Exploring the molecular pathways linking sleep phenotypes and POGZ-associated neurodevelopmental disorder

表型 生物 自闭症谱系障碍 遗传学 神经发育障碍 自闭症 睡眠障碍 生物信息学 基因 神经科学 医学 精神科 认知
作者
Bruna Pereira Marquezini,Mariana Moysés‐Oliveira,Anna Kloster,Lais Cunha,Tais Bassani Deconto,Amanda Cristina Mosini,Pedro M. Guerreiro,Mayara Paschalidis,Luana Nayara Gallego Adami,Mônica L. Andersen,Sérgio Tufik
出处
期刊:Journal of Medical Genetics [BMJ]
卷期号:61 (6): 586-589 被引量:1
标识
DOI:10.1136/jmg-2023-109508
摘要

Pogo transposable element-derived protein with ZNF domain ( POGZ ) gene encodes a chromatin regulator and rare variants on this gene have been associated with a broad spectrum of neurodevelopmental disorders, such as White-Sutton syndrome. Patient clinical manifestations frequently include developmental delay, autism spectrum disorder and obesity. Sleep disturbances are also commonly observed in these patients, yet the biological pathways which link sleep traits to the POGZ -associated syndrome remain unclear. We screened for sleep implications among individuals with causative POGZ variants previously described. Sleep disturbances were observed in 52% of patients, and being obese was not observed as a risk factor for sleep problems. Next, we identified genes associated with sleep-associated traits among the POGZ regulatory targets, aiming to uncover the molecular pathways that, when disrupted by POGZ loss of function, contribute to the aetiology of sleep phenotypes in these patients. The intersect between POGZ targets and sleep-related genes was used in a pathway enrichment analysis. Relevant pathways among these overlapping genes are involved in the regulation of circadian rhythm, tau protein binding, ATPase activator activity. This study may represent the beginning for novel functional investigations on shared molecular mechanisms between sleep disturbances and rare developmental syndromes related to POGZ and its regulatory targets.

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