Michelhaugh Sharon K, Guastella Anthony R, Varadarajan Kaushik, Klinger Neil V, Parajuli Prahlad, Ahmad Aamir, Sethi Seema, Aboukameel Amro, Kiousis Sam, Zitron Ian M, Ebrahim Salah A, Polin Lisa A, Sarkar Fazlul H, Bollig-Fischer Aliccia, Mittal Sandeep
Department of Neurosurgery, Wayne State University, 4160 John R Street, Suite 930, Detroit, MI, 48201, USA.
Department of Oncology, Wayne State University, Detroit, MI, 48201, USA.
J Transl Med. 2015 Jul 15;13:227. doi: 10.1186/s12967-015-0596-8.
There is a paucity of effective therapies for recurrent/aggressive meningiomas. Establishment of improved in vitro and in vivo meningioma models will facilitate development and testing of novel therapeutic approaches.
A primary meningioma cell line was generated from a patient with an olfactory groove meningioma. The cell line was extensively characterized by performing analysis of growth kinetics, immunocytochemistry, telomerase activity, karyotype, and comparative genomic hybridization. Xenograft models using immunocompromised SCID mice were also developed.
Histopathology of the patient tumor was consistent with a WHO grade I typical meningioma composed of meningothelial cells, whorls, and occasional psammoma bodies. The original tumor and the early passage primary cells shared the standard immunohistochemical profile consistent with low-grade, good prognosis meningioma. Low passage KCI-MENG1 cells were composed of two cell types with spindle and round morphologies, showed linear growth curve, had very low telomerase activity, and were composed of two distinct unrelated clones on cytogenetic analysis. In contrast, high passage cells were homogeneously round, rapidly growing, had high telomerase activity, and were composed of a single clone with a near triploid karyotype containing 64-66 chromosomes with numerous aberrations. Following subcutaneous and orthotopic transplantation of low passage cells into SCID mice, firm tumors positive for vimentin and progesterone receptor (PR) formed, while subcutaneous implant of high passage cells yielded vimentin-positive, PR-negative tumors, concordant with a high-grade meningioma.
Although derived from a benign meningioma specimen, the newly-established spontaneously immortal KCI-MENG1 meningioma cell line can be utilized to generate xenograft tumor models with either low- or high-grade features, dependent on the cell passage number (likely due to the relative abundance of the round, near-triploid cells). These human meningioma mouse xenograft models will provide biologically relevant platforms from which to investigate differences in low- vs. high-grade meningioma tumor biology and disease progression as well as to develop novel therapies to improve treatment options for poor prognosis or recurrent meningiomas.
对于复发性/侵袭性脑膜瘤,缺乏有效的治疗方法。建立改进的体外和体内脑膜瘤模型将有助于新型治疗方法的开发和测试。
从一名患有嗅沟脑膜瘤的患者中建立了一种原发性脑膜瘤细胞系。通过对生长动力学、免疫细胞化学、端粒酶活性、核型和比较基因组杂交进行分析,对该细胞系进行了广泛的表征。还建立了使用免疫缺陷SCID小鼠的异种移植模型。
患者肿瘤的组织病理学与世界卫生组织I级典型脑膜瘤一致,由脑膜内皮细胞、漩涡和偶尔的砂粒体组成。原始肿瘤和早期传代的原代细胞具有与低级别、预后良好的脑膜瘤一致的标准免疫组化特征。低传代的KCI-MENG1细胞由两种具有纺锤形和圆形形态的细胞类型组成,呈线性生长曲线,端粒酶活性非常低,细胞遗传学分析显示由两个不同的无关克隆组成。相比之下,高传代细胞均为圆形,生长迅速,端粒酶活性高,由一个具有近三倍体核型的单一克隆组成,含有64-66条染色体且有许多畸变。将低传代细胞皮下和原位移植到SCID小鼠中后,形成了波形蛋白和孕激素受体(PR)阳性的坚实肿瘤,而高传代细胞的皮下植入产生了波形蛋白阳性、PR阴性的肿瘤,与高级别脑膜瘤一致。
尽管源自良性脑膜瘤标本,但新建立的自发永生化KCI-MENG1脑膜瘤细胞系可用于生成具有低级别或高级别特征的异种移植肿瘤模型,这取决于细胞传代次数(可能是由于圆形、近三倍体细胞的相对丰度)。这些人脑膜瘤小鼠异种移植模型将提供生物学相关的平台,从中研究低级别与高级别脑膜瘤肿瘤生物学和疾病进展的差异,以及开发新的疗法以改善预后不良或复发性脑膜瘤的治疗选择。
Zotero 插件
