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首页> 外文期刊>Oncology reports >Maintenance of retinal cancer stem cell-like properties through long-term serum-free culture from human retinoblastoma.
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Maintenance of retinal cancer stem cell-like properties through long-term serum-free culture from human retinoblastoma.

机译:通过人类视网膜母细胞瘤的长期无血清培养来维持视网膜癌干细胞样特性。

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Previous studies have demonstrated that a small population of cancer stem cell-like cells exists in retinoblastoma. To provide a model for studying this population, we sought to establish a long-term culture from human retinoblastoma that have cancer stem cell-like properties. Fresh tumor tissue was digested and cultured in serum-free medium. Tumor spheres formed and were passaged continuously. Stem cell properties were examined through immunostaining, real-time quantitative RT-PCR and chemoresistance assay. Tumorigenicity of the tumor sphere-forming cells was confirmed by xenograft experiments. Furthermore, we examined the expression of cell surface markers CD44 and CD133. Tumor cells expanded as floating spheres for more than 30 passages. Sphere-forming cells overexpressed stem cell genes Oct4, Nestin and Pax6. Immunostaining of spheres showed positivity for Nestin, Pax6 and also ABCG2. In contrast, differentiated cells derived from these spheres expressed high levels of mature retinal cell markers MAP2, GFAP, recoverin, Opsin B and Nrl, and showed immunoreactivity for NF200, GFAP, recoverin and PKCalpha. Furthermore, both CD44 and CD133 were highly expressed in sphere-forming cells vs. differentiated cells. Sphere-forming cells displayed higher chemoresistance to carboplatin as opposed to differentiated cells. Moreover, intraocular injection of as few as 2x103 sphere-forming cells into NOD/SCID mice gave rise to new tumors similar to the original patient tumors. These results revealed that the sphere-forming cells preserved their stem cell properties and tumorigenicity, even after long-term culture. This would be a suitable in vitro model to study cancer stem-like cells in retinoblastoma and to develop chemotherapeutic drugs and strategies.
机译:先前的研究表明,视网膜母细胞瘤中存在少量癌症干细胞样细胞。为了提供用于研究该人群的模型,我们试图从具有癌症干细胞样特性的人视网膜母细胞瘤中建立长期培养物。消化新鲜的肿瘤组织并在无血清培养基中培养。肿瘤球形成并连续通过。通过免疫染色,实时定量RT-PCR和化学抗性检测来检查干细胞的特性。通过异种移植实验证实了肿瘤球形成细胞的致瘤性。此外,我们检查了细胞表面标志物CD44和CD133的表达。肿瘤细胞以浮球形式扩展了30多个传代。形成球的细胞过表达干细胞基因Oct4,Nestin和Pax6。球的免疫染色显示巢蛋白,Pax6和ABCG2阳性。相反,衍生自这些领域的分化细胞表达高水平的成熟视网膜细胞标志物MAP2,GFAP,recoverin,Opsin B和Nrl,并显示出对NF200,GFAP,recoverin和PKCalpha的免疫反应性。此外,CD44和CD133在球形细胞与分化细胞中均高表达。与分化细胞相反,成球细胞对卡铂显示出更高的化学抗性。而且,向NOD / SCID小鼠眼内注射少至2x103的球形成细胞会产生类似于原始患者肿瘤的新肿瘤。这些结果表明,即使经过长期培养,形成球形的细胞仍能保持其干细胞特性和致瘤性。这将是研究视网膜母细胞瘤中癌干样细胞并开发化学治疗药物和策略的合适的体外模型。

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