Abstract
BackgroundHigh myopia with alopecia areata in the occipital region has been observed in patients with Knobloch syndrome caused by COL18A1 mutations. This study investigated other possible genetic causes of high myopia in patients with alopecia areata in the cranial midline.MethodsSix patients with early onset high myopia and alopecia areata in the cranial midline were recruited. Targeted high-throughput sequencing was performed on the proband’s DNA to detect potential pathogenic variants. Cosegregation analysis was performed for available family members. Minigene assay and RNA Sequencing were used to validate the abnormality of possible splicing change and gross deletion. Ophthalmological and neuroimaging examinations were performed.ResultsEight novel and one known loss-of-function mutants were detected in all six patients, including a gross deletion detected by RNA sequencing. Four COL18A1 mutants in three patients with scalp leisure in the occipital region; and five LAMA1 mutations in three patients with scalp leisure in the parietal region. Further assessments indicated that patients with COL18A1 mutations had Knobloch syndrome, and the patients with LAMA1 mutations had Poretti–Boltshauser syndrome.ConclusionOur study found that early onset high myopia with midline alopecia areata could be caused not only by mutations of the COL18A1 gene but also by mutations in the LAMA1 gene. To our knowledge, we are the first to observe scalp defects in patients with LAMA1 mutations. High myopia with alopecia areata in the cranial midline could be treated as an early diagnostic clue for ophthalmologists to consider the two kinds of rare diseases.
Highlights
Myopia, high myopia, could occur independently or as a feature in hundreds of ocular and systemic syndromes
Alert for Syndromic Myopia involved in these syndromes in addition to myopia; when affected, it can present with typical signs such as intellectual disability, microcephaly, cerebellar hypoplasia, special facial features, and hearing loss
Because high myopia might be an early feature in these syndromes or due to unawareness of the atypical manifestations of other signs, it is challenging for ophthalmologists to recognize these myopic syndromes, especially in children under 10 years of age
Summary
High myopia, could occur independently or as a feature in hundreds of ocular and systemic syndromes. Alert for Syndromic Myopia involved in these syndromes in addition to myopia; when affected, it can present with typical signs such as intellectual disability, microcephaly, cerebellar hypoplasia, special facial features, and hearing loss. Because high myopia might be an early feature in these syndromes or due to unawareness of the atypical manifestations of other signs, it is challenging for ophthalmologists to recognize these myopic syndromes, especially in children under 10 years of age. It would be helpful if certain signs could be obtained by physical examination to help doctors consider myopic syndromes with nervous system involvement, as is possible with Marfan syndrome. This study investigated other possible genetic causes of high myopia in patients with alopecia areata in the cranial midline
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