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Merkel 细胞多瘤病毒阳性 Merkel 细胞癌细胞系 MS-1 的早期传代特征及其在 NOD scid gamma 小鼠中的生长。

Characterization of an early passage Merkel cell polyomavirus-positive Merkel cell carcinoma cell line, MS-1, and its growth in NOD scid gamma mice.

机构信息

Cancer Virology Program, University of Pittsburgh Cancer Institute, Pittsburgh, PA 15213, USA.

出版信息

J Virol Methods. 2013 Jan;187(1):6-14. doi: 10.1016/j.jviromet.2012.10.001. Epub 2012 Oct 18.

Abstract

Merkel cell carcinoma (MCC) is an aggressive skin cancer with a high mortality rate. The majority of MCC (70-80%) harbor clonally integrated Merkel cell polyomavirus (MCV) in the tumor genome and express viral T antigen oncoproteins. The characterization of an early passage MCV-positive MCC cell line MS-1 is described, and its cellular, immunohistochemical, and virological features to MCV-negative (UISO, MCC13, and MCC26) and MCV-positive cell lines (MKL-1 and MKL-2) were compared. The MS-1 cellular genome harbors integrated MCV, which preserves an identical viral sequence from its parental tumor. Neither VP2 gene transcripts nor VP1 protein are detectable in MS-1 or other MCV-positive MCC cell lines tested. Mapping of viral and cellular integration sites in MS-1 and MCC tumor samples demonstrates no consistent viral or cellular gene integration locus. All MCV-positive cell lines show cytokeratin 20 positivity and grow in suspension. When injected subcutaneously into NOD scid gamma (NSG) mice, MS-1 forms a discrete macroscopic tumor. Immunophenotypic analysis of the MS-1 cell line and xenografts in mice show identical profiles to the parental tumor biopsy. Hence, MS-1 is an early passage cell line that provides a useful in vitro model to characterize MCV-positive MCC.

摘要

默克尔细胞癌(Merkel cell carcinoma,MCC)是一种具有高死亡率的侵袭性皮肤癌。大多数 MCC(70-80%)在肿瘤基因组中具有克隆整合的默克尔细胞多瘤病毒(Merkel cell polyomavirus,MCV),并表达病毒 T 抗原致癌蛋白。本文描述了一株早期传代的 MCV 阳性 MCC 细胞系 MS-1,并比较了其细胞、免疫组织化学和病毒学特征与 MCV 阴性(UISO、MCC13 和 MCC26)和 MCV 阳性细胞系(MKL-1 和 MKL-2)。MS-1 细胞基因组中整合了 MCV,保留了与其亲本肿瘤相同的病毒序列。在 MS-1 或其他测试的 MCV 阳性 MCC 细胞系中,均无法检测到 VP2 基因转录本或 VP1 蛋白。MS-1 和 MCC 肿瘤样本中病毒和细胞整合位点的定位表明,没有一致的病毒或细胞基因整合位点。所有 MCV 阳性细胞系均显示角蛋白 20 阳性,并在悬浮状态下生长。当将 MS-1 细胞系皮下注射到 NOD scid gamma(NSG)小鼠中时,可形成离散的肉眼可见肿瘤。MS-1 细胞系和小鼠异种移植物的免疫表型分析显示与亲本肿瘤活检具有相同的特征。因此,MS-1 是一株早期传代的细胞系,为研究 MCV 阳性 MCC 提供了有用的体外模型。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9dec/3606892/936355422f51/nihms-416636-f0001.jpg

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