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PRAME的低甲基化是其在人类恶性肿瘤中异常过表达的原因。

Hypomethylation of PRAME is responsible for its aberrant overexpression in human malignancies.

作者信息

Schenk Tino, Stengel Sven, Goellner Stefanie, Steinbach Daniel, Saluz Hans Peter

机构信息

Department of Cell and Molecular Biology, Leibniz Institute for Natural Products Research and Infection Biology-Hans Knoell Institute, 07745 Jena, Germany.

出版信息

Genes Chromosomes Cancer. 2007 Sep;46(9):796-804. doi: 10.1002/gcc.20465.

Abstract

The preferentially expressed antigen of melanoma (PRAME) is expressed at high levels in large fractions of human malignancies, e.g., acute myeloid leukemia. Therefore, PRAME is an important marker for diagnosis of various malignant diseases and a relevant parameter for monitoring minimal residual disease. It is supposed to be involved in tumorigenic processes. Because of these important aspects we investigated its transcriptional regulation in detail. Most relevant was a detailed DNA methylation analysis of the PRAME 5' region by genomic sequencing in correlation with PRAME expression in various human patient samples and cell lines. In combination with DNA-truncation/transfection experiments with respect to DNA methylation, we show that changes in the methylation pattern in defined parts of the regulatory regions of PRAME are sufficient for its upregulation in cells usually not expressing the gene.

摘要

黑色素瘤优先表达抗原(PRAME)在大部分人类恶性肿瘤中高表达,如急性髓系白血病。因此,PRAME是诊断各种恶性疾病的重要标志物以及监测微小残留病的相关参数。它被认为参与肿瘤发生过程。鉴于这些重要方面,我们详细研究了其转录调控。最相关的是通过基因组测序对PRAME 5'区域进行详细的DNA甲基化分析,并将其与各种人类患者样本和细胞系中的PRAME表达相关联。结合关于DNA甲基化的DNA截短/转染实验,我们表明PRAME调控区域特定部分甲基化模式的改变足以使其在通常不表达该基因的细胞中上调。

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