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Please use this identifier to cite or link to this item: http://hdl.handle.net/20.500.12710/33040
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dc.contributor.authorNeagu, Anastasia-
dc.date.accessioned2026-04-03T15:19:57Z-
dc.date.available2026-04-03T15:19:57Z-
dc.date.issued2026-
dc.identifier.citationNEAGU, Anastasia. Translational perinatal medicine in non-immune fetal hydrops: from prenatal to modern cellular therapies. In: Cells and Tissues Transplantation. Actualities and Perspectives: The Materials of the National Scientific Conference with International Participation, the 4 th edition, Chisinau, March 20-21, 2026. Chișinău : CEP Medicina, 2026, p. 49. ISBN 978-9975-82-477-4 (PDF).en_US
dc.identifier.isbn978-9975-82-477-4-
dc.identifier.urihttps://repository.usmf.md/handle/20.500.12710/33040-
dc.description.abstractIntroduction. Non-immune fetal hydrops (NIHF) represents one of the most severe conditions in fetal medicine, characterized by the pathological accumulation of fluid in at least two fetal compartments and associated with high perinatal mortality. Its heterogeneous etiology includes genetic anomalies, cardiovascular pathologies, congenital infections, and idiopathic causes. Recent advances in prenatal diagnostics have improved early etiological identification; however, therapeutic options remain limited. Translational perinatal medicine aims to integrate insights from cellular biology and regenerative medicine into fetal management, including the use of cellular therapies and intrauterine transplantation strategies. The objective of this study is to evaluate the potential role of modern cellular therapies in the management of NIHF. Materials and Methods. A narrative review of recent scientific literature published between 2022 and 2025 in PubMed, Scopus, and Web of Science was conducted, including review articles and experimental studies. Data were synthesized descriptively, and results from experimental studies were analyzed comparatively. Results. Current literature confirms that the prognosis of NIHF largely depends on the prenatal etiological diagnosis and the timeliness of therapeutic intervention. The development of stem cell– based therapies, including transamniotic administration of mesenchymal and hematopoietic stem cells, has shown promising effects on fetal hematopoiesis, placental inflammation, and fetal survival in experimental models. Innovative strategies, such as transamniotic stem cell therapy, enable systemic fetal cell distribution through minimally invasive approaches. Furthermore, extracellular vesicles derived from amniotic fluid–derived stem cells have demonstrated regenerative potential in compromised fetal lung development, a mechanism relevant to the progression of fetal hydrops. These approaches support a transition from purely supportive care toward targeted biological interventions. Conclusions The integration of advanced prenatal diagnostics with cellular therapies represents a promising approach in managing non-immune fetal hydrops. Translational perinatal medicine enables the shift from understanding pathogenic mechanisms to fetal regenerative interventions. Future studies are needed to validate the safety and efficacy of intrauterine cellular transplantation and improve neonatal outcomes.en_US
dc.language.isoenen_US
dc.publisherCEP Medicinaen_US
dc.relation.ispartofCells and Tissues Transplantation. Actualities and Perspectives: The Materials of the National Scientific Conference with International Participation, the 4 th edition, Chisinau, March 20-21, 2026en_US
dc.subjectnon-immune fetal hydropsen_US
dc.subjectprenatal diagnosisen_US
dc.subjectstem cell therapyen_US
dc.subjectfetal therapyen_US
dc.subjecttranslational medicineen_US
dc.titleTranslational perinatal medicine in non-immune fetal hydrops: from prenatal to modern cellular therapiesen_US
dc.typeOtheren_US
Appears in Collections:Cells and Tissues Transplantation. Actualities and Perspectives: The Materials of the National Scientific Conference with International Participation, the 4 th edition, Chisinau, March 20-21, 2026



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