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128 例疑似先天性骨骼畸形的捷克患者中参与人类骨骼发育的选定基因的临床遗传学分析。

Clinical-genetic analysis of selected genes involved in the development of the human skeleton in 128 Czech patients with suspected congenital skeletal abnormalities.

机构信息

Institute of Medical Genetics, Olomouc University Hospital, Olomouc, Czech Republic; Institute of Medical Genetics, Palacký University in Olomouc, Olomouc, Czech Republic.

Institute of Medical Genetics, Olomouc University Hospital, Olomouc, Czech Republic; Institute of Medical Genetics, Palacký University in Olomouc, Olomouc, Czech Republic.

出版信息

Gene. 2024 Jan 20;892:147881. doi: 10.1016/j.gene.2023.147881. Epub 2023 Oct 6.

DOI:10.1016/j.gene.2023.147881
PMID:37806643
Abstract

BACKGROUND

Congenital skeletal abnormalities are a heterogeneous group of diseases most commonly associated with small or disproportionate growth, cranial and facial dysmorphisms, delayed bone maturation, etc. Nonetheless, no detailed genotype-phenotype correlation in patients with specific genetic variants is readily available. Ergo, this study focuses on the analysis of patient phenotypes with candidate variants in genes involved in bone growth as detected by molecular genetic analysis.

METHODS

In this study we used molecular genetic methods to analyse the ACAN, COL2A1, FGFR3, IGFALS, IGF1, IGF1R, GHR, NPR2, STAT5B and SHOX genes in 128 Czech children with suspected congenital skeletal abnormalities. Pathogenic variants and variants of unclear clinical significance were identified and we compared their frequency in this study cohort to the European non-Finnish population. Furthermore, a prediction tool was utilised to determine their possible impact on the final protein. All clinical patient data was obtained during pre-test genetic counselling.

RESULTS

Pathogenic variants were identified in the FGFR3, GHR, COL2A1 and SHOX genes in a total of six patients. Furthermore, we identified 23 variants with unclear clinical significance and high allelic frequency in this cohort of patients with skeletal abnormalities. Five of them have not yet been reported in the scientific literature.

CONCLUSION

Congenital skeletal abnormalities may lead to a number of musculoskeletal, neurological, cardiovascular problems. Knowledge of specific pathogenic variants may help us in therapeutic procedures.

摘要

背景

先天性骨骼异常是一组异质性疾病,最常见的表现为生长迟缓或不成比例、颅面畸形、骨成熟延迟等。然而,特定遗传变异患者的详细基因型-表型相关性尚未明确。因此,本研究专注于分析通过分子遗传学分析检测到的涉及骨骼生长的候选基因中的患者表型与变异。

方法

在这项研究中,我们使用分子遗传学方法分析了 128 名捷克疑似先天性骨骼异常儿童的 ACAN、COL2A1、FGFR3、IGFALS、IGF1、IGF1R、GHR、NPR2、STAT5B 和 SHOX 基因。鉴定了致病性变异和临床意义不明的变异,并将其在本研究队列中的频率与欧洲非芬兰人群进行了比较。此外,还使用预测工具来确定它们对最终蛋白质的可能影响。所有临床患者数据均在预测试遗传咨询期间获得。

结果

共在 6 名患者的 FGFR3、GHR、COL2A1 和 SHOX 基因中发现了致病性变异。此外,我们在该骨骼异常患者队列中还发现了 23 个具有临床意义不明和高等位基因频率的变异。其中 5 个变异尚未在科学文献中报道。

结论

先天性骨骼异常可能导致许多肌肉骨骼、神经、心血管问题。了解特定的致病性变异可能有助于我们进行治疗。

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Clinical-genetic analysis of selected genes involved in the development of the human skeleton in 128 Czech patients with suspected congenital skeletal abnormalities.128 例疑似先天性骨骼畸形的捷克患者中参与人类骨骼发育的选定基因的临床遗传学分析。
Gene. 2024 Jan 20;892:147881. doi: 10.1016/j.gene.2023.147881. Epub 2023 Oct 6.
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