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Please use this identifier to cite or link to this item: https://swslhd.intersearch.com.au/swslhdjspui/handle/1/12965
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dc.contributor.authorMoise, K. J.-
dc.contributor.authorLing, L. E.-
dc.contributor.authorOepkes, D.-
dc.contributor.authorTiblad, E.-
dc.contributor.authorVerweij, E. J. T. J.-
dc.contributor.authorLopriore, E.-
dc.contributor.authorSmoleniec, J.-
dc.contributor.authorSachs, U. J.-
dc.contributor.authorBein, G.-
dc.contributor.authorKilby, M. D.-
dc.contributor.authorMiller, R. S.-
dc.contributor.authorDevlieger, R.-
dc.contributor.authorAudibert, F.-
dc.contributor.authorEmery, S. P.-
dc.contributor.authorMarkham, K.-
dc.contributor.authorNorton, M. E.-
dc.contributor.authorOc�n-Hern�ndez, O.-
dc.contributor.authorPandya, P.-
dc.contributor.authorPereira, L.-
dc.contributor.authorSilver, R. M.-
dc.contributor.authorWindrim, R.-
dc.contributor.authorStreisand, J. B.-
dc.contributor.authorLeu, J. H.-
dc.contributor.authorMirza, A.-
dc.contributor.authorSmith, V.-
dc.contributor.authorSchwartz, L. B.-
dc.contributor.authorTjoa, M. L.-
dc.contributor.authorSaeed-Khawaja, S.-
dc.contributor.authorKomatsu, Y.-
dc.contributor.authorBussel, J. B.-
dc.date.accessioned2024-09-02T05:57:00Z-
dc.date.available2024-09-02T05:57:00Z-
dc.date.issued2024-
dc.identifier.issn00284793 (ISSN)-
dc.identifier.urihttps://swslhd.intersearch.com.au/swslhdjspui/handle/1/12965-
dc.description.abstractIn early-onset severe hemolytic disease of the fetus and newborn (HDFN), transplacental transfer of maternal antierythrocyte IgG alloantibodies causes fetal anemia that leads to the use of high-risk intrauterine transfusions in order to avoid fetal hydrops and fetal death. Nipocalimab, an anti-neonatal Fc receptor blocker, inhibits transplacental IgG transfer and lowers maternal IgG levels. METHODS In an international, open-label, single-group, phase 2 study, we assessed treatment with intravenous nipocalimab (30 or 45 mg per kilogram of body weight per week) administered from 14 to 35 weeks' gestation in participants with pregnancies at high risk for recurrent early-onset severe HDFN. The primary end point was live birth at 32 weeks' gestation or later without intrauterine transfusions as assessed against a historical benchmark (0%; clinically meaningful difference, 10%). RESULTS Live birth at 32 weeks' gestation or later without intrauterine transfusions occurred in 7 of 13 pregnancies (54%; 95% confidence interval, 25 to 81) in the study. No cases of fetal hydrops occurred, and 6 participants (46%) did not receive any antenatal or neonatal transfusions. Six fetuses received an intrauterine transfusion: five fetuses at 24 weeks' gestation or later and one fetus before fetal loss at 22 weeks and 5 days' gestation. Live birth occurred in 12 pregnancies. The median gestational age at delivery was 36 weeks and 4 days. Of the 12 live-born infants, 1 received one exchange transfusion and one simple transfusion and 5 received only simple transfusions. Treatment-related decreases in the alloantibody titer and IgG level were observed in maternal samples and cord blood. No unusual maternal or pediatric infections were observed. Serious adverse events were consistent with HDFN, pregnancy, or prematurity. CONCLUSIONS Nipocalimab treatment delayed or prevented fetal anemia or intrauterine transfusions, as compared with the historical benchmark, in pregnancies at high risk for early-onset severe HDFN. Copyright � 2024 Massachusetts Medical Society.-
dc.publisherMassachussetts Medical Society-
dc.subjectalbumin alloantibody Fc receptor human immunoglobulin immunoglobulin immunoglobulin G monoclonal antibody nipocalimab abdominal pain abnormal fetal heart rate adult anemia antibody titer Apgar score Article bacteriuria binding affinity birth weight body mass body weight candidiasis cost effectiveness analysis Doppler ultrasonography drug safety ear infection echography electrocardiography erythrocyte transfusion exchange blood transfusion female fetus gestational age gestational weight gain hematoma hemoglobin blood level hemolytic anemia hospitalization human hyperbilirubinemia hypoalbuminemia intrauterine blood transfusion intrauterine growth retardation jaundice live birth mastitis maternal age newborn otorrhea peak systolic velocity phase 2 clinical trial physical examination placenta insufficiency placental transfer plasmapheresis pregnancy outcome prematurity respiratory distress stillbirth Streptococcus infection urinary tract infection vaginal delivery-
dc.titleNipocalimab in Early-Onset Severe Hemolytic Disease of the Fetus and Newborn-
dc.typeJournal Article-
dc.contributor.swslhdauthorSmoleniec, John-
dc.description.affiliatesDell Medical School, University of Texas at Austin, The Comprehensive Fetal Care Center, Dell Children's Medical Center, Austin, United States Janssen Pharmaceuticals, Cambridge, MA, United States The Department of Obstetrics, Leiden University Medical Center, Leiden, Netherlands The Department of Pediatrics, Leiden University Medical Center, Leiden, Netherlands The Clinical Epidemiology Division, Department of Medicine Solna, Karolinska Institutet, Stockholm, Sweden The Feto-Maternal Unit, Liverpool Hospital, Liverpool, NSW, Australia The Institute for Clinical Immunology and Transfusion Medicine, Justus Liebig University, Giessen, Germany The Department of Thrombosis and Hemostasis, Giessen University Hospital, Giessen, Germany The University of Birmingham, The Fetal Medicine Center, Birmingham Women's and Children's NHS Foundation Trust, Birmingham, United Kingdom University College London Hospitals, NHS Foundation Trust, London, United Kingdom The Division of Maternal-Fetal Medicine, Department of Obstetrics and Gynecology, Columbia University, Irving Medical Center, New York, United States The Department of Pediatrics, Division of Hematology-Oncology, Weill Cornell Medical College, New York, United States NewYork-Presbyterian Hospital, New York, United States The Department of Obstetrics and Gynecology, University Hospitals KU Leuven, Leuven, Belgium The Department of Obstetrics, Gynecology, and Fertility, GZA Campus Sint-Augustinus, Wilrijk, Belgium Centre Hospitalier Universitaire Sainte-Justine Research Center, Universit� de Montr�al, Montreal, Canada Mount Sinai Hospital Toronto, University of Toronto, Toronto, Canada UPMC Magee-Womens Hospital, Pittsburgh, United States The Division of Maternal-Fetal Medicine, Department of Obstetrics and Gynecology, University of Cincinnati Medical Center, Cincinnati, United States The Department of Obstetrics and Gynecology, University of California, San Francisco, San Francisco, United States Zuckerberg San Francisco General Hospital, San Francisco, United States San Cecilio University Hospital, Granada, Spain The Department of Obstetrics and Gynecology, Oregon Health and Science University, Portland, United States University of Utah Health, Salt Lake City, United States Streisand Biomedical Consulting, Wayland, MA, United States-
dc.identifier.doi10.1056/NEJMoa2314466-
dc.identifier.departmentLiverpool Hospital, Department of Obstetrics and Gynecology-
dc.type.studyortrialArticle-
dc.identifier.journaltitleNew England Journal of Medicine-
Appears in Collections:Liverpool Hospital

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