Characterization of severity of hemolytic disease of the fetus and newborn due to Rhesus antigen alloimmunization

AJOG global reports Pub Date : 2025-02-01 DOI:10.1016/j.xagr.2024.100439

Alexis A. Krumme ScD , Robert Y. Suruki ScD , Clair Blacketer MPH , Jill Hardin PhD , Joel N. Swerdel PhD , May Lee Tjoa PhD , Kara B. Markham MD

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引用次数: 0

Abstract

BACKGROUND

Clinical manifestations of hemolytic disease of the fetus and newborn include anemia, hyperbilirubinemia, hydrops fetalis, kernicterus, and fetal or neonatal demise. More than 50 antibodies are linked to hemolytic disease of the fetus and newborn, with Rhesus (including D and c) and Kell antigens carrying the highest risk of disease. To date, a multicenter, comprehensive evaluation of hemolytic disease of the fetus and newborn due to Rhesus antigen alloantibodies in the United States has not been undertaken.

OBJECTIVE

This study aimed to implement a novel severity index to characterize the real-world disease spectrum of hemolytic disease of the fetus and newborn due to alloantibodies from the Rhesus class.

STUDY DESIGN

This retrospective cohort study was conducted in neonates with commercial insurance available through Optum's deidentified Clinformatics® Data Mart Database (Clinformatics®) and Merative MarketScan® Commercial Claims and Encounters (CCAE) Database from 2000 to 2022. Neonatal and maternal records were linked algorithmically by shared family identifier. A hierarchical severity index was developed for neonates with a Rhesus antigen hemolytic disease of the fetus and newborn diagnosis code in the first 30 days of life, using antenatal and neonatal diagnoses and treatments: Severe (neonatal death, hydrops fetalis, intrauterine transfusion); Moderate (neonatal exchange transfusion); Mild (neonatal simple transfusion); Minimal (neonatal phototherapy or hyperbilirubinemia). Maternal, antenatal, and perinatal demographic and clinical characteristics were summarized descriptively by severity.

RESULTS

In Clinformatics® and Commercial Claims and Encounters Database, respectively, 1927 and 1268 neonates met the inclusion criteria. Most (93.1% Clinformatics®; 93.5% CCAE Database) displayed minimal severity, although in both databases nearly 40% of these neonates still required phototherapy. More neonates were mildly affected (3.3% Clinformatics®; 2.2% Commercial Claims and Encounters Database) than moderately (1.0% Clinformatics®; 1.1% Commercial Claims and Encounters Database). In Clinformatics® and Commercial Claims and Encounters Database, respectively, severe hemolytic disease of the fetus and newborn affected 2.6% and 3.2% of neonates, 54% and 46% of whom received exchange or simple transfusions. Severely affected neonates were more commonly delivered by cesarean delivery and at a lower gestational age (34.1 weeks Clinformatics®; 35.4 weeks Commercial Claims and Encounters Database) than those minimally affected (38.5 weeks Clinformatics®; 38.4 weeks Commercial Claims and Encounters Database).

CONCLUSION

Results across 2 real-world US databases found that although most neonates affected by hemolytic disease of the fetus and newborn due to Rhesus antigen alloantibodies did not require intervention beyond phototherapy, nearly 7% experienced disease severity requiring invasive intervention or resulting in neonatal mortality. More severely affected neonates had lower gestational age at birth, higher rates of cesarean delivery and neonatal intensive care unit admission, and longer length of hospital stay at birth compared with minimally affected neonates. The HDFN Severity Index is a useful tool to characterize hemolytic disease of the fetus and newborn and may be valuable alongside guideline-driven care in subsequent pregnancies.

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恒河猴抗原同种免疫对胎儿和新生儿溶血性疾病严重程度的影响

背景：胎儿和新生儿溶血性疾病的临床表现包括贫血、高胆红素血症、胎儿水肿、核黄疸和胎儿或新生儿死亡。超过50种抗体与胎儿和新生儿的溶血性疾病有关，恒河（包括D和c）和凯尔抗原携带的疾病风险最高。迄今为止，在美国尚未对恒河猴抗原同种异体抗体引起的胎儿和新生儿溶血性疾病进行多中心、全面的评估。目的：本研究旨在建立一种新的严重程度指数，以表征由恒河猴类同种异体抗体引起的胎儿和新生儿溶血性疾病的真实疾病谱。研究设计：这项回顾性队列研究是在2000年至2022年期间通过Optum的确定的Clinformatics®数据集市数据库（Clinformatics®）和Merative MarketScan®商业索赔和遭遇（CCAE）数据库获得商业保险的新生儿中进行的。新生儿和母亲的记录通过共享的家庭标识符进行算法链接。采用产前和新生儿诊断和治疗方法，为出生30天内患有恒河猴抗原溶血性疾病的新生儿制定了分级严重程度指数：严重（新生儿死亡、胎儿水肿、宫内输血）；中度（新生儿换血）；轻度（新生儿单纯输血）；最小（新生儿光疗或高胆红素血症）。根据严重程度对孕产妇、产前和围产期人口统计学和临床特征进行描述性总结。结果在Clinformatics®和Commercial Claims and Encounters数据库中，分别有1927例和1268例新生儿符合纳入标准。大多数(93.1% Clinformatics®；93.5% CCAE数据库)显示轻微的严重性，尽管在两个数据库中，近40%的新生儿仍然需要光疗。更多的新生儿受到轻度影响(3.3% Clinformatics®；2.2%商业索赔和遭遇数据库)比中度(1.0% Clinformatics®；1.1%商业索赔和事故数据库)。在Clinformatics®和Commercial Claims and Encounters数据库中，胎儿和新生儿的严重溶血性疾病分别影响2.6%和3.2%的新生儿，其中54%和46%接受交换或简单输血。严重影响的新生儿更常见于剖宫产和低胎龄分娩(34.1周Clinformatics®；35.4周商业索赔和遭遇数据库)比受影响最小的患者(38.5周Clinformatics®；38.4周商业索赔和遭遇数据库)。结论：来自美国2个真实世界数据库的结果发现，尽管大多数因恒河猴抗原同种抗体而患胎儿和新生儿溶血性疾病的新生儿不需要光治疗以外的干预，但近7%的疾病严重程度需要侵入性干预或导致新生儿死亡。与受影响最小的新生儿相比，受影响更严重的新生儿出生时胎龄更低，剖宫产率和新生儿重症监护病房入院率更高，出生时住院时间更长。HDFN严重程度指数是表征胎儿和新生儿溶血性疾病的有用工具，在随后的妊娠中与指南驱动的护理一起可能是有价值的。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

AJOG global reports Endocrinology, Diabetes and Metabolism, Obstetrics, Gynecology and Women's Health, Perinatology, Pediatrics and Child Health, Urology

CiteScore

1.20

自引率

0.00%

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