Artem Borovikov, Nailya Galeeva, Andrey Marakhonov, Aysylu Murtazina, Varvara Kadnikova, Kseniya Davydenko, Anna Orlova, Peter Sparber, Tatiana Markova, Maria Orlova, Darya Osipova, Tatyana Nagornova, Natalia Semenova, Olga Levchenko, Alexandra Filatova, Margarita Sharova, Peter Vasiluev, Ilya Kanivets, Denis Pyankov, Artem Sharkov, Vasilisa Udalova, Vladimir Kenis, Natalia Nikitina, Maria Sumina, Konstantin Zherdev, Aleksandr Petel′guzov, Oleg Chelpachenko, Pavel Zubkov, Ivan Dan, Andrey Snetkov, Alexandra Akinshina, Yury Buklemishev, Oxana Ryzhkova, Vyacheslav Tabakov, Ekaterina Zakharova, Sergey Korostelev, Rena Zinchenko, Mikhail Skoblov, Alexander Polyakov, Elena Dadali, Sergey Kutsev, Olga Shchagina
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引用次数: 0
Abstract
This study is aimed at investigating the clinical and genetic characteristics of 244 unrelated probands diagnosed with multiple osteochondromas (MO). The diagnosis of MO typically involves identifying multiple benign bone tumors known as osteochondromas (OCs) through imaging studies and physical examinations. However, cases with both OCs and enchondromas (ECs) may indicate the more rare condition metachondromatosis (MC), which is assumed to be distinct disease. Previous cohort studies of MO found heterozygous loss-of-function (LoF) variants only in the EXT1 or EXT2 genes, with DNA diagnostic yield ranging from 78 to 95%. The PTPN11 gene, which is causative for MC, was not previously investigated as a gene candidate for MO. In this study, we detected a total of 177 unique single nucleotide and copy number variants in three genes across 220 probands, consisting of 80 previously reported and 97 novel variants. Specifically, we identified five cases with OCs and no ECs as well as four cases with MC carrying LoF variants in the PTPN11 gene and two additional cases with ECs harboring variants in the EXT1/2 genes. These findings suggest a potential overlap between the MO and MC both phenotypically and genetically. These findings highlight the importance of expanding genetic testing beyond the EXT1 and EXT2 genes in MO cases, as other genes such as PTPN11 may also be causative. This can improve the accuracy of diagnosis and treatment for individuals with MO and MC. It is essential to determine whether MO and MC represent distinct diseases or if they encompass a broader clinical spectrum.
本研究旨在调查 244 名被诊断患有多发性骨软骨瘤(MO)的非亲属关系探亲者的临床和遗传特征。多发性骨软骨瘤(MO)的诊断通常需要通过影像学检查和体格检查来确定多发性良性骨肿瘤,即骨软骨瘤(OC)。然而,同时伴有骨软骨瘤(OC)和软骨瘤(EC)的病例可能预示着更罕见的变态软骨瘤病(MC),而变态软骨瘤病被认为是一种不同的疾病。以往对 MO 的队列研究仅在 EXT1 或 EXT2 基因中发现了杂合功能缺失(LoF)变异,DNA 诊断率为 78% 至 95%。PTPN11基因是MC的致病基因,但此前并未将其作为MO的候选基因进行研究。在这项研究中,我们在220名受试者的三个基因中检测到了177个独特的单核苷酸和拷贝数变异,其中包括80个以前报道过的变异和97个新变异。具体来说,我们发现了五例有OC而无EC的病例,以及四例携带PTPN11基因LoF变异的MC病例和另外两例携带EXT1/2基因变异的EC病例。这些发现表明,MO 和 MC 在表型和基因上都可能存在重叠。这些发现强调了在 MO 病例中扩大 EXT1 和 EXT2 基因以外的基因检测的重要性,因为 PTPN11 等其他基因也可能是致病因素。这可以提高 MO 和 MC 患者诊断和治疗的准确性。必须确定 MO 和 MC 是否代表不同的疾病,或者它们是否包含更广泛的临床范围。
期刊介绍:
Human Mutation is a peer-reviewed journal that offers publication of original Research Articles, Methods, Mutation Updates, Reviews, Database Articles, Rapid Communications, and Letters on broad aspects of mutation research in humans. Reports of novel DNA variations and their phenotypic consequences, reports of SNPs demonstrated as valuable for genomic analysis, descriptions of new molecular detection methods, and novel approaches to clinical diagnosis are welcomed. Novel reports of gene organization at the genomic level, reported in the context of mutation investigation, may be considered. The journal provides a unique forum for the exchange of ideas, methods, and applications of interest to molecular, human, and medical geneticists in academic, industrial, and clinical research settings worldwide.