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东南亚患者先天性疾病的遗传特征:基于孟德尔表型的基因panel 测序结果。

Genetic landscape of congenital disorders in patients from Southeast Asia: results from sequencing using a gene panel for Mendelian phenotypes.

机构信息

KK Research Centre, KK Women's & Children's Hospital, Singapore.

Paediatric Academic Clinical Programme, SingHealth Duke-NUS Graduate Medical School, Singapore.

出版信息

Arch Dis Child. 2021 Jan;106(1):38-43. doi: 10.1136/archdischild-2020-319177. Epub 2020 Sep 25.

Abstract

OBJECTIVE

To test the utility and diagnostic yield of a medical-exome gene panel for identifying pathogenic variants in Mendelian disorders.

METHODS

Next-generation sequencing was performed with the TruSight One gene panel (targeting 4813 genes) followed by MiSeq sequencing on 216 patients who presented with suspected genetic disorders as assessed by their attending physicians.

RESULTS

There were 56 pathogenic and 36 likely pathogenic variants across 57 genes identified in 87 patients. Causal mutations were more likely to be truncating and from patients with a prior clinical diagnosis. Another 18 promising variants need further evaluation for more evidence to meet the requirement for potential upgrade to pathogenic. Forty-five of the 92 clinically significant variants were novel.

CONCLUSION

The 40.3% positive yield compares favourably with similar studies using either this panel or whole exome sequencing, demonstrating that large gene panels could be a good alternative to whole exome sequencing for quick genetic confirmation of Mendelian disorders.

摘要

目的

测试用于鉴定孟德尔疾病中致病性变异的外显子组基因panel 的实用性和诊断效果。

方法

对 216 名疑似遗传疾病的患者进行了下一代测序,使用 TruSight One 基因 panel(靶向 4813 个基因),然后在 MiSeq 上进行测序,这些患者是由他们的主治医生评估的。

结果

在 87 名患者中,共发现了 57 个基因的 56 个致病性和 36 个可能致病性变异。因果突变更可能是截断性的,而且来自于有先前临床诊断的患者。另外 18 个有前途的变异需要进一步评估,以获得更多证据,使其有可能升级为致病性。92 个具有临床意义的变异中有 45 个是新的。

结论

阳性检出率为 40.3%,与使用该 panel 或全外显子测序的类似研究相比,结果相当好,表明大的基因 panel 可能是孟德尔疾病快速遗传确认的全外显子测序的一个很好的替代方案。

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