4.21) |
| ≤100 g/L |
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| ≤110 g/L |
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| Overall estimate |
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notes: The sample size for individual studies is provided in Table S2 (online only), and the total number of studies included in each Hb cutoff effect estimate and timing are specified in Table S8 (online only). A number of studies included for an overall estimate (<110 g/L): LBW (36), PTB (33), SGA (21), stillbirth (21), perinatal mortality (11), and neonatal mortality (5). Reference groups for individual studies included in the meta‐analysis were highly variable, with some providing a range (e.g., 110−119 g/L) and others a cut off (≥110 g/L), with little consensus on what represents a “healthy” reference value. Reference groups for all studies included in meta‐analyses can be found in Figures S1–S6 (online only). Categories are cumulative; for example, the ≤100 g/L category includes studies using the ≤100 g/L cutoff or any subset where all Hb values were ≤100 g/L. Definitions: LBW, low birth weight (<2500 g); PTB, preterm birth (birth at <37 weeks gestation); SGA, small for gestational age (birth weight below the 10th percentile for gestational age or as defined by study authors); stillbirth (as defined by study authors); perinatal mortality (defined as the sum of fetal deaths (28 weeks or more gestation), and infant deaths occurring less than 7 days after birth); neonatal mortality (death within 28 days of life); first trimester: ≤13 weeks; second trimester: 14–26 weeks; third trimester: ≥27 weeks. Bold values are statically significant with P < 0.05.
*Summary estimates from meta‐analyses of <3 studies.
**Overall estimates using Hb concentrations measured at any point during pregnancy.
Meta‐analysis of association between high maternal Hb and child outcomes
| LBW OR (95% CI) | PTB OR (95% CI) | SGA OR (95% CI) | Stillbirth OR (95% CI) | |
|---|---|---|---|---|
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| Preconception | 1.04 (0.93−1.16) | 1.06 (1.00−1.13) | 1.03 (0.97−1.10) | 0.83 (0.52−1.33) |
| First trimester | 1.34 (0.52−3.46) | 0.93 (0.84−1.03) | 1.12 (0.99−1.27) | 1.28 (0.96−1.70) |
| Second trimester |
| 1.07 (0.83−1.39) |
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| Third trimester |
| 0.92 (0.55−1.56) | 1.08 (0.92−1.27) |
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| ≥120 g/L | 1.41 (0.94−2.13) | 1.16 (0.97−1.38) |
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| ≥130 g/L | 1.61 (0.82−3.16) | 1.14 (0.95−1.37) |
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| ≥140 g/L | 1.37 (0.44−4.23) | 1.10 (0.84−1.46) | 1.18 (0.97−1.42) |
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| ≥150 g/L | 0.78 (0.19−3.18) | 1.01 (0.55−1.85) | 0.92 (0.55−1.56) | |
| ≥160 g/L | 0.78 (0.19−3.18) | 0.42 (0.14−1.29) | 0.61 (0.22−1.56) | |
| Overall estimate | 1.80 (0.86−3.77) | 1.17 (0.94−1.45) |
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notes: The sample size for individual studies is provided in Table S2 (online only), and the total number of studies included in each Hb cut‐off effect estimate and timing are specified in Table S8 (online only). A number of studies included for an overall estimate (>130): LBW (5), PTB (10), SGA (4), and stillbirth (4). Reference groups for individual studies included in the meta‐analysis were highly variable, with some providing a range (e.g., 110−119 g/L) and others a cut off (≥110), with little consensus on what represents a “healthy” reference value. Reference groups for all studies included in meta‐analyses can be found in Figures S1−S4 (online only). Categories are cumulative; for example, the ≥140 g/L category includes studies using the ≥140 g/L cutoff or any subset where all Hb values were ≥140 g/L. Definitions: LBW, low birth weight (<2500 g); PTB, preterm birth (birth at <37 weeks gestation); SGA, small‐for‐gestational‐age (birth weight below the 10th percentile for gestational age or as defined by study authors); stillbirth (as defined by study authors); perinatal mortality (defined as the sum of fetal deaths (28 weeks or more gestation) and infant deaths occurring less than 7 days after birth); first trimester: ≤13 weeks; second trimester: 1–26 weeks; third trimester: ≥27 weeks. Bold values are statically significant with P < 0.05.
*Summary estimates from meta‐analyses of <3 studies.
**Summary estimates for ≥120 g/L presented, but high Hb defined as ≥130 g/L for inclusion in meta‐analysis summary estimates.
***Overall estimates using Hb concentrations measured at any point during pregnancy.
Figure 2Meta‐analysis summary estimates of association of maternal hemoglobin concentration (g/L) measured at any point during pregnancy and LBW, PTB, and SGA by hemoglobin concentration cutoffs.
Figure 3Meta‐analysis summary estimates of association of maternal hemoglobin concentration (g/L) measured at any point during pregnancy and stillbirth, perinatal mortality, and neonatal mortality by hemoglobin concentration cutoffs.
Meta‐analysis summary estimates of association of IDA and non‐IDA with birth outcomes
| Outcome | IDA OR (95% CI) | Non‐IDA OR (95% CI) |
|---|---|---|
| LBW | 1.17 (0.95−1.43) | 1.43 (0.82−2.50) |
| SGA | 0.77 (0.68−0.87) | 1.20 (0.85−1.70) |
| PTB | 1.07 (0.68−1.70) |
LBW: IDA: n = 2; non‐IDA: n = 3; SGA: IDA: n = 2; non‐IDA: n = 4; PTB: non‐IDA: n = 4.
Meta‐analyses of association between maternal Hb concentrations and maternal outcomes by Hb concentration cutoffs
| PPH OR (95% CI) | Preeclampsia OR (95% CI) | Transfusion OR (95% CI) | GDM | |
|---|---|---|---|---|
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| ≤70 g/L |
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| ≤80 g/L |
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| ≤90 g/L |
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| ≤100g/L |
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| ≤110 g/L |
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| 0.92 (0.73−1.16) |
| Overall estimate |
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| 0.92 (0.73−1.16) |
| ≥120 g/L | 0.84 (0.67−1.05) |
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| ≥130 g/L | 0.84 (0.67−1.05) |
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| ≥140 g/L | 0.84 (0.67−1.05) | 1.58 (0.88−2.83) |
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| Overall estimate | 0.84 (0.67−1.05) |
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notes: The sample size for individual studies is provided in Table S2 (online only), and the total number of studies included in each Hb cutoff effect estimate and timing are specified in Table S9 (online only). A number of studies included for overall estimates for low Hb (<110 g/L) are PPH (6), preeclampsia (8), transfusion (4), GDM (2), and for high Hb (>130 g/L) are PPH (1), preeclampsia (3), and GDM (4). Reference groups for individual studies included in the meta‐analysis were highly variable, with some providing a range (e.g., 110−119 g/L) and others a cut off (≥110 g/L), with little consensus on what represents a “healthy” reference value. Reference groups for all studies included in meta‐analyses can be found in Figures S7–S10 (online only). Reference groups for all studies included in meta‐analyses can be found in Figures S1–S6 (online only). Categories are cumulative; for example, the ≤100 g/L category includes studies using the ≤100 g/L cutoff or any subset where all Hb values were ≤100 g/L. Bold values are statically significant with P < 0.05.
*Summary estimates from meta‐analyses of <3 studies. Note, for PPH outcome, one study contributes data to the high Hb cutoffs and overall estimate and one study contributes to the lowest Hb cutoffs (≤70 and ≤80 g/L).
**Estimates using Hb concentrations measured at any point during pregnancy.
PPH, postpartum hemorrhage; GDM, gestational diabetes mellitus.
Key priority areas of research
| Key priority areas of research |
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It remains unclear how the relationship between anemia and maternal and child outcomes may vary based on the cause of anemia and potential implications for anemia cutoffs. Additional research is required to better understand the association of maternal Hb with maternal outcomes (e.g., depression) and long‐term child health outcomes (e.g., cardiovascular outcomes, diabetes, and child development). Few studies report relationships between continuous measures of maternal Hb and health outcomes. Further research is required on the role of maternal preconception Hb and birth outcomes. Few studies provide maternal Hb data during multiple time periods during pregnancy in the same cohort of women. This information is needed to guide potential trimester‐specific cutoff decisions. Limited data are available in high‐risk populations and further research is needed to understand if separate cutoffs are needed (i.e., twin pregnancies). Pooled, high‐quality, individual‐level prospective cohort data are needed to conduct cutoff analysis to inform the reevaluation of Hb cutoffs during pregnancy. |