Shanes Elisheva, Propst Lauren, Ouyang David W, Ernst Linda M
Department of Pathology and Laboratory Medicine, NorthShore University HealthSystem, Evanston, Illinois.
Pritzker School of Medicine, University of Chicago, Chicago, Illinois.
Pediatr Dev Pathol. 2019 Oct;22(5):465-471. doi: 10.1177/1093526619834809. Epub 2019 Feb 27.
Immune dysregulation, polyendocrinopathy, enteropathy, X-linked (IPEX) is a clinical syndrome associated with mutations in FOXP3 and consequent abnormalities of T regulatory cells. Affected males typically die in infancy or early childhood from a variety of autoimmune conditions. Reports of recurrent pregnancy loss of male fetuses in these families have been accompanied by descriptions of nonimmune fetal hydrops, with or without additional fetal anomalies. Here, we report an additional family affected by IPEX with a novel mutation leading to recurrent second trimester fetal hydrops and intrauterine fetal demise with associated fetal anomalies. This report underscores how careful genetic and pathologic analysis of even midtrimester fetuses can provide important information impacting an entire family. It also further substantiates the use of broad, symptom-targeted genetic screening panels in cases of recurrent pregnancy loss even in the absence of a remarkable pedigree.
免疫失调、多内分泌腺病、肠病、X连锁综合征(IPEX)是一种与FOXP3基因突变及随后的调节性T细胞异常相关的临床综合征。受影响的男性通常在婴儿期或幼儿期死于各种自身免疫性疾病。这些家庭中男性胎儿反复流产的报告伴有非免疫性胎儿水肿的描述,有或没有其他胎儿异常。在此,我们报告了另一个受IPEX影响的家庭,该家庭存在一种新的突变,导致孕中期反复出现胎儿水肿和宫内胎儿死亡,并伴有相关的胎儿异常。本报告强调,即使对孕中期胎儿进行仔细的基因和病理分析,也能提供影响整个家庭的重要信息。它还进一步证实了,即使在没有显著家族史的情况下,对于反复流产的病例,使用广泛的、针对症状的基因筛查 panel 也是合理的。
