Errichiello Edoardo, Vetro Annalisa, Mina Tommaso, Wischmeijer Anita, Berrino Enrico, Carella Miriam, Romagnoli Maria, Sacchini Patrizia, Venesio Tiziana, Zecca Marco, Zuffardi Orsetta
Department of Molecular Medicine, University of Pavia, Pavia, Italy.
Department of Molecular Medicine, University of Pavia, Pavia, Italy.
Blood Cells Mol Dis. 2017 May;64:38-44. doi: 10.1016/j.bcmd.2017.03.002. Epub 2017 Mar 6.
Diamond-Blackfan anemia (DBA) is a rare congenital disorder presenting remarkable phenotypic overlap with other inherited bone marrow failure syndromes, making differential diagnosis challenging and its confirmation often reached with great delay. By whole exome sequencing, we unraveled the presence of pathogenic variants affecting genes already known to be involved in DBA pathogenesis (RPL5 and RPS19) in three patients with otherwise uncertain clinical diagnosis, and provided new insights on DBA genotype-phenotype correlations. Remarkably, the RPL5 c.482del frameshift mutation has never been reported before, whereas the RPS19 c.3G>T missense mutation, although previously described in a 2-month-old DBA patient without malformations and refractory to steroid therapy, was detected here in the mosaic state in different bodily tissues for the first time in DBA patients.
钻石黑范贫血(DBA)是一种罕见的先天性疾病,其临床表现与其他遗传性骨髓衰竭综合征有显著重叠,这使得鉴别诊断具有挑战性,且往往会延迟很久才能确诊。通过全外显子组测序,我们在三名临床诊断不明确的患者中发现了影响已知参与DBA发病机制的基因(RPL5和RPS19)的致病变异,并为DBA基因型-表型相关性提供了新的见解。值得注意的是,RPL5基因c.482del移码突变此前从未被报道过,而RPS19基因c.3G>T错义突变虽然此前在一名2个月大、无畸形且对类固醇治疗无效的DBA患者中被描述过,但在此处首次在DBA患者的不同身体组织中以嵌合状态被检测到。
