%0 Journal Article %J J Med Genet %D 2021 %T Diagnostic yield and clinical impact of exome sequencing in early-onset scoliosis (EOS). %A Zhao, Sen %A Zhang, Yuanqiang %A Chen, Weisheng %A Li, Weiyu %A Wang, Shengru %A Wang, Lianlei %A Zhao, Yanxue %A Lin, Mao %A Ye, Yongyu %A Lin, Jiachen %A Zheng, Yu %A Liu, Jiaqi %A Zhao, Hengqiang %A Yan, Zihui %A Yang, Yongxin %A Huang, Yingzhao %A Lin, Guanfeng %A Chen, Zefu %A Zhang, Zhen %A Liu, Sen %A Jin, Lichao %A Wang, Zhaoyang %A Chen, Jingdan %A Niu, Yuchen %A Li, Xiaoxin %A Wu, Yong %A Wang, Yipeng %A Du, Renqian %A Gao, Na %A Zhao, Hong %A Yang, Ying %A Liu, Ying %A Tian, Ye %A Li, Wenli %A Zhao, Yu %A Liu, Jia %A Yu, Bin %A Zhang, Na %A Yu, Keyi %A Yang, Xu %A Li, Shugang %A Xu, Yuan %A Hu, Jianhua %A Liu, Zhe %A Shen, Jianxiong %A Zhang, Shuyang %A Su, Jianzhong %A Khanshour, Anas M %A Kidane, Yared H %A Ramo, Brandon %A Rios, Jonathan J %A Liu, Pengfei %A Sutton, V Reid %A Posey, Jennifer E %A Wu, Zhihong %A Qiu, Guixing %A Wise, Carol A %A Zhang, Feng %A James R Lupski %A Zhang, Jianguo %A Wu, Nan %K Adolescent %K Adult %K Age of Onset %K Child, Preschool %K China %K Cohort Studies %K Exome %K Exome Sequencing %K Female %K Genetic Predisposition to Disease %K Humans %K Male %K Retrospective Studies %K Scoliosis %X

BACKGROUND: Early-onset scoliosis (EOS), defined by an onset age of scoliosis less than 10 years, conveys significant health risk to affected children. Identification of the molecular aetiology underlying patients with EOS could provide valuable information for both clinical management and prenatal screening.

METHODS: In this study, we consecutively recruited a cohort of 447 Chinese patients with operative EOS. We performed exome sequencing (ES) screening on these individuals and their available family members (totaling 670 subjects). Another cohort of 13 patients with idiopathic early-onset scoliosis (IEOS) from the USA who underwent ES was also recruited.

RESULTS: After ES data processing and variant interpretation, we detected molecular diagnostic variants in 92 out of 447 (20.6%) Chinese patients with EOS, including 8 patients with molecular confirmation of their clinical diagnosis and 84 patients with molecular diagnoses of previously unrecognised diseases underlying scoliosis. One out of 13 patients with IEOS from the US cohort was molecularly diagnosed. The age at presentation, the number of organ systems involved and the Cobb angle were the three top features predictive of a molecular diagnosis.

CONCLUSION: ES enabled the molecular diagnosis/classification of patients with EOS. Specific clinical features/feature pairs are able to indicate the likelihood of gaining a molecular diagnosis through ES.

%B J Med Genet %V 58 %P 41-47 %8 2021 Jan %G eng %N 1 %1 https://www.ncbi.nlm.nih.gov/pubmed/32381727?dopt=Abstract %R 10.1136/jmedgenet-2019-106823 %0 Journal Article %J Hum Mutat %D 2020 %T TBX6 missense variants expand the mutational spectrum in a non-Mendelian inheritance disease. %A Chen, Weisheng %A Lin, Jiachen %A Wang, Lianlei %A Li, Xiaoxin %A Zhao, Sen %A Liu, Jiaqi %A Akdemir, Zeynep C %A Zhao, Yanxue %A Du, Renqian %A Ye, Yongyu %A Song, Xiaofei %A Zhang, Yuanqiang %A Yan, Zihui %A Yang, Xinzhuang %A Lin, Mao %A Shen, Jianxiong %A Wang, Shengru %A Gao, Na %A Yang, Ying %A Liu, Ying %A Li, Wenli %A Liu, Jia %A Zhang, Na %A Yang, Xu %A Xu, Yuan %A Zhang, Jianguo %A Delgado, Mauricio R %A Posey, Jennifer E %A Qiu, Guixing %A Rios, Jonathan J %A Liu, Pengfei %A Wise, Carol A %A Zhang, Feng %A Wu, Zhihong %A James R Lupski %A Wu, Nan %K Alleles %K Cell Line %K Exome Sequencing %K Female %K Gene Expression %K Genes, Reporter %K Genetic Association Studies %K Genetic Predisposition to Disease %K Genotype %K Haplotypes %K Humans %K Inheritance Patterns %K Male %K Models, Molecular %K Molecular Diagnostic Techniques %K Mutation, Missense %K Phenotype %K Protein Conformation %K Radiography %K Sequence Analysis, DNA %K Spine %K Structure-Activity Relationship %K T-Box Domain Proteins %X

Congenital scoliosis (CS) is a birth defect with variable clinical and anatomical manifestations due to spinal malformation. The genetic etiology underlying about 10% of CS cases in the Chinese population is compound inheritance by which the gene dosage is reduced below that of haploinsufficiency. In this genetic model, the trait manifests as a result of the combined effect of a rare variant and common pathogenic variant allele at a locus. From exome sequencing (ES) data of 523 patients in Asia and two patients in Texas, we identified six TBX6 gene-disruptive variants from 11 unrelated CS patients via ES and in vitro functional testing. The in trans mild hypomorphic allele was identified in 10 of the 11 subjects; as anticipated these 10 shared a similar spinal deformity of hemivertebrae. The remaining case has a homozygous variant in TBX6 (c.418C>T) and presents a more severe spinal deformity phenotype. We found decreased transcriptional activity and abnormal cellular localization as the molecular mechanisms for TBX6 missense loss-of-function alleles. Expanding the mutational spectrum of TBX6 pathogenic alleles enabled an increased molecular diagnostic detection rate, provided further evidence for the gene dosage-dependent genetic model underlying CS, and refined clinical classification.

%B Hum Mutat %V 41 %P 182-195 %8 2020 Jan %G eng %N 1 %1 https://www.ncbi.nlm.nih.gov/pubmed/31471994?dopt=Abstract %R 10.1002/humu.23907