NAFTNet回顾性报道地塞米松治疗抗ro /SSA介导的胎儿心脏传导阻滞。

Sherzana Sunderji, Shabnam Peyvandi, Edgar Jaeggi, Anita Szwast, Greg Ryan, Francine Tessier, Saad Siddiqui, Bettina Cuneo, Shreya Sheth, Marjorie Treadwell, Michele Frommelt, Shifa Turan, Joshua Copel, Stephen Emery, Larry Rand, Anita J Moon-Grady
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引用次数: 3

摘要

背景:完全性房室传导阻滞(CAVB)是母体抗体阳性的并发症,胎儿疾病的治疗在有效性和安全性方面存在争议。我们假设地塞米松治疗胎儿抗ro /SSA抗体介导的心脏病的妊娠结局优于预期治疗。方法:对2010年1月至2018年12月北美胎儿治疗网络(NAFTNet)中心报告的抗ro /SSA抗体阳性妊娠伴胎导病进行回顾性多中心队列研究。主要结局包括:胎儿死亡、羊水过少、生长受限、早产和新的母体合并症。次要结局包括:接受地塞米松治疗与未接受地塞米松治疗的产妇/胎儿对28天前起搏器、移植和新生儿死亡。结果:127例抗ro /SSA阳性妊娠中,地塞米松治疗98例,未治疗29例。在接受治疗的患者中,61/96(63.5%)达到主要结局,包括45/91(49.4%)早产;20名母亲在治疗期间出现合并症(5例胎儿死亡,10例生长受限,14例羊水过少,2例新发/加重妊娠糖尿病)。在未治疗组中,15/25(60%)达到主要结局,包括11/22(50%)早产和4名母亲在妊娠期间出现合并症(胎儿死亡3例,1例生长受限,1例新发产妇高血压)。至于次要结局,37/96(43%)接受治疗的胎儿需要放置起搏器或在28天内死亡,而未接受治疗的13/25(52%)需要放置起搏器,在28天前死亡或需要移植名单。排除终止妊娠,未经治疗的患者无移植生存期为17(68%),而接受治疗的患者无移植生存期为85(89%)。结论:虽然抗ro /SSA阳性妊娠中使用地塞米松与不良妊娠结局的高发生率相关,但未经治疗的阳性妊娠中也有类似的高发生率。这表明母体疾病本身是独立于地塞米松影响妊娠并发症。我们的数据表明,治疗降低了新生儿发病率和总体死亡率,而没有增加总体妊娠并发症,值得进一步研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
NAFTNet retrospective report on the treatment of anti-Ro/SSA mediated fetal heart block with dexamethasone.

Background: Complete atrioventricular block (CAVB) is a complication of maternal antibody positivity and treatment of fetal disease is controversial in terms of efficacy and safety. We hypothesized that dexamethasone treatment for fetal anti-Ro/SSA antibody-mediated cardiac disease leads to better pregnancy outcomes than expectant management.

Methods: A retrospective multi-center cohort study of anti-Ro/SSA antibody positive pregnancies with fetal conduction disease reported by participating North American Fetal Therapy Network (NAFTNet) centers between January 2010 and December 2018. The primary outcomes included: fetal death, oligohydramnios, growth restriction, preterm delivery, and new maternal comorbidities. Secondary outcomes included: pacemaker prior to 28 days, transplantation, and neonatal death in maternal/fetal dyads treated with dexamethasone versus not.

Results: In 127 anti-Ro/SSA positive pregnancies, 98 were treated with dexamethasone and 29 were not. Of those treated, 61/96 (63.5%) met the primary outcome including 45/91 (49.4%) premature deliveries; 20 mothers developed comorbidities during treatment (fetal death 5, 10 growth restriction, 14 oligohydramnios, two new/worsening gestational diabetes). In the untreated group, 15/25 (60%) met the primary outcome including 11/22 (50%) premature deliveries and four mothers developing comorbidities during their pregnancy (fetal death 3, one growth restriction, one new onset maternal hypertension). Regarding secondary outcomes, 37/96 (43%) treated fetuses required a pacemaker or died by 28 days, while untreated 13/25 (52%) required pacemaker placement, died prior to 28 days or required listing for transplantation. Excluding terminations, survival without transplant was 17 (68%) in untreated and 85 (89%) in treated patients (p<.01).

Conclusions: While the use of dexamethasone in anti-Ro/SSA positive pregnancies is associated with a high rate of poor pregnancy outcomes, there was an unexpected similarly high rate in untreated positive pregnancies. This suggests that the maternal disease itself is influencing pregnancy complications independent of dexamethasone. Our data, which show that treatment decreases neonatal morbidity and overall mortality without increasing overall pregnancy complications, warrant further study.

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