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首页> 外文期刊>BMC Cancer >A novel spheroid-based co-culture model mimics loss of keratinocyte differentiation, melanoma cell invasion, and drug-induced selection of ABCB5-expressing cells
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A novel spheroid-based co-culture model mimics loss of keratinocyte differentiation, melanoma cell invasion, and drug-induced selection of ABCB5-expressing cells

机译:一种新型球形的共培养模型模拟角蛋白酶细胞分化,黑素瘤细胞侵袭和药物诱导的ABCB5表达细胞选择

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摘要

Different 3D-cell culture approaches with varying degrees of complexity have been developed to serve as melanoma models for drug testing or mechanistic studies. While these 3D-culture initiatives are already often superior to classical 2D approaches, they are either composed of only melanoma cells or they are so complex that the behavior of individual cell types is hard to understand, and often they are difficult to establish and expensive. This study used low-attachment based generation of spheroids composed of up to three cell types. Characterization of cells and spheroids involved cryosectioning, immunofluorescence, FACS, and quantitative analyses. Statistical evaluation used one-way ANOVA with post-hoc Tukey test or Student's t-test. The tri-culture model allowed to track cellular behavior in a cell-type specific manner and recapitulated different characteristics of early melanoma stages. Cells arranged into a collagen-IV rich fibroblast core, a ring of keratinocytes, and groups of highly proliferating melanoma cells on the outside. Regularly, some melanoma cells were also found to invade the fibroblast core. In the absence of melanoma cells, the keratinocyte ring stratified into central basal-like and peripheral, more differentiated cells. Conversely, keratinocyte differentiation was clearly reduced upon addition of melanoma cells. Treatment with the cytostatic drug, docetaxel, restored keratinocyte differentiation and induced apoptosis of external melanoma cells. Remaining intact external melanoma cells showed a significantly increased amount of ABCB5-immunoreactivity. In the present work, a novel, simple spheroid-based melanoma tri-culture model composed of fibroblasts, keratinocytes, and melanoma cells was described. This model mimicked features observed in early melanoma stages, including loss of keratinocyte differentiation, melanoma cell invasion, and drug-induced increase of ABCB5 expression in external melanoma cells.
机译:已经开发出不同程度的复杂程度的不同3D细胞培养方法,以作为药物测试或机械研究的黑色素瘤模型。虽然这些3D文化倡议经常优于古典2D方法,但它们只由黑色素瘤细胞组成,或者它们是如此复杂的是,单个细胞类型的行为很难理解,并且通常它们难以建立和昂贵。这项研究使用了由最多三种细胞类型组成的低附着的球形球体。细胞和球状体的表征涉及冷冻渗滤,免疫荧光,FACS和定量分析。统计评估使用单向ANOVA与HOC TUKEY测试或学生的T检验。三培养模型允许以细胞型特异性方式追踪细胞行为,并综合早期黑色素瘤阶段的不同特征。细胞排列成胶原-4-富集的成纤维细胞核心,异腔环的环,外部的高增殖黑素瘤细胞。定期,还发现一些黑色素瘤细胞侵入成纤维细胞核心。在没有黑素瘤细胞的情况下,角蛋白细胞环分层成中央基质和外周,更分化的细胞。相反,在加入黑素瘤细胞时显着降低了角质形成细胞分化。用细胞抑制药物,多西紫杉醇治疗,恢复角质形成细胞分化,诱导外部黑素瘤细胞凋亡。剩余的完整外部黑素瘤细胞显示出显着增加的ABCB5-免疫反应性。在本作本作中,描述了由成纤维细胞,角质形成细胞和黑色素瘤细胞组成的新颖的简单的基于Sphanoid的黑色素瘤三培养模型。这种模型在早期黑色素瘤阶段观察到的特征,包括异心细胞分化,黑素瘤细胞侵袭和外部黑素瘤细胞中ABCB5表达的药物诱导的增长。

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