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原发性人类睾丸生殖细胞肿瘤中OCT3/4上游区域的差异甲基化

Differential methylation of the OCT3/4 upstream region in primary human testicular germ cell tumors.

作者信息

De Jong Jeroen, Weeda Sannah, Gillis Ad J M, Oosterhuis J Wolter, Looijenga Leendert H J

机构信息

Department of Pathology, Erasmus MC-University Medical Center Rotterdam, Josephine Nefkens Institute, Daniel den Hoed Cancer Center, 3000 CA Rotterdam, The Netherlands.

出版信息

Oncol Rep. 2007 Jul;18(1):127-32.

PMID:17549357
Abstract

Germ cell tumors show many similarities to normal embryogenesis. This is, for example, illustrated by the expression of the marker of pluripotency, OCT3/4, known to play a pivotal role in the early stages of normal development. Interestingly, it is found to be the most informative diagnostic marker for the early developmental stages of malignant germ cell tumors. Expression regulation of OCT3/4 has been extensively studied in murine and human cell lines, including embryonic stem cell lines and tumor derived cell lines. We investigated for the first time the methylation status of the upstream region of the OCT3/4 gene in normal and neoplastic testicular primary tissues using bisulfite genomic sequencing. The cell line JKT-1, supposedly seminoma-derived, was included in the survey. Normal testis parenchyma, peripheral blood lymphocytes, spermatocytic seminoma, yolk sac tumor and teratoma, and JKT-1 showed a consistent hypermethylation. In contrast, seminoma and embryonal carcinoma were hypomethylated, confirmed by analyses after tumor micro-dissection. Testicular lymphomas showed the most heterogeneous pattern, although specific regions were consistently hypermethylated. In conclusion, the results obtained from this set of adult normal and neoplastic in vivo derived samples is in accordance to the in vitro data that expression of OCT3/4 is associated with specific changes in methylation. Moreover, the findings argue against OCT3/4 being a driving oncogenic factor in the pathogenesis of human germ cell tumors.

摘要

生殖细胞肿瘤与正常胚胎发育有许多相似之处。例如,多能性标志物OCT3/4的表达就说明了这一点,已知该标志物在正常发育的早期阶段起着关键作用。有趣的是,它被发现是恶性生殖细胞肿瘤早期发育阶段最具信息价值的诊断标志物。OCT3/4的表达调控已在小鼠和人类细胞系中进行了广泛研究,包括胚胎干细胞系和肿瘤衍生细胞系。我们首次使用亚硫酸氢盐基因组测序研究了正常和肿瘤性睾丸原发性组织中OCT3/4基因上游区域的甲基化状态。调查中纳入了据推测源自精原细胞瘤的JKT-1细胞系。正常睾丸实质、外周血淋巴细胞、精母细胞性精原细胞瘤、卵黄囊瘤和畸胎瘤以及JKT-1均表现出一致的高甲基化。相比之下,精原细胞瘤和胚胎癌呈低甲基化,肿瘤微切割后的分析证实了这一点。睾丸淋巴瘤表现出最具异质性的模式,尽管特定区域始终呈高甲基化。总之,从这组成年正常和肿瘤性体内衍生样本中获得的结果与体外数据一致,即OCT3/4的表达与甲基化的特定变化相关。此外,这些发现反对OCT3/4是人类生殖细胞肿瘤发病机制中的驱动致癌因素。

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