复合杂合度
张力减退
神经退行性变
表型
杂合子优势
基因
生物
错义突变
遗传学
脑病
萎缩
未能茁壮成长
微管
基因型
医学
疾病
病理
内科学
作者
Chih‐Ling Chen,Chien‐Nan Lee,Yin‐Hsiu Chien,Wuh‐Liang Hwu,Tung‐Ming Chang,Ni‐Chung Lee
出处
期刊:Children (Basel)
[Multidisciplinary Digital Publishing Institute]
日期:2021-12-05
卷期号:8 (12): 1140-1140
被引量:5
标识
DOI:10.3390/children8121140
摘要
Mutations in tubulin-specific chaperon D (TBCD), the gene encoding one of the co-chaperons required for the assembly and disassembly of the α/β-tubulin heterodimers, have been reported to cause perturbed microtubule dynamics, resulting in debilitating early-onset progressive neurodegenerative disorder. Here, we identified two novel TBCD variants, c.1340C>T (p.Ala447Val), and c.817+2T>C, presented as compound heterozygotes in two affected siblings born to unaffected carrier parents. Clinical features included early-onset neurodegeneration, failure to thrive, respiratory failure, hypotonia, muscle weakness and atrophy and seizures. We established the genotype-phenotype relationship of these TBCD pathogenic variants and provided insight into the protein structural alteration that may contribute to this chaperone-associated tubulinopathy.
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