Lane Michael, Allen Nicholas M, Letshwiti Johannes
Paediatrics, National University of Ireland, Galway, Ireland.
Paediatrics, Galway University Hospitals, Galway, Ireland.
BMJ Case Rep. 2023 Mar 21;16(3):e253035. doi: 10.1136/bcr-2022-253035.
TARP (talipes equinovarus, atrial septal defect (ASD), Robin sequence, persistent left superior vena cava) syndrome is a rare X-linked disorder affecting the gene. It was previously viewed as universally fatal in the early neonatal period, however, recent cases have shown patients surviving beyond this stage. We present a male toddler diagnosed with TARP syndrome due to a a previously unreported splicing mutation c.2295+1G>A in the gene. At birth, he had an ASD and Robin sequence, two of the eponymous features, as well as other associated phenotypic features. During infancy, he had an extremely high alpha-fetoprotein, conjugated hyperbilirubinaemia and thrombocytopaenia, features not previously described in TARP syndrome. We discuss these findings as well as our patient's survival past the neonatal period with special consideration to recent genotype-phenotypes correlations.
TARP(马蹄内翻足、房间隔缺损(ASD)、罗宾序列征、永存左上腔静脉)综合征是一种罕见的X连锁疾病,影响该基因。它以前被认为在新生儿早期普遍致命,然而,最近的病例显示患者能存活超过这个阶段。我们报告一名男童,因该基因中一个先前未报道的剪接突变c.2295+1G>A被诊断为TARP综合征。出生时,他患有房间隔缺损和罗宾序列征这两个该综合征的特征性表现,以及其他相关的表型特征。婴儿期,他甲胎蛋白极高、结合胆红素血症和血小板减少,这些特征以前在TARP综合征中未曾描述。我们讨论这些发现以及我们的患者在新生儿期后的存活情况,并特别考虑最近的基因型-表型相关性。
