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Exonization of a deep intronic long interspersed nuclear element in Becker muscular dystrophy.


ABSTRACT: The precise identification of pathogenic DMD variants is sometimes rather difficult, mainly due to complex structural variants (SVs) and deep intronic splice-altering variants. We performed genomic long-read whole DMD gene sequencing in a boy with asymptomatic hyper-creatine kinase-emia who remained genetically undiagnosed after standard genetic testing, dystrophin protein and DMD mRNA studies, and genomic short-read whole DMD gene sequencing. We successfully identified a novel pathogenic SV in DMD intron 1 via long-read sequencing. The deep intronic SV consists of a long interspersed nuclear element-1 (LINE-1) insertion/non-tandem duplication rearrangement causing partial exonization of the LINE-1, establishing a genetic diagnosis of Becker muscular dystrophy. Our study expands the genetic spectrum of dystrophinopathies and highlights the significant role of disease-causing LINE-1 insertions in monogenic diseases.

SUBMITTER: Xie Z 

PROVIDER: S-EPMC9453646 | biostudies-literature | 2022

REPOSITORIES: biostudies-literature

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Exonization of a deep intronic long interspersed nuclear element in Becker muscular dystrophy.

Xie Zhiying Z   Liu Chang C   Lu Yanyu Y   Sun Chengyue C   Liu Yilin Y   Yu Meng M   Shu Junlong J   Meng Lingchao L   Deng Jianwen J   Zhang Wei W   Wang Zhaoxia Z   Lv He H   Yuan Yun Y  

Frontiers in genetics 20220825


The precise identification of pathogenic <i>DMD</i> variants is sometimes rather difficult, mainly due to complex structural variants (SVs) and deep intronic splice-altering variants. We performed genomic long-read whole <i>DMD</i> gene sequencing in a boy with asymptomatic hyper-creatine kinase-emia who remained genetically undiagnosed after standard genetic testing, dystrophin protein and <i>DMD</i> mRNA studies, and genomic short-read whole <i>DMD</i> gene sequencing. We successfully identifi  ...[more]

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