Department of Clinical Genetics, Human Genetics and Genome Research Institute, National Research Centre, Cairo, Egypt.
Department of Pediatrics, Faculty of Medicine, Kuwait University, Safat, Kuwait.
Clin Genet. 2023 Sep;104(3):344-349. doi: 10.1111/cge.14348. Epub 2023 May 9.
Pathogenic biallelic variants in LSS are associated with three Mendelian rare disease traits including congenital cataract type 44, autosomal recessive hypotrichosis type 14, and alopecia-intellectual disability syndrome type 4 (APMR4). We performed trio research exome sequencing on a family with a four-year-old male with global developmental delay, epilepsy and striking alopecia, and identified novel compound heterozygous LSS splice site (c.14+2T>C) and missense (c.1357 G>A; p.V453L) variant alleles. Rare features associated with APMR4 such as cryptorchidism, micropenis, mild cortical brain atrophy and thin corpus callosum were detected. Previously unreported APMR4 findings including cerebellar involvement in the form of unsteady ataxic gait, small vermis with prominent folia, were noted. A review of all reported variants to date in 29 families with LSS-related phenotypes showed an emerging genotype-phenotype correlation. Our report potentially expands LSS-related phenotypic spectrum and highlights the importance of performing brain imaging in LSS-related conditions.
致病的 LSS 双等位基因变异与三种孟德尔罕见疾病特征有关,包括先天性白内障 44 型、常染色体隐性毛发稀疏症 14 型和脱发-智力障碍综合征 4 型(APMR4)。我们对一个有一名四岁男性的家庭进行了三联体研究外显子组测序,该男性患有全面发育迟缓、癫痫和明显脱发,发现了新的 LSS 剪接位点(c.14+2T>C)和错义(c.1357 G>A;p.V453L)复合杂合变异等位基因。检测到与 APMR4 相关的罕见特征,如隐睾、小阴茎、轻度皮质脑萎缩和薄胼胝体。还注意到以前未报道的 APMR4 发现,包括小脑受累的形式为不稳定共济失调步态、小的蚓部和明显的叶片。对迄今为止在 29 个具有 LSS 相关表型的家庭中报告的所有变异进行的综述显示出一种新兴的基因型-表型相关性。我们的报告可能扩展了 LSS 相关表型谱,并强调了在 LSS 相关疾病中进行脑部成像的重要性。
