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Growing colorectal tumors: minimizing microbial and stromal competition and assessing in vitro selection pressures

机译:结直肠肿瘤的生长:最大程度地减少微生物和基质竞争,并评估体外选择压力

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Development of primary colorectal cancer cell lines ishampered by contamination from regional microbes, overgrowthof stromal cells, and purported genetic drift from selectionpressures in vitro. We initiated 32 primaryadenocarcinomas, 3 recurrences and 6 distant metastases incell culture. Twelve cell lines from eleven tumors weregenerated (26.8%) overall. Nine of 32 primary tumorsyielded 10 cell lines, 5 were lost to contamination, 13 wereoverwhelmed by stromal cells, and 5 demonstrated no growth.Addition of isobutyl methyl xanthine (IBMX) to culturelimited fibroblastoid growth. There was no associationbetween tumor location (p = 0.535, mid-P), degree ofdifferentiation (p = 0.850, mid-P) or clinicopathologic stage(p = 0.400, mid-P), and the ability of cells to becomeestablished in culture. The majority of cell lines hadsimilar nuclear DNA content and expression of cell-surfaceantigens compared with their parent tumors. Microbialcontamination and stromal cell overgrowth present thegreatest obstacle to capturing a representative bank ofcolon tumors in vitro.
机译:原发性结肠直肠癌细胞系的发展受到区域微生物的污染,过度生长的基质细胞和体外选择压力的遗传漂移的阻碍。我们在细胞培养中启动了32例原发性腺癌,3例复发和6例远处转移。总共产生了来自11个肿瘤的12个细胞系(26.8%)。 32个原发性肿瘤产生的10个细胞系中有9个被污染,其中5个被污染而丢失,13个被基质细胞淹没,其中5个没有生长。在培养受限的成纤维细胞生长中加入了异丁基甲基黄嘌呤(IBMX)。肿瘤的位置(p = 0.535,中-P),分化程度(p = 0.850,中-P)或临床病理阶段(p = 0.400,中-P)与细胞在培养物中建立的能力之间没有关联。与它们的亲代肿瘤相比,大多数细胞系具有相似的核DNA含量和细胞表面抗原表达。微生物污染和基质细胞过度生长是在体外捕获代表性结肠癌库的最大障碍。

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