Perinatal risk factors associated with severity of haemolytic disease of the foetus and newborn due to <scp>Rhc</scp> maternal‐foetal incompatibility: A retrospective cohort study

Franchinard, Loriane; Maisonneuve, Emeline; Friszer, Stéphanie; Toly-Ndour, Cécile; Huguet-Jacquot, Stéphanie; Maurice, P; Mailloux, Agnès; Cortey, A.; Jouannic, Jean‐Marie

doi:10.1111/vox.13215

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Cited by 3 publications

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Immunohematological testing and transfusion management of the prenatal patient

Quraishy,

Sapatnekar

2023

Advances in Clinical Chemistry

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Immunohematological testing and transfusion management of the prenatal patient

Quraishy,

Sapatnekar

2023

Advances in Clinical Chemistry

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Recommandations pour la réalisation des examens d’immuno-hématologie de première intention par les laboratoires médicaux

Joubaud,

Giannoli

2024

Transfusion Clinique et Biologique

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Management of Red Cell Alloimmunization in Pregnancy

Moise,

Abels

2024

Obstetrics &Amp; Gynecology

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Rhesus immune globulin has resulted in a marked decrease in the prevalence of RhD alloimmunization in pregnancy; however, antibody formation to other red cell antigens continues to occur. Evaluation for the presence of anti–red cell antibodies should be routinely undertaken at the first prenatal visit. If anti–red cell antibodies are detected, consideration of a consultation or referral to a maternal–fetal medicine specialist with experience in the monitoring and treatment of these patients is warranted. Cell-free DNA can be used to determine fetal red cell antigen status to determine whether the pregnancy is at risk of complications from the red cell antibodies. First-time sensitized pregnancies are followed up with serial maternal titers, and, when indicated, serial Doppler assessment of the peak systolic velocity in the middle cerebral artery should be initiated by 16 weeks of gestation. When there is a history of an affected fetus or neonate, maternal titers are less predictive of fetal risk; if the fetus is antigen positive, serial peak systolic velocity in the middle cerebral artery measurements should be initiated by 15 weeks of gestation because intraperitoneal intrauterine blood transfusions can be used at this gestation if needed. The mainstay of fetal therapy involves intrauterine transfusion through ultrasound-directed puncture of the umbilical cord with the direct intravascular injection of red cells. A perinatal survival rate exceeding 95% can be expected at experienced centers. Neonatal phototherapy and “top-up” transfusions attributable to suppressed reticulocytosis often are still required for therapy after delivery.

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Perinatal risk factors associated with severity of haemolytic disease of the foetus and newborn due to Rhc maternal‐foetal incompatibility: A retrospective cohort study

Cited by 3 publications

References 24 publications

Immunohematological testing and transfusion management of the prenatal patient

Immunohematological testing and transfusion management of the prenatal patient

Recommandations pour la réalisation des examens d’immuno-hématologie de première intention par les laboratoires médicaux

Management of Red Cell Alloimmunization in Pregnancy

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