Quantitative Phenotype Morbidity Description of SATB2-Associated Syndrome

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC ACS Applied Electronic Materials Pub Date : 2023-04-26 DOI:10.1155/2023/8200176
Y. Zarate, K. Bosanko, Amrit Kannan, Ashlen Thomason, Beth Nutt, Nihit Kumar, K. Simmons, Aaron Hiegert, Larry D Hartzell, Adam Johnson, Tabitha Prater, Eduardo Pérez-Palma, Tobias Brünger, A. Stefanski, D. Lal, A. Caffrey
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Abstract

Characterized by developmental delay with severe speech delay, dental anomalies, cleft palate, skeletal abnormalities, and behavioral difficulties, SATB2-associated syndrome (SAS) is caused by pathogenic variants in SATB2. The SAS phenotype range of severity has been documented previously in large series. Using data from the SAS registry, we present the SAS severity score, a comprehensive scoring rubric that encompasses 15 different individual neurodevelopmental and systemic features. Higher (more severe) systemic and total (sum of neurodevelopmental and systemic scores) scores were seen for null variants located after amino acid 350 (the start of the CUT1 domain), the recurrent missense Arg389Cys variant ( n = 10 ), intragenic deletions, and larger chromosomal deletions. The Arg389Cys variant had the highest cognitive, verbal, and sialorrhea severity scores, while large chromosomal deletions had the highest expressive, ambulation, palate, feeding and growth, neurodevelopmental, and total scores. Missense variants not located in the CUT1 or CUT2 domain scored lower in several subcategories. We conclude that the SAS severity score allows quantitative phenotype morbidity description that can be used in routine clinical counseling. Further refinement and validation of the SAS severity score are expected over time. All data from this project can be interactively explored in a new portal.
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SATB2相关综合征的定量表型发病率描述
SATB2相关综合征(SAS)以发育迟缓伴严重言语迟缓、牙齿异常、腭裂、骨骼异常和行为困难为特征,由SATB2的致病性变异引起。严重程度的SAS表型范围以前已经有大量文献记载。使用SAS注册表中的数据,我们提出了SAS严重程度评分,这是一个综合评分标准,包括15种不同的个体神经发育和系统特征。位于氨基酸350(CUT1结构域的起点)之后的无效变体、复发性错义Arg389Cys变体(n=10)、基因内缺失和较大的染色体缺失的系统和总(神经发育和系统评分的总和)评分更高(更严重)。Arg389Cys变体的认知、言语和唾液溢严重程度得分最高,而大型染色体缺失的表达、行走、味觉、进食和生长、神经发育和总分最高。不位于CUT1或CUT2结构域的错义变体在几个子类别中得分较低。我们的结论是,SAS严重程度评分允许定量表型发病率描述,可用于常规临床咨询。预计随着时间的推移,SAS严重程度评分将进一步细化和验证。该项目中的所有数据都可以在新的门户中进行交互式浏览。
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CiteScore
7.20
自引率
4.30%
发文量
567
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