神经发育障碍
小头畸形
桑格测序
外显子组测序
表型
全球发育迟缓
智力残疾
胡说
遗传学
生物
损失函数
无义突变
基因
突变
外显子组
错义突变
作者
Ahmed Waqas,Romana Liaqat,Sidrah Shaheen,Ali Zaman Khan,Mujahid,Alaa Hamed Habib,Najat Binothman,Majidah Aljadani,Zamrud Zehri,Shabnam Shaheen,Afnan Alkathiri,Rubina Naz,Muhammad Umair,Safdar Abbas
摘要
Neurodevelopmental disorders (NDDs) are classified as a group of disorders affecting function and development of the brain and having wide clinical variability. Herein, we describe two affected individuals segregating a recessive NDD. The affected individuals exhibited phenotypes such as global developmental delay (GDD), intellectual disability (ID), microcephaly and speech delay. Whole-exome sequencing (WES) followed by bidirectional Sanger sequencing techniques identified a homozygous nonsense variant (c.466C > T; p.Gln156*) in the PPFIBP1 gene (NM_003622.4) that segregated with the disease phenotype. Further, to elucidate the effect of the variant on protein structure, 3D protein modelling was performed for the mutant and normal protein that suggested substantial reduction of the mutant protein. Our data support the evidence that PPFIBP1 has a pivotal role in neurodevelopment in humans, and loss-of-function variants cause clinically variable neurodevelopmental phenotypes.
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