Boyden Lynn M, Vincent Nicholas G, Zhou Jing, Hu Ronghua, Craiglow Brittany G, Bayliss Susan J, Rosman Ilana S, Lucky Anne W, Diaz Luis A, Goldsmith Lowell A, Paller Amy S, Lifton Richard P, Baserga Susan J, Choate Keith A
Department of Genetics, Yale University School of Medicine, New Haven, CT 06510, USA.
Department of Microbiology, Yale University School of Medicine, New Haven, CT 06510, USA.
Am J Hum Genet. 2017 Jun 1;100(6):978-984. doi: 10.1016/j.ajhg.2017.05.003.
The discovery of new genetic determinants of inherited skin disorders has been instrumental to the understanding of epidermal function, differentiation, and renewal. Here, we show that mutations in KDSR (3-ketodihydrosphingosine reductase), encoding an enzyme in the ceramide synthesis pathway, lead to a previously undescribed recessive Mendelian disorder in the progressive symmetric erythrokeratoderma spectrum. This disorder is characterized by severe lesions of thick scaly skin on the face and genitals and thickened, red, and scaly skin on the hands and feet. Although exome sequencing revealed several of the KDSR mutations, we employed genome sequencing to discover a pathogenic 346 kb inversion in multiple probands, and cDNA sequencing and a splicing assay established that two mutations, including a recurrent silent third base change, cause exon skipping. Immunohistochemistry and yeast complementation studies demonstrated that the mutations cause defects in KDSR function. Systemic isotretinoin therapy has achieved nearly complete resolution in the two probands in whom it has been applied, consistent with the effects of retinoic acid on alternative pathways for ceramide generation.
遗传性皮肤病新遗传决定因素的发现有助于理解表皮功能、分化和更新。在此,我们表明,编码神经酰胺合成途径中一种酶的KDSR(3-酮二氢鞘氨醇还原酶)突变会导致进行性对称性红斑角化病谱系中一种先前未描述的隐性孟德尔疾病。这种疾病的特征是面部和生殖器出现严重的厚鳞屑性皮肤病变,以及手脚皮肤增厚、发红和脱屑。虽然外显子组测序揭示了几个KDSR突变,但我们采用基因组测序在多个先证者中发现了一个致病性的346 kb倒位,并且cDNA测序和剪接分析确定了两个突变,包括一个反复出现的沉默第三位碱基变化,导致外显子跳跃。免疫组织化学和酵母互补研究表明,这些突变导致KDSR功能缺陷。全身性异维甲酸治疗已在应用该治疗的两名先证者中实现了几乎完全缓解,这与视黄酸对神经酰胺生成替代途径的作用一致。
