Gálvez Eva, Vallespín Elena, Arias-Salgado Elena G, Sánchez-Valdepeñas Carmen, Giménez Yari, Navarro Susana, Río Paula, Bogliolo Massimo, Pujol Roser, Peiró Montserrat, Nevado Julián, Zubicaray Josune, Sebastián Elena, Catalá Albert, Beléndez Cristina, Díaz de Heredia Cristina, Galera Ana, Badell Isabel, Madero Luis, Perona Rosario, Sastre Leandro, Surrallés Jordi, Bueren Juan, Lapunzina Pablo, Sevilla Julián
Servicio de Hematología y Oncología Pediátrica, Fundación de Investigación Biomédica, Hospital Infantil Universitario Niño Jesús, Madrid, Spain.
Centro de Investigación Biomédica en Red de Enfermedades Raras (CIBERER), ISCIII, Madrid, Spain.
Hemasphere. 2021 Mar 9;5(4):e539. doi: 10.1097/HS9.0000000000000539. eCollection 2021 Apr.
Inherited bone marrow failure syndromes (IBMFSs) are a group of congenital rare diseases characterized by bone marrow failure, congenital anomalies, high genetic heterogeneity, and predisposition to cancer. Appropriate treatment and cancer surveillance ideally depend on the identification of the mutated gene. A next-generation sequencing (NGS) panel of genes could be 1 initial genetic screening test to be carried out in a comprehensive study of IBMFSs, allowing molecular detection in affected patients. We designed 2 NGS panels of IBMFS genes: version 1 included 129 genes and version 2 involved 145 genes. The cohort included a total of 204 patients with suspected IBMFSs without molecular diagnosis. Capture-based targeted sequencing covered > 99% of the target regions of 145 genes, with more than 20 independent reads. No differences were seen between the 2 versions of the panel. The NGS tool allowed a total of 91 patients to be diagnosed, with an overall molecular diagnostic rate of 44%. Among the 167 patients with classified IBMFSs, 81 patients (48%) were diagnosed. Unclassified IBMFSs involved a total of 37 patients, of whom 9 patients (24%) were diagnosed. The preexisting diagnosis of 6 clinically classified patients (6%) was amended, implying a change of therapy for some of them. Our NGS IBMFS gene panel assay is a useful tool in the molecular diagnosis of IBMFSs and a reasonable option as the first tier genetic test in these disorders.
遗传性骨髓衰竭综合征(IBMFSs)是一组先天性罕见疾病,其特征为骨髓衰竭、先天性异常、高度遗传异质性以及易患癌症。理想情况下,恰当的治疗和癌症监测取决于突变基因的识别。基因二代测序(NGS) panel 可作为对IBMFSs进行全面研究时首先开展的一项初始基因筛查检测,从而在受影响的患者中进行分子检测。我们设计了两个IBMFS基因的NGS panel:版本1包含129个基因,版本2涉及145个基因。该队列总共纳入了204例疑似IBMFSs但未进行分子诊断的患者。基于捕获的靶向测序覆盖了145个基因目标区域的> 99%,有超过20条独立读数。两个版本的panel之间未观察到差异。NGS工具总共诊断出91例患者,总体分子诊断率为44%。在167例已分类的IBMFSs患者中,81例(48%)被诊断出来。未分类的IBMFSs共有37例患者,其中9例(24%)被诊断出来。6例临床分类患者(6%)之前的诊断被修正,这意味着他们中的一些人治疗方案发生了改变。我们的NGS IBMFS基因panel检测是IBMFSs分子诊断中的一种有用工具,也是这些疾病一级基因检测的合理选择。 (注:原文中“NGS panel of genes”表述不太准确,可能“NGS panel”更合适,这里按原文翻译了。)
