Department of Psychiatry & Behavioral Sciences, University of Kansas Medical Center, 3901 Rainbow Blvd. MS 4015, Kansas City, KS 66160, USA.
Department of Pediatrics, University of Kansas Medical Center, 3901 Rainbow Blvd. MS 4015, Kansas City, KS 66160, USA.
Int J Mol Sci. 2021 Feb 7;22(4):1660. doi: 10.3390/ijms22041660.
The 15q11.2 BP1-BP2 deletion (Burnside-Butler) syndrome is emerging as the most common cytogenetic finding in patients with neurodevelopmental or autism spectrum disorders (ASD) presenting for microarray genetic testing. Clinical findings in Burnside-Butler syndrome include developmental and motor delays, congenital abnormalities, learning and behavioral problems, and abnormal brain findings. To better define symptom presentation, we performed comprehensive cognitive and behavioral testing, collected medical and family histories, and conducted clinical genetic evaluations. The 15q11.2 BP1-BP2 region includes the , , , and genes. To determine if additional genomic variation outside of the 15q11.2 region influences expression of symptoms in Burnside-Butler syndrome, whole-exome sequencing was performed on the parents and affected children for the first time in five families with at least one parent and child with the 15q1l.2 BP1-BP2 deletion. In total, there were 453 genes with possibly damaging variants identified across all of the affected children. Of these, 99 genes had exclusively de novo variants and 107 had variants inherited exclusively from the parent without the deletion. There were three genes (, , and ) with de novo variants that encode proteins evidenced to interact with CYFIP1. In addition, one other gene of interest () had variants inherited from the parent without the deletion and encoded a protein interacting with CYFIP1. The affected individuals commonly displayed a neurodevelopmental phenotype including ASD, speech delay, abnormal reflexes, and coordination issues along with craniofacial findings and orthopedic-related connective tissue problems. Of the 453 genes with variants, 35 were associated with ASD. On average, each affected child had variants in 6 distinct ASD-associated genes (x¯ = 6.33, sd = 3.01). In addition, 32 genes with variants were included on clinical testing panels from Clinical Laboratory Improvement Amendments (CLIA) approved and accredited commercial laboratories reflecting other observed phenotypes. Notably, the dataset analyzed in this study was small and reported results will require validation in larger samples as well as functional follow-up. Regardless, we anticipate that results from our study will inform future research into the genetic factors influencing diverse symptoms in patients with Burnside-Butler syndrome, an emerging disorder with a neurodevelopmental behavioral phenotype.
15q11.2BP1-BP2 缺失(Burnside-Butler)综合征在因微阵列基因检测而就诊的神经发育或自闭症谱系障碍(ASD)患者中,是最常见的细胞遗传学发现。Burnside-Butler 综合征的临床发现包括发育和运动迟缓、先天性异常、学习和行为问题以及异常的脑部发现。为了更好地定义症状表现,我们进行了全面的认知和行为测试,收集了医疗和家族史,并进行了临床遗传评估。15q11.2 区包括、、、和基因。为了确定 15q11.2 区以外的基因组是否会影响 Burnside-Butler 综合征症状的表达,我们首次对五个有父母和孩子患有 15q1l.2 BP1-BP2 缺失的家庭进行了全外显子测序。总共有 453 个可能具有破坏性变异的基因在所有受影响的儿童中被识别出来。其中,99 个基因仅具有新生变异,107 个基因仅从没有缺失的父母那里遗传。有三个基因(、和)具有新生变异,这些变异编码的蛋白质与 CYFIP1 相互作用。此外,还有一个感兴趣的基因()从没有缺失的父母那里遗传了变异,并编码与 CYFIP1 相互作用的蛋白质。受影响的个体通常表现出神经发育表型,包括 ASD、言语延迟、异常反射和协调问题,以及颅面发现和骨科相关的结缔组织问题。在具有变异的 453 个基因中,有 35 个与 ASD 相关。平均而言,每个受影响的孩子都有 6 个不同的 ASD 相关基因的变异(x¯=6.33,sd=3.01)。此外,在临床实验室改进修正案(CLIA)批准和认可的商业实验室的临床检测面板中,有 32 个具有变异的基因被列入其中,反映了其他观察到的表型。值得注意的是,本研究分析的数据集较小,报告的结果需要在更大的样本中进行验证,并进行功能随访。尽管如此,我们预计我们的研究结果将为未来研究影响 Burnside-Butler 综合征患者不同症状的遗传因素提供信息,这是一种具有神经发育行为表型的新兴疾病。
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