量化神经发育遗传综合征和特发性神经发育障碍的神经行为特征。

IF 3.8 2区 医学 Q1 CLINICAL NEUROLOGY
Thomas W Frazier, Robyn M Busch, Patricia Klaas, Katherine Lachlan, Eva Loth, Constance Smith-Hicks, Mustafa Sahin, Antonio Y Hardan, Mirko Uljarevic
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引用次数: 0

摘要

目的:研究三种遗传综合征(PTEN hamartoma肿瘤综合征、马兰综合征[NFIX基因突变]和SYNGAP1相关障碍)、其他神经发育遗传综合征(NDGS)混合组、特发性神经发育障碍和神经典型对照组参与者的神经行为发现:方法:采用纵向病例对照设计,由护理人员报告 498 名参与者的神经行为信息(PTEN hamartoma 肿瘤综合征 n = 112、马兰综合征 n = 24、SYNGAP1 相关障碍 n = 47、其他 NDGS n = 72、特发性神经发育障碍 n = 48)、特发性神经发育障碍 n = 54、神经畸形兄弟姐妹 n = 74 和非相关神经畸形对照组参与者 n = 115)在三个时间点(基线、1 个月和 4 个月随访)的神经行为信息。结果显示NET量表具有良好的量表可靠性和重测可靠性。神经行为结果出现了独特的模式,SYNGAP1相关障碍和马兰综合征的症状和技能模式普遍比其他组患者严重。估计的认知水平、语言水平和自闭症谱系障碍的存在可以部分解释这些模式。然而,即使考虑到这些因素,群体差异依然存在。报告了可靠的变化指数:与神经发育障碍相关的遗传综合征具有独特的神经行为特征,可为未来临床试验中选择结果测量指标提供参考。在临床实践中,NET可能是一种有用的筛查和监测工具,因为许多患者很难经常到医院就诊。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Quantifying neurobehavioral profiles across neurodevelopmental genetic syndromes and idiopathic neurodevelopmental disorders.

Aim: To examine neurobehavioral findings in three genetic syndromes (PTEN hamartoma tumor syndrome, Malan syndrome [mutations in the NFIX gene], and SYNGAP1-related disorder), a mixed group of other neurodevelopmental genetic syndromes (NDGS), idiopathic neurodevelopmental disorder, and neurotypical control participants.

Method: Using a longitudinal case-control design, caregivers reported neurobehavioral information for 498 participants (PTEN hamartoma tumor syndrome n = 112, Malan syndrome n = 24, SYNGAP1-related disorder n = 47, other NDGS n = 72, idiopathic neurodevelopmental disorder n = 54, neurotypical siblings n = 74, and unrelated neurotypical control participants n = 115) at three timepoints (baseline, and 1-month and 4-month follow-ups) using the online-administered Neurobehavioral Evaluation Tool (NET).

Results: NET scales had good scale and test-retest reliability. Unique patterns of neurobehavioral findings emerged, with SYNGAP1-related disorder and Malan syndrome showing generally more severe symptom and skill patterns than for other groups of patients. Patterns could be partly accounted for by estimated cognitive level, speech level, and the presence of autism spectrum disorder. However, even when accounting for these factors, group differences remained. Reliable change indices are reported.

Interpretation: Genetic syndromes associated with neurodevelopmental disorders present with unique neurobehavioral profiles that can inform selection of outcome measures in future clinical trials. The NET may be a useful screening and monitoring instrument in clinical practice, where frequent in-person clinic attendance is difficult for many patients.

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来源期刊
CiteScore
7.80
自引率
13.20%
发文量
338
审稿时长
3-6 weeks
期刊介绍: Wiley-Blackwell is pleased to publish Developmental Medicine & Child Neurology (DMCN), a Mac Keith Press publication and official journal of the American Academy for Cerebral Palsy and Developmental Medicine (AACPDM) and the British Paediatric Neurology Association (BPNA). For over 50 years, DMCN has defined the field of paediatric neurology and neurodisability and is one of the world’s leading journals in the whole field of paediatrics. DMCN disseminates a range of information worldwide to improve the lives of disabled children and their families. The high quality of published articles is maintained by expert review, including independent statistical assessment, before acceptance.
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