首页> 外文期刊>The American Journal of Human Genetics >TINF2, a component of the shelterin telomere protection complex, is mutated in dyskeratosis congenita.
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TINF2, a component of the shelterin telomere protection complex, is mutated in dyskeratosis congenita.

机译:TINF2是庇护蛋白端粒保护复合物的一个组成部分,在先天性角化不全中发生突变。

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摘要

Patients with dyskeratosis congenita (DC), a heterogeneous inherited bone marrow failure syndrome, have abnormalities in telomere biology, including very short telomeres and germline mutations in DKC1, TERC, TERT, or NOP10, but approximately 60% of DC patients lack an identifiable mutation. With the very short telomere phenotype and a highly penetrant, rare disease model, a linkage scan was performed on a family with autosomal-dominant DC and no mutations in DKCI, TERC, or TERT. Evidence favoring linkage was found at 2p24 and 14q11.2, and this led to the identification of TINF2 (14q11.2) mutations, K280E, in the proband and her five affected relatives and TINF2 R282H in three additional unrelated DC probands, including one with Revesz syndrome; a fifth DC proband had a R282S mutation. TINF2 mutations were not present in unaffected relatives, DC probands with mutations in DKC1, TERC, or TERT or 298 control subjects. We demonstrate that a fifth gene, TINF2, is mutated in classical DC and, for the first time, in Revesz syndrome. This represents the first shelterin complex mutation linked to human disease and confirms the role of very short telomeres as a diagnostic test for DC.
机译:先天性角化异常(DC)患者是异质性遗传性骨髓衰竭综合征,其端粒生物学异常,包括端粒和DKC1,TERC,TERT或NOP10的种系突变非常短,但约60%的DC患者缺乏可识别的突变。对于端粒非常短的表型和高度渗透的稀有疾病模型,对具有常染色体显性DC且DKCI,TERC或TERT无突变的家庭进行了连锁扫描。在2p24和14q11.2发现了有利于连锁的证据,这导致在先证者及其五个受影响亲戚中发现了TINF2(14q11.2)突变K280E,并在另外三个不相关的DC先证者中发现了TINF2 R282H,包括一个雷夫兹综合征第五名DC先证者具有R282S突变。在未受影响的亲戚,DKC1,TERC或TERT或298名对照受试者中具有突变的DC先证者中不存在TINF2突变。我们证明了第五个基因TINF2在经典DC中发生了突变,并且首次出现在Revesz综合征中。这代表了与人类疾病相关的第一个庇护蛋白复合突变,并证实了非常短的端粒作为DC诊断测试的作用。

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