扩展pura相关神经发育障碍的临床表型和遗传谱

S. Choi, Heun-Sik Lee, T. Park, Soojin Park, Y. Ko, S. Kim, B. Lim, Ki Joong Kim, J. Chae
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引用次数: 5

摘要

PURA相关神经发育障碍(PURA- ndd)包括5q31.3缺失综合征和PURA综合征。pura - ndd的特征是新生儿张力低下、中度至重度整体发育迟缓/智力残疾(GDD/ID)、面部畸形、癫痫发作、非癫痫性运动障碍和眼科问题。pura - ndd最近在神经发育队列中被发现并被低估,但其诊断仍然具有挑战性。方法回顾性分析pura - ndd患者的临床特征、遗传谱和诊断过程。结果我们报告了2例5q31.3微缺失和5例PURA致病变异。他们在新生儿期表现为张力不足(7/ 7,100 %),喂养困难(4/ 5,80 %)和呼吸问题(4/ 7,57 %)。所有患者均有严重的GDD/ID,不能独立行走和言语反应。最常见的面部特征为上朱砂张开,中鼻长,鼻梁前倾,视觉固定和追踪不良,伴或不伴眼球震颤(5/ 7,71.4%)。5q31.3微缺失综合征与PURA综合征在临床表型上无显著差异。pura - ndd需要被视为严重张力不足的鉴别诊断,包括自出生以来的喂养困难和严重发育迟缓,具有明显的面部和眼科特征。结论sour数据扩展了PURA-NDD的表型和遗传谱。基于详细表型评估的下一代测序方法将缩短诊断延迟,并将帮助这种罕见疾病成为神经发育迟缓的可识别原因。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Expanding the clinical phenotype and genetic spectrum of PURA-related neurodevelopmental disorders
BACKGROUND PURA-related neurodevelopmental disorders (PURA-NDDs) include 5q31.3 deletion syndrome and PURA syndrome. PURA-NDDs are characterized by neonatal hypotonia, moderate to severe global developmental delay/intellectual disability (GDD/ID), facial dysmorphism, epileptic seizures, nonepileptic movement disorders, and ophthalmological problems. PURA-NDDs have recently been identified and underestimated in neurodevelopmental cohorts, but their diagnosis is still challenging. METHODS We retrospectively reviewed the clinical characteristics, genetic spectrum, and diagnostic journey of patients with PURA-NDDs. RESULTS We report 2 patients with 5q31.3 microdeletion and 5 with PURA pathogenic variants. They demonstrated hypotonia (7/7, 100%), feeding difficulties (4/5, 80%), and respiratory problems (4/7, 57%) in the neonatal period. All of them had severe GDD/ID and could not achieve independent walking and verbal responses. Distinctive facial features of open-tented upper vermilion, long philtrum, and anteverted nares and poor visual fixation and tracking with or without nystagmus were most commonly found (5/7, 71.4%). There were no significant differences in clinical phenotypes between 5q31.3 microdeletion syndrome and PURA syndrome. PURA-NDDs need to be considered as a differential diagnosis in individuals who show severe hypotonia, including feeding difficulties since birth and severe developmental retardation with distinctive facial and ophthalmological features. CONCLUSIONS Our data expands the phenotypic and genetic spectrum of PURA-NDD. Next-generation sequencing methods based on the detailed phenotypic evaluation would shorten the diagnostic delay and would help this rare disorder become a recognizable cause of neurodevelopmental delay.
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