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TERC and TERT gene mutations in patients with bone marrow failure and the significance of telomere length measurements

机译:骨髓衰竭患者的TERC和TERT基因突变及端粒长度测量的意义

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摘要

Dyskeratosis congenita (DC) is a rare inherited form of bone marrow failure (BMF) caused by mutations in telomere maintaining genes including TERC and TERT. Here we studied the prevalence of TERC and TERT gene mutations and of telomere shortening in an unselected population of patients with BMF at our medical center and in a selected group of patients referred from outside institutions. Less than 5% of patients with BMF had pathogenic mutations in TERC or TERT. In patients with BMF, pathogenic TERC or TERT gene mutations were invariably associated with marked telomere shortening (≪ 1st percentile) in peripheral blood mononuclear cells (PBMCs). In asymptomatic family members, however, telomere length was not a reliable predictor for the presence or absence of a TERC or TERT gene mutation. Telomere shortening was not pathognomonic of DC, as approximately 30% of patients with BMF due to other causes had PBMC telomere lengths at the 1st percentile or lower. We conclude that in the setting of BMF, measurement of telomere length is a sensitive but nonspecific screening method for DC. In the absence of BMF, telomere length measurements should be interpreted with caution.
机译:先天性角化病(DC)是一种罕见的遗传性骨髓衰竭(BMF),由端粒维持基因(包括TERC和TERT)的突变引起。在这里,我们研究了未选择的BMF患者群体在我们医疗中心以及从外部机构转诊的一组特定患者中TERC和TERT基因突变的发生率以及端粒缩短的情况。不到5%的BMF患者在TERC或TERT中具有致病性突变。在患有BMF的患者中,致病性TERC或TERT基因突变总是与外周血单核细胞(PBMC)的端粒明显缩短(约1%百分位数)相关。然而,在无症状家庭成员中,端粒长度不是TERC或TERT基因突变存在与否的可靠预测指标。端粒缩短不是DC的病因,因为大约30%的BMF患者由于其他原因而导致PBMC端粒长度处于1%或更低。我们得出结论,在BMF的设置中,端粒长度的测量是DC的一种敏感但非特异性的筛选方法。在没有BMF的情况下,端粒长度的测量应谨慎解释。

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