Department of Oncology and Sidney Kimmel Comprehensive Cancer Center, Johns Hopkins University School of Medicine, Baltimore, Maryland.
Hum Mutat. 2013 Nov;34(11):1481-5. doi: 10.1002/humu.22397. Epub 2013 Sep 11.
Dyskeratosis congenita (DC) is a telomere-mediated syndrome defined by mucocutaneous features. The X-linked mode of inheritance accounts for half the cases, and is thought to predominantly manifest in childhood as bone marrow failure. We identified two male probands who presented in the fifth decade with idiopathic pulmonary fibrosis and cancer. Their pedigrees displayed consecutively affected generations. Five of six females (83%) manifested mucocutaneous features of DC, and two had wound-healing complications. No mutations in autosomal dominant telomere genes were present, but exome sequencing revealed novel variants in the X-chromosome DKC1 gene that predicted missense mutations in conserved residues, p.Thr49Ser and p.Pro409Arg. Variants segregated with the telomere phenotype, and affected females were heterozygotes, showing skewed X-inactivation. Telomerase RNA levels were compromised in cells from DKC1 mutation carriers, consistent with their pathogenic role. These findings indicate that females with heterozygous DKC1 mutations may be at increased risk for developing penetrant telomere phenotypes that, at times, may be associated with clinical morbidity.
先天性角化不良症(DC)是一种由端粒介导的综合征,其特征为黏膜皮肤表现。半数病例呈 X 连锁遗传模式,主要在儿童期表现为骨髓衰竭。我们发现了两名男性先证者,他们在 50 多岁时出现特发性肺纤维化和癌症。他们的家族史显示连续受累的几代人。6 名女性中有 5 名(83%)表现出 DC 的黏膜皮肤特征,其中 2 名有伤口愈合并发症。不存在常染色体显性端粒基因的突变,但外显子组测序显示 X 染色体 DKC1 基因存在新的变异,预测保守残基发生错义突变,即 p.Thr49Ser 和 p.Pro409Arg。变异与端粒表型共分离,受影响的女性为杂合子,表现出 X 染色体失活偏倚。来自 DKC1 突变携带者的细胞中端粒酶 RNA 水平受损,这与其致病作用一致。这些发现表明,携带杂合性 DKC1 突变的女性可能面临更高的风险,出现外显的端粒表型,有时可能与临床发病相关。
