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.
Long-read sequencing (LRS) identified skewed X-inactivation patterns and complex structural variants in the IKBKG gene in three families with incontinentia pigmenti that previously received negative clinical testing, demonstrating LRS’s utility for diagnosing disorders involving challenging genomic regions.