Variations in antenatal management and outcomes in haemolytic disease of the fetus and newborn: an international, retrospective, observational cohort study.

IF 15.4 1区医学 Q1 HEMATOLOGY

Lancet Haematology Pub Date : 2024-11-08 DOI:10.1016/S2352-3026(24)00314-4

Derek P de Winter, Enrico Lopriore, Emilie Thorup, Olav Bjørn Petersen, Morten H Dziegiel, Karin Sundberg, Roland Devlieger, Luc de Catte, Liesbeth Lewi, Anne Debeer, Véronique Houfflin-Debarge, Louise Ghesquiere, Charles Garabedian, Kévin Le Duc, Eugenia Antolin, Nieves Mendez, James Castleman, Wing Ting Tse, Jean-Marie Jouannic, Paul Maurice, Jane Currie, Emma Mullen, Lut Geerts, Kerry Rademan, Asma Khalil, Borna Poljak, Smriti Prasad, Eleonor Tiblad, Kajsa Bohlin, Annegret Geipel, Johanna Rath, Fergal Malone, David Mackin, Yoav Yinon, Stav Cohen, Greg Ryan, Evangelia Vlachodimitropoulou, Karl-Philipp Gloning, Stefan Verlohren, Beate Mayer, Mariano Lanna, Stefano Faiola, Tanja Premru Sršen, Lilijana Kornhauser Cerar, Saul Snowise, Luming Sun, Lucas Otaño, César Hernan Meller, Ngina K Connors, Matthew Saxonhouse, Aline Wolter, Ivonne Bedei, Philipp Klaritsch, Sarah Jauch, Eduardo Teixeira da Silva Ribeiro, Fernando Maia Peixoto Filho, Raigam Jafet Martinez-Portilla, Alexandra Matias, Obdulia Alejos Abad, Juan Parra Roca, Ángel Guillermo Alcázar Grisi, Edgar Juan José Chávez Navarro, Johanna G van der Bom, Masja de Haas, Ejt Joanne Verweij

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We report practice variations in the management and outcomes of haemolytic disease of the fetus and newborn in at-risk pregnancies.Methods: In this international, retrospective, observational cohort study, data from cases with moderate or severe haemolytic disease of the fetus and newborn were retrieved from 31 centres in 22 countries. Eligible participants had pregnancies with haemolytic disease of the fetus that led to fetal death at 16 + 0 weeks or later, those treated antenatally with intrauterine transfusion or intravenous immunoglobulins, or neonates without antenatal treatment who were treated with intensive phototherapy, exchange transfusion, or red blood cell transfusions. All patients had confirmed maternal alloantibodies and an antigen-positive fetus incompatible with the maternal alloantibody. Patients with ABO-incompatibility only were excluded. We assessed serological diagnostics and referrals, antenatal treatment and timing, complications, delivery route, and gestational age at birth. Outcomes were analysed in all eligible participants who had complete data available.Findings: 2443 pregnancies with haemolytic disease of the fetus and newborn treated between Jan 1, 2006, and July 1, 2021, were shared by the centres and analysed between Dec 1, 2021, and March 1, 2023. 23 pregnancies were excluded due to missing information and we included 2420 for further analysis. 1764 (72·9%) of 2420 pregnancies were affected by D-antibodies. 95 (3·9%) of 2420 pregnancies resulted in fetal death. Of the 2325 liveborn neonates, 1349 (58·1%) received any form of antenatal treatment and 976 (41·9%) were only treated postnatally. Median gestational age at referral was 20·4 weeks (IQR 14·9-28·0) and ranged between medians of 10·0 and 26·3 weeks between centres. Severe hydrops at first intrauterine transfusion was present in 185 (14·5%) of 1276 pregnancies, with proportions ranging between 0 and 42% between centres. A median of two intrauterine transfusions (IQR 1-4) were done per pregnancy. The fetal access sites used in intrauterine transfusions varied widely between centres. Non-lethal complications in intrauterine transfusions by transfusion site occurred at a lower rate in intrahepatic approaches (2·0%, 95% CI 1·1-3·3) than in placental insertion (6·9%, 5·8-8·0) and free loop (13·3%, 8·9-18·9). The use and indication for intravenous immunoglobulin administration varied widely. 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引用次数: 0

Abstract

Background: Advances in haemolytic disease of the fetus and newborn have led to numerous treatment options. We report practice variations in the management and outcomes of haemolytic disease of the fetus and newborn in at-risk pregnancies.

Methods: In this international, retrospective, observational cohort study, data from cases with moderate or severe haemolytic disease of the fetus and newborn were retrieved from 31 centres in 22 countries. Eligible participants had pregnancies with haemolytic disease of the fetus that led to fetal death at 16 + 0 weeks or later, those treated antenatally with intrauterine transfusion or intravenous immunoglobulins, or neonates without antenatal treatment who were treated with intensive phototherapy, exchange transfusion, or red blood cell transfusions. All patients had confirmed maternal alloantibodies and an antigen-positive fetus incompatible with the maternal alloantibody. Patients with ABO-incompatibility only were excluded. We assessed serological diagnostics and referrals, antenatal treatment and timing, complications, delivery route, and gestational age at birth. Outcomes were analysed in all eligible participants who had complete data available.

Findings: 2443 pregnancies with haemolytic disease of the fetus and newborn treated between Jan 1, 2006, and July 1, 2021, were shared by the centres and analysed between Dec 1, 2021, and March 1, 2023. 23 pregnancies were excluded due to missing information and we included 2420 for further analysis. 1764 (72·9%) of 2420 pregnancies were affected by D-antibodies. 95 (3·9%) of 2420 pregnancies resulted in fetal death. Of the 2325 liveborn neonates, 1349 (58·1%) received any form of antenatal treatment and 976 (41·9%) were only treated postnatally. Median gestational age at referral was 20·4 weeks (IQR 14·9-28·0) and ranged between medians of 10·0 and 26·3 weeks between centres. Severe hydrops at first intrauterine transfusion was present in 185 (14·5%) of 1276 pregnancies, with proportions ranging between 0 and 42% between centres. A median of two intrauterine transfusions (IQR 1-4) were done per pregnancy. The fetal access sites used in intrauterine transfusions varied widely between centres. Non-lethal complications in intrauterine transfusions by transfusion site occurred at a lower rate in intrahepatic approaches (2·0%, 95% CI 1·1-3·3) than in placental insertion (6·9%, 5·8-8·0) and free loop (13·3%, 8·9-18·9). The use and indication for intravenous immunoglobulin administration varied widely. Neonates with intrauterine transfusion were born at a median gestational age of 35·6 weeks (IQR 34·0-36·7), ranging between medians of 33·2 and 37·3 weeks between centres, while neonates without antenatal treatment were born at a median gestational age of 37·3 (IQR 36·3-38·1), ranging between medians of 34·9 and 38·9 weeks between centres.

Interpretation: We found considerable variation in antenatal management and outcomes in haemolytic disease of the fetus and newborn between sites in different countries. Our study shows the capacity of the field to gather valuable data on a rare disease and to optimise care.

Funding: None.

查看原文本刊更多论文

胎儿和新生儿溶血病产前管理和结果的差异：一项国际性、回顾性、观察性队列研究。

背景：胎儿和新生儿溶血病的研究进展带来了许多治疗方案。我们报告了高危妊娠中胎儿和新生儿溶血病的管理和结果的实践差异：在这项国际性、回顾性、观察性队列研究中，我们从 22 个国家的 31 个中心获取了中度或重度胎儿和新生儿溶血病病例的数据。符合条件的参与者包括：妊娠16+0周或之后导致胎儿死亡的溶血病孕妇、接受宫内输血或静脉注射免疫球蛋白治疗的产前孕妇、未接受产前治疗但接受强化光疗、交换输血或输注红细胞治疗的新生儿。所有患者均已确诊母体存在异体抗体，且胎儿抗原阳性，与母体异体抗体不相容。仅 ABO 不相容的患者被排除在外。我们对血清学诊断和转诊、产前治疗和时间、并发症、分娩途径和出生时胎龄进行了评估。结果：各中心共享了 2006 年 1 月 1 日至 2021 年 7 月 1 日期间接受治疗的 2443 例溶血性胎儿和新生儿妊娠，并在 2021 年 12 月 1 日至 2023 年 3 月 1 日期间对这些妊娠进行了分析。由于信息缺失，我们排除了 23 例妊娠，并纳入了 2420 例妊娠进行进一步分析。2420 例妊娠中有 1764 例（72-9%）受到 D 型抗体的影响。2420例孕妇中有95例（3-9%）导致胎儿死亡。在2325名活产新生儿中，1349名（58-1%）接受了任何形式的产前治疗，976名（41-9%）只接受了产后治疗。转诊时的中位胎龄为 20-4 周（IQR 14-9-28-0），各中心的中位数介于 10-0 周和 26-3 周之间。在 1276 例妊娠中，185 例（14-5%）在首次宫内输血时出现严重肾积水，各中心的比例在 0 到 42% 之间。每次宫内输血的中位数为两次（IQR 1-4）。各中心宫内输血时使用的胎儿入路部位差异很大。按输血部位划分，肝内途径（2-0%，95% CI 1-1-3-3）的宫内输血非致死性并发症发生率低于胎盘植入（6-9%，5-8-8-0）和游离环（13-3%，8-9-18-9）。静脉注射免疫球蛋白的使用和适应症差异很大。接受宫内输血的新生儿的中位胎龄为 35-6 周（IQR 34-0-36-7），各中心的中位数介于 33-2 周和 37-3 周之间，而未接受产前治疗的新生儿的中位胎龄为 37-3 周（IQR 36-3-38-1），各中心的中位数介于 34-9 周和 38-9 周之间：我们发现，不同国家的医疗中心在胎儿和新生儿溶血病的产前管理和治疗效果方面存在很大差异。我们的研究表明，该领域有能力收集有关罕见疾病的宝贵数据并优化护理：无。

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来源期刊

Lancet Haematology HEMATOLOGY-

CiteScore

26.00

自引率

0.80%

发文量

323

期刊介绍： Launched in autumn 2014, The Lancet Haematology is part of the Lancet specialty journals, exclusively available online. This monthly journal is committed to publishing original research that not only sheds light on haematological clinical practice but also advocates for change within the field. Aligned with the Lancet journals' tradition of high-impact research, The Lancet Haematology aspires to achieve a similar standing and reputation within its discipline. It upholds the rigorous reporting standards characteristic of all Lancet titles, ensuring a consistent commitment to quality in its contributions to the field of haematology.