Hydrops: Diagnosing & Redefining Outcomes With Precision Study (HyDROPS)
Sponsor: Eunice Kennedy Shriver National Institute of Child Health and Human Development (NICHD)
Listed as NCT03412760, this observational or N/A phase trial focuses on Birth Defect and Fetal Anomaly and remains ongoing. Sponsored by Eunice Kennedy Shriver National Institute of Child Health and Human Development (NICHD), it has been updated 16 times since 2018, reflecting substantial change activity. This study adds to the evidence base for this therapeutic area through structured, versioned documentation.
Study Description(click to expand)Up to 1:1700 pregnancies are affected by non-immune hydrops fetalis (NIHF), and this condition is associated with significant perinatal risks ranging from preterm birth to Ballantyne (maternal mirror) syndrome, stillbirth, and neonatal death. Birth defects affect 1:33 pregnancies, and are the leading cause of infant death (contributing to approximately 20% of infant deaths). The investigators are performing exome sequencing (ES) for the affected fetus or neonate in unexplained cases, as well as enrolling cases with a genetic explanation to represent the full spectrum of diseases underlying NIHF and other birth defects. This study is open for enrollment by invitation. In addition to performing ES, the investigators are collecting clinical data prospectively on all cases of NIHF and other birth defects, including demographics, medical and obstetric history, prenatal and delivery course, and postnatal outcomes. The specific research aims include: 1. Create registry of clinical data for cases of NIHF and other birth defects. 2. Investigate genetic variants underlying NIHF and other birth defects via ES. 3. Characterize the features and outcomes of genetic diseases presenting with NIHF and other birth defects. * In particular, the researchers are focused on enrolling cases of increased nuchal translucency, cystic hygroma, abnormal fetal fluid collection...
Up to 1:1700 pregnancies are affected by non-immune hydrops fetalis (NIHF), and this condition is associated with significant perinatal risks ranging from preterm birth to Ballantyne (maternal mirror) syndrome, stillbirth, and neonatal death. Birth defects affect 1:33 pregnancies, and are the leading cause of infant death (contributing to approximately 20% of infant deaths). The investigators are performing exome sequencing (ES) for the affected fetus or neonate in unexplained cases, as well as enrolling cases with a genetic explanation to represent the full spectrum of diseases underlying NIHF and other birth defects.
This study is open for enrollment by invitation. In addition to performing ES, the investigators are collecting clinical data prospectively on all cases of NIHF and other birth defects, including demographics, medical and obstetric history, prenatal and delivery course, and postnatal outcomes.
The specific research aims include:
1. Create registry of clinical data for cases of NIHF and other birth defects. 2. Investigate genetic variants underlying NIHF and other birth defects via ES. 3. Characterize the features and outcomes of genetic diseases presenting with NIHF and other birth defects.
* In particular, the researchers are focused on enrolling cases of increased nuchal translucency, cystic hygroma, abnormal fetal fluid collection (even single fluid compartments such as isolated pleural effusion), and/or frank NIHF.
This research will contribute novel information about the frequency and types of genetic disorders in fetuses and newborns with a diagnosis of NIHF and other birth defects, enabling providers to more accurately counsel about prognosis and individualize perinatal care. This information will also facilitate informed decision-making for parents, allow the care team to anticipate specific perinatal needs, and enable more precise counseling for the parents about recurrence risks for NIHF and other birth defects. Further, the research will facilitate future aims such as novel fetal therapies for genetic diseases.
Status Flow
Change History
16 versions recorded-
Apr 18, 2026 — Present [daily]
Active Not Recruiting
Phase: NA → None
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Feb 2026 — Apr 2026 [monthly]
Active Not Recruiting NA
Status: Enrolling By Invitation → Active Not Recruiting
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May 2025 — Feb 2026 [monthly]
Enrolling By Invitation NA
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Sep 2024 — May 2025 [monthly]
Enrolling By Invitation NA
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Jul 2024 — Sep 2024 [monthly]
Enrolling By Invitation NA
▶ Show 11 earlier versions
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Mar 2024 — Jul 2024 [monthly]
Enrolling By Invitation NA
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Feb 2023 — Mar 2024 [monthly]
Enrolling By Invitation NA
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Nov 2021 — Feb 2023 [monthly]
Enrolling By Invitation NA
Status: Recruiting → Enrolling By Invitation
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Jan 2021 — Nov 2021 [monthly]
Recruiting NA
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May 2020 — Jan 2021 [monthly]
Recruiting NA
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Feb 2020 — May 2020 [monthly]
Recruiting NA
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Jun 2019 — Feb 2020 [monthly]
Recruiting NA
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May 2019 — Jun 2019 [monthly]
Recruiting NA
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Nov 2018 — May 2019 [monthly]
Recruiting NA
Status: Not Yet Recruiting → Recruiting
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Jun 2018 — Nov 2018 [monthly]
Not Yet Recruiting NA
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Feb 2018 — Jun 2018 [monthly]
Not Yet Recruiting NA
First recorded
Eligibility Summary
This is a national, prospective study designed to investigate the genetic etiologies of non-immune hydrops fetalis (NIHF) and other birth defects. At least half of prenatally diagnosed NIHF cases remain of unknown etiology after standard work up, and a substantial proportion of other birth defects remain of unknown etiology as well. The investigators are performing exome sequencing (ES) for the affected fetus or neonate in unexplained cases, as well as enrolling cases with a genetic explanation to represent the full spectrum of diseases underlying NIHF and other birth defects.
Contact Information
- Eunice Kennedy Shriver National Institute of Child Health and Human Development (NICHD)
- Fetal Health Foundation
- National Institutes of Health (NIH)
- University of California, San Francisco
For direct contact, visit the study record on ClinicalTrials.gov .