首页> 美国卫生研究院文献>Journal of the Boston Society of Medical Sciences >Proto-oncogene and growth factor/receptor expression in the establishment of primary human non-small cell lung carcinoma cell lines.
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Proto-oncogene and growth factor/receptor expression in the establishment of primary human non-small cell lung carcinoma cell lines.

机译:原发性人类非小细胞肺癌细胞系建立中的原癌基因和生长因子/受体表达。

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摘要

In our effort to delineate factors that govern the ability of non-small cell lung carcinoma (NSCLC) to form monolayer cell lines, we have attempted to derive monolayer cell lines from the primary cultures of 29 unselected human NSCLCs. Eight new lines were obtained. Cell lines were easier to establish from poorly differentiated tumors, especially adenocarcinomas. One cell line was from a large cell neuroendocrine carcinoma. All cell lines were aneuploid, and they exhibited heterogeneous nutritional requirements for growth in vitro. Cell line-forming primary tumors demonstrated higher mean messenger RNA expression levels for transforming growth factor-alpha and c-met proto-oncogene than did tumors that failed to form cell lines. Although a high level of c-myc expression was correlated with the ability of NSCLC cell lines to form xenograft tumors in nude mice, it was not correlated with the ability of primary tumors to establish cell lines. The results suggest that autocrine growth loops play important roles in the ability of NSCLC cells to proliferate continuously in monolayer culture. The fact that the overexpression of transforming growth factor-alpha in NSCLCs has been negatively correlated with patient survival and that most cell lines can be established only from poorly differentiated carcinomas may provide the explanation for a previous report that the capability for cell line establishment constitutes a negative prognostic indicator for patient survival. However, when the genotype and phenotype of the cell lines were compared with those of their corresponding primary or xenograft tumors, the tumor cells that grew continuously as a cell line often represented a selective subpopulation of the heterogeneous neoplastic cells in the primary tumors. This finding should be taken into consideration when cell lines are used to evaluate the chemo- and radiosensitivity of tumor cells.
机译:为了描述控制非小细胞肺癌(NSCLC)形成单层细胞系能力的因素,我们尝试从29种未选人类NSCLC的原代培养物中衍生出单层细胞系。获得了八条新线。细胞系更容易从低分化的肿瘤,尤其是腺癌中建立。一种细胞系来自大细胞神经内分泌癌。所有细胞系均为非整倍体,并且在体外生长中表现出不同的营养需求。与未能形成细胞系的肿瘤相比,形成细胞系的原发性肿瘤在转化生长因子-α和c-met原癌基因方面表现出更高的平均信使RNA表达水平。尽管高水平的c-myc表达与NSCLC细胞系在裸鼠中形成异种移植肿瘤的能力有关,但与原发肿瘤建立细胞系的能力无关。结果表明自分泌生长环在单层培养中持续增殖NSCLC细胞的能力中发挥重要作用。 NSCLCs中转化生长因子-α的过表达与患者存活率呈负相关,并且大多数细胞系只能由分化较弱的癌建立,这一事实可能为以前的报道提供了解释,即细胞系建立能力构成了患者生存的阴性预后指标。然而,当将细胞系的基因型和表型与其相应的原发性或异种移植肿瘤的基因型和表型进行比较时,作为细胞系连续生长的肿瘤细胞通常代表原发性肿瘤中异质性肿瘤细胞的选择性亚群。当使用细胞系评估肿瘤细胞的化学敏感性和放射敏感性时,应考虑到这一发现。

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