Amniotic Fluid Disorders: From Prenatal Management to Neonatal Outcomes
Abstract
:1. Introduction
2. Amniotic Fluid Volume Measurement
3. Normal Amniotic Fluid Volume
4. Oligohydramnios
5. Isolated Oligohydramnios
6. Polyhydramnios
7. Idiopathic Polyhydramnios
8. Conclusions and Implications for Future Research
- In clinical practice, one set of diagnostic thresholds is used throughout pregnancy to diagnose AFV disorders. Nevertheless, many physiological factors, such as race, parity, and gestational age, may contribute to the actual AFV. Further studies are warranted to clarify whether the inclusion of these variables in the diagnosis improves the detection rate of adverse outcomes. Furthermore, ultrasound semiquantitative methods to measure the amniotic fluid have low accuracy in detecting true abnormal AFV, and it is questionable whether they are necessary in low-risk pregnancies [22].
- Currently, data on the association of isolated oligohydramnios or idiopathic polyhydramnios with adverse obstetric and perinatal outcomes are conflicting. Further large, well-designed studies should be performed to investigate the association between sonographic AFV disorders and ominous outcomes, in particular intrauterine fetal demise, severe perinatal morbidity and neonatal mortality. For idiopathic polyhydramnios, such studies should be stratified by the degree of polyhydramnios (mild, moderate or severe).
- Oligohydramnios is associated with an increased rate of obstetric interventions, as it is classically considered an indicator of potential fetal compromise. It is still unclear, however, whether isolated oligohydramnios is an expression of an underlying placental dysfunction and therefore an indication for antepartum fetal surveillance and earlier delivery. Consequently, while the management of secondary oligohydramnios is usually guided by the underlying condition, the best management of isolated oligohydramnios is still poorly defined.
- Similarly, the management of idiopathic and secondary polyhydramnios has not yet been standardised. A diagnosis of polyhydramnios should prompt identification of the underlying cause. The association with fetal anomalies is stronger with higher severity of polyhydramnios, while mild polyhydramnios should be considered a separate entity. The role of antenatal fetal surveillance and active management in mild, moderate or severe idiopathic polyhydramnios is unclear, especially considering the high rate of cesarean sections associated with all classes of polyhydramnios.
- There is an urgent need for randomized clinical trials comparing expectant management versus labor induction in the presence of isolated oligohydramnios or moderate to severe idiopathic polyhydramnios, in order to provide stronger recommendations on the management of these conditions.
Author Contributions
Funding
Institutional Review Board Statement
Informed Consent Statement
Data Availability Statement
Conflicts of Interest
References
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Maternal Causes | Fetal Causes | Placental Causes | Isolated Oligohydramnios |
---|---|---|---|
Hypertensive disorders Medications (angiotensin-converting enzyme inhibitors, angiotensin receptor blockers, indomethacin); drug abuse | Genitourinary tract abnormalities (lower urinary tract obstruction; Renal anomalies) Congenital infections Stillbirth | Placental insufficiency (fetal growth restriction) Twin-to-twin transfusion syndrome (TTTS) in monochorionic twin pregnancies Post-term pregnancies | No etiology identified |
(Preterm) Premature Rupture of Membranes |
Amniotic Fluid Index | Single Vertical Deepest Pocket | Incidence | |
---|---|---|---|
Mild | 25–29.9 cm | 8–11 cm | 65–70% |
Moderate | 30–34.9 cm | 12–15 cm | 20% |
Severe | ≥35 cm | ≥16 cm | <15% |
Maternal Diabetes (15–24%) | Fetal Causes (11–33%) | Placental Causes | Idiopathic (50–70%) |
---|---|---|---|
Gestational diabetes mellitus Pregestational diabetes mellitus (type I; type II) | Fetal malformations Chromosomal anomalies/genetic syndromes Metabolic disorders Fetal anemia Congenital infections | Chorioangioma Twin-to-twin transfusion syndrome (TTTS) in monochorionic twin pregnancies | No etiology identified |
Impaired Swallowing | Increased Cardiac Output/Cardiac Failure | Excessive Urine Production |
---|---|---|
Intracranial anomalies:
Craniofacial anomalies:
Intrathoracic masses:
Gastrointestinal obstruction/compression:
Neuromuscular disorders:
Chromosomal anomalies/genetic syndromes | Sacrococcygeal teratoma Placental chorioangioma Severe Cardiac structural anomalies, e.g.,:
Vascular anomalies Fetal anemia (maternal alloimmunization, parvovirus infection) Fetal thyrotoxicosis | Ureteropelvic junction obstruction Mesoblastic nephroma Bartter syndrome |
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Huri, M.; Di Tommaso, M.; Seravalli, V. Amniotic Fluid Disorders: From Prenatal Management to Neonatal Outcomes. Children 2023, 10, 561. https://doi.org/10.3390/children10030561
Huri M, Di Tommaso M, Seravalli V. Amniotic Fluid Disorders: From Prenatal Management to Neonatal Outcomes. Children. 2023; 10(3):561. https://doi.org/10.3390/children10030561
Chicago/Turabian StyleHuri, Mor, Mariarosaria Di Tommaso, and Viola Seravalli. 2023. "Amniotic Fluid Disorders: From Prenatal Management to Neonatal Outcomes" Children 10, no. 3: 561. https://doi.org/10.3390/children10030561
APA StyleHuri, M., Di Tommaso, M., & Seravalli, V. (2023). Amniotic Fluid Disorders: From Prenatal Management to Neonatal Outcomes. Children, 10(3), 561. https://doi.org/10.3390/children10030561