Long-read sequencing is required for precision diagnosis of incontinentia pigmenti.

IF 3.6 Q2 GENETICS & HEREDITY

HGG Advances Pub Date : 2025-07-10 Epub Date: 2025-06-12 DOI:10.1016/j.xhgg.2025.100468

Monica H Wojcik, Robin D Clark, Abdallah F Elias, Casie A Genetti, Jill A Madden, Dana Simpson, Linda Golkar, Miranda P G Zalusky, Angela L Miller, Araceli Rodriguez, Joy Goffena, Camille A Dash, Nikhita Damaraju, Sophia B Gibson, Sophie H R Storz, Zachary B Anderson, Jonas A Gustafson, Isabelle Thiffault, Emily G Farrow, Tomi Pastinen, Jasmine Lin, Jennifer T Huang, Alan H Beggs, Pankaj B Agrawal, David T Miller, Danny E Miller

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Abstract

Incontinentia pigmenti (IP) is caused by loss-of-function variants in IKBKG, with molecular genetic diagnosis complicated by a pseudogene. We describe seven individuals from three families with IP but negative clinical genetic testing in whom long-read sequencing identified causal variants, including one family with the common exon 4-10 deletion not identified by conventional clinical genetic testing. Concurrent methylation analysis explained disease severity in one individual who died from neurologic complications, identified a mosaic variant in an individual with an atypical presentation, and confirmed skewed X chromosome inactivation in an XXY individual.

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长读测序是精确诊断色素失禁所必需的。

色素失禁（IP）是由IKBKG的功能丧失变异引起的，分子遗传学诊断伴有假基因。我们描述了来自三个IP家族但临床基因检测阴性的7个人，其中长读测序发现了因果变异，包括一个具有常规临床基因检测未发现的常见外显子4-10缺失的家族。同步甲基化分析解释了一名死于神经系统并发症的个体的疾病严重程度，在一名非典型表现的个体中发现了一种马赛克变异，并在一名XXY个体中证实了扭曲的x染色体失活。

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