Diagnosis of a mild peroxisomal phenotype with next-generation sequencing

Meredith J. Ventura; Dianna Wheaton; Mingchu Xu; David Birch; Sara J. Bowne; Lori S. Sullivan; Stephen P. Daiger; Annette E. Whitney; Richard O. Jones; Ann B. Moser; Rui Chen; Michael F. Wangler

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Diagnosis of a mild peroxisomal phenotype with next-generation sequencing

机译：下一代测序诊断轻度过氧化物酶体表型

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Peroxisomal biogenesis disorders (PBD) are caused by mutations in PEX genes, and are typically diagnosed with biochemical testing in plasma followed by confirmatory testing. Here we report the unusual diagnostic path of a child homozygous for PEX1 p.G843D. The patient presented with sensorineural hearing loss, pigmentary retinopathy, and normal intellect. After testing for Usher syndrome was negative, he was found to have PBD through a research sequencing panel. When evaluating a patient with hearing loss and pigmentary retinopathy, mild PBD should be on the differential regardless of cognitive function.

机译：过氧化物酶体生物发生障碍（PBD）是由PEX基因突变引起的，通常通过血浆中的生化检测和确证性检测来诊断。在这里，我们报告了PEX1 p.G843D纯合子的异常诊断路径。该患者表现为感觉神经性听力减退，色素性视网膜病变和智力正常。在测试Usher综合征为阴性后，通过研究测序小组发现他患有PBD。在评估患有听力损失和色素性视网膜病变的患者时，无论认知功能如何，轻度PBD都应有所区别。

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《Molecular Genetics and Metabolism Reports》 |2016年第2期|共4页
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Meredith J. Ventura; Dianna Wheaton; Mingchu Xu; David Birch; Sara J. Bowne; Lori S. Sullivan; Stephen P. Daiger; Annette E. Whitney; Richard O. Jones; Ann B. Moser; Rui Chen; Michael F. Wangler;
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Diagnosis of a mild peroxisomal phenotype with next-generation sequencing

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