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通过hTERT介导的永生化建立良性脑膜瘤细胞系。

Establishment of a benign meningioma cell line by hTERT-mediated immortalization.

作者信息

Püttmann Sylvia, Senner Volker, Braune Stephan, Hillmann Beate, Exeler Rita, Rickert Christian H, Paulus Werner

机构信息

Institute of Neuropathology, University Hospital, Münster, Germany.

出版信息

Lab Invest. 2005 Sep;85(9):1163-71. doi: 10.1038/labinvest.3700307.

Abstract

Meningioma represents the most common intracranial tumor, but well-characterized cell lines derived from benign meningiomas are not available. A major reason for the lack of benign tumor cell lines is senescence of nonmalignant cells in vitro, while malignant cells are often immortal. We have developed a meningioma cell line by retrovirally transducing primary cells derived from a human WHO grade I meningothelial meningioma with the human telomerase reverse transcriptase (hTERT) gene, which enables bypassing cellular senescence. Five clones have been cultured for more than 21 months so far, while corresponding nontransfected cells ceased proliferation within 3 months. Quantitative RT-PCR and a telomeric repeat amplification protocol (TRAP) assay revealed high hTERT mRNA levels and high telomerase activity in all transduced populations, while nontransduced cells were negative. The average telomere size of transduced cells was considerably longer than that of parental cells and the biopsy specimen. One clone, designated Ben-Men-1, was characterized in more detail, and exhibited typical cytological, immunocytochemical, ultrastructural and genetical features of meningioma, including whorl formation, expression of epithelial membrane antigen, desmosomes and interdigitating cell processes, as well as -22q. Following subdural transplantation into nude mice, tumor tissue with typical histological features of meningothelial meningioma was found. We conclude that Ben-Men-1 represents an immortalized yet differentiated cell line useful for biological and therapeutical studies on meningioma.

摘要

脑膜瘤是最常见的颅内肿瘤,但源自良性脑膜瘤的特征明确的细胞系尚不存在。缺乏良性肿瘤细胞系的一个主要原因是体外非恶性细胞的衰老,而恶性细胞往往是永生的。我们通过逆转录病毒转导来自一名WHO I级人脑膜内皮型脑膜瘤的原代细胞与人端粒酶逆转录酶(hTERT)基因,开发出了一种脑膜瘤细胞系,该基因能够绕过细胞衰老。目前已有5个克隆培养超过21个月,而相应的未转染细胞在3个月内停止增殖。定量逆转录聚合酶链反应(RT-PCR)和端粒重复序列扩增协议(TRAP)分析显示,所有转导群体中hTERT mRNA水平高且端粒酶活性高,而未转导细胞为阴性。转导细胞的平均端粒大小明显长于亲代细胞和活检标本。对一个名为Ben-Men-1的克隆进行了更详细的表征,其表现出脑膜瘤典型的细胞学、免疫细胞化学、超微结构和遗传学特征,包括漩涡状形成、上皮膜抗原表达、桥粒和指状细胞突起,以及-22q。将其硬膜下移植到裸鼠体内后,发现了具有脑膜内皮型脑膜瘤典型组织学特征的肿瘤组织。我们得出结论,Ben-Men-1代表了一种永生化但已分化的细胞系,可用于脑膜瘤的生物学和治疗研究。

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