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高级别软组织肉瘤的综合DNA甲基化和基因表达分析

Integrative DNA methylation and gene expression analysis in high-grade soft tissue sarcomas.

作者信息

Renner Marcus, Wolf Thomas, Meyer Hannah, Hartmann Wolfgang, Penzel Roland, Ulrich Alexis, Lehner Burkhard, Hovestadt Volker, Czwan Esteban, Egerer Gerlinde, Schmitt Thomas, Alldinger Ingo, Renker Eva Kristin, Ehemann Volker, Eils Roland, Wardelmann Eva, Büttner Reinhard, Lichter Peter, Brors Benedikt, Schirmacher Peter, Mechtersheimer Gunhild

出版信息

Genome Biol. 2013 Dec 17;14(12):r137. doi: 10.1186/gb-2013-14-12-r137.

Abstract

BACKGROUND

High-grade soft tissue sarcomas are a heterogeneous, complex group of aggressive malignant tumors showing mesenchymal differentiation. Recently, soft tissue sarcomas have increasingly been classified on the basis of underlying genetic alterations; however, the role of aberrant DNA methylation in these tumors is not well understood and, consequently, the usefulness of methylation-based classification is unclear.

RESULTS

We used the Infinium HumanMethylation27 platform to profile DNA methylation in 80 primary, untreated high-grade soft tissue sarcomas, representing eight relevant subtypes, two non-neoplastic fat samples and 14 representative sarcoma cell lines. The primary samples were partitioned into seven stable clusters. A classification algorithm identified 216 CpG sites, mapping to 246 genes, showing different degrees of DNA methylation between these seven groups. The differences between the clusters were best represented by a set of eight CpG sites located in the genes SPEG, NNAT, FBLN2, PYROXD2, ZNF217, COL14A1, DMRT2 and CDKN2A. By integrating DNA methylation and mRNA expression data, we identified 27 genes showing negative and three genes showing positive correlation. Compared with non-neoplastic fat, NNAT showed DNA hypomethylation and inverse gene expression in myxoid liposarcomas, and DNA hypermethylation and inverse gene expression in dedifferentiated and pleomorphic liposarcomas. Recovery of NNAT in a hypermethylated myxoid liposarcoma cell line decreased cell migration and viability.

CONCLUSIONS

Our analysis represents the first comprehensive integration of DNA methylation and transcriptional data in primary high-grade soft tissue sarcomas. We propose novel biomarkers and genes relevant for pathogenesis, including NNAT as a potential tumor suppressor in myxoid liposarcomas.

摘要

背景

高级别软组织肉瘤是一组异质性、复杂的侵袭性恶性肿瘤,具有间充质分化特征。近来,软组织肉瘤越来越多地依据潜在的基因改变进行分类;然而,异常DNA甲基化在这些肿瘤中的作用尚未完全明确,因此基于甲基化的分类的实用性尚不清楚。

结果

我们使用Infinium HumanMethylation27平台对80例原发性、未经治疗的高级别软组织肉瘤(代表8种相关亚型)、2份非肿瘤性脂肪样本以及14种代表性肉瘤细胞系进行DNA甲基化分析。原发性样本被分为7个稳定的簇。一种分类算法鉴定出216个CpG位点,定位于246个基因,这些位点在这7组样本间呈现出不同程度的DNA甲基化。簇间差异最好由位于SPEG、NNAT、FBLN2、PYROXD2、ZNF217、COL14A1、DMRT2和CDKN2A基因中的8个CpG位点来体现。通过整合DNA甲基化和mRNA表达数据,我们鉴定出27个呈负相关的基因以及3个呈正相关的基因。与非肿瘤性脂肪相比,NNAT在黏液样脂肪肉瘤中表现为DNA低甲基化及基因表达下调,而在去分化脂肪肉瘤和多形性脂肪肉瘤中表现为DNA高甲基化及基因表达下调。在一个高甲基化的黏液样脂肪肉瘤细胞系中恢复NNAT表达可降低细胞迁移能力和活力。

结论

我们的分析首次全面整合了原发性高级别软组织肉瘤中的DNA甲基化和转录数据。我们提出了与发病机制相关的新生物标志物和基因,包括NNAT作为黏液样脂肪肉瘤中一种潜在的肿瘤抑制因子。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b678/4054884/b2d36ba0491d/gb-2013-14-12-r137-1.jpg

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