Department of Clinical Genetics, University and Regional Laboratories, Skåne University Hospital, Lund University, Lund, Sweden.
Eur J Haematol. 2012 Feb;88(2):136-43. doi: 10.1111/j.1600-0609.2011.01710.x. Epub 2011 Nov 17.
Acquired trisomy 21 is one of the most common numerical abnormalities in acute myeloid leukemia (AML), myelodysplastic syndrome (MDS), myeloproliferative neoplasms (MPN), and MDS/MPN; however, little is known about its pathogenic impact, accompanying submicroscopic changes, and its relation to other clinical features. Furthermore, previous studies addressing this issue have mainly focused on cases in which +21 was part of a complex karyotype.
We ascertained the incidence of +21, both as a sole change (T21s) and irrespective of additional changes (T21all), in relation to disease type, morphologic subgroup, gender, and age in all published AML, MDS, MPN, and MDS/MPN cases. Furthermore, single nucleotide polymorphism (SNP) array analysis was performed on 11 myeloid malignancies with T21s, followed by mutation analysis of the FGFR1, FLT3, GATA1, JAK2, KIT, NPM1, NRAS, RUNX1, and TET2 genes.
The frequencies of T21s and/or T21all varied significantly among the AML, MDS, MPN, and MDS/MPN cases, among the AML and MPN subtypes, and in relation to the age of the AML, MDS, and MPN patients. In the 11 cases analyzed by SNP array, a total of nine genomic imbalances, comprising seven deletions and two duplications, were identified in six cases; none of the alterations were recurrent. Partial uniparental disomies (UPDs) were found in five cases; two recurrent UPDs were identified, namely UPD4q and UPD7q. Mutations in NPM1, RUNX1, and TET2 were detected in five cases, three of which harbored a pathogenic RUNX1 mutation. The TET2 mutation was found in one of the cases with UPD4q.
The results show that trisomy 21-positive myeloid malignancies are clinically highly variable and that they display a heterogeneous pattern of copy number alterations and mutations.
获得性 21 三体是急性髓系白血病(AML)、骨髓增生异常综合征(MDS)、骨髓增殖性肿瘤(MPN)和 MDS/MPN 中最常见的数量异常之一;然而,其致病影响、伴随的亚微观变化及其与其他临床特征的关系知之甚少。此外,以前研究这个问题的主要集中在+21 是复杂核型一部分的情况下。
我们确定了+21 的发生率,包括作为单一变化(T21s)和不考虑其他变化(T21all),与疾病类型、形态亚组、性别和年龄在所有已发表的 AML、MDS、MPN 和 MDS/MPN 病例中的关系。此外,对 11 例 T21s 的髓系恶性肿瘤进行了单核苷酸多态性(SNP)阵列分析,随后对 FGFR1、FLT3、GATA1、JAK2、KIT、NPM1、NRAS、RUNX1 和 TET2 基因进行了突变分析。
T21s 和/或 T21all 的频率在 AML、MDS、MPN 和 MDS/MPN 病例之间、AML 和 MPN 亚型之间以及 AML、MDS 和 MPN 患者的年龄之间存在显著差异。在通过 SNP 阵列分析的 11 例病例中,在 6 例中总共鉴定出 9 种基因组不平衡,包括 7 种缺失和 2 种重复;没有发现反复出现的改变。在 5 例中发现部分单亲二体性(UPD);鉴定出 2 个重复的 UPD,即 UPD4q 和 UPD7q。在 5 例中检测到 NPM1、RUNX1 和 TET2 的突变,其中 3 例携带致病性 RUNX1 突变。在一个携带 UPD4q 的病例中发现了 TET2 突变。
结果表明,21 三体阳性髓系恶性肿瘤在临床上具有高度的可变性,并且表现出异质性的拷贝数改变和突变模式。
