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肿瘤几何形状与肿瘤细胞对细胞毒性药物反应之间的关系——一项使用EMT6多细胞球体的体外研究。

The relationship between tumour geometry and the response of tumour cells to cytotoxic drugs--an in vitro study using EMT6 multicellular spheroids.

作者信息

Kwok T T, Twentyman P R

出版信息

Int J Cancer. 1985 May 15;35(5):675-82. doi: 10.1002/ijc.2910350517.

Abstract

Multicellular spheroids of the EMT6/Ca/VJAC mouse mammary tumour cell line have been used in an investigation of the effect of tumour geometry on the response of tumour cells to 3 cytotoxic drugs, adriamycin (ADM), nitrogen mustard (HN2) and CCNU. In addition to the inherent cellular drug response, factors related to spheroid structure, namely cell-cycle distribution, intercellular contact, drug penetration and microenvironment (pH, oxygen, glucose, etc.) are believed to influence the response of cells within spheroids to cytotoxic drugs. Selective enzymatic dissociation (with bacterial neutral protease) has been used to separate the cells within large (approximately 800 micron in diameter) spheroids into 4 distinct subpopulations. The cells within the subpopulations have been characterized by their DNA content, RNA content, tritiated thymidine labelling index, cell size and clonogenic capacity. It was found that cells at the surface of spheroids are relatively larger and more proliferative than cells towards the centre while their clonogenic capacity is similar. Studies on the responses of EMT6/Ca/VJAC log and plateau-phase monolayer cells have been carried out in parallel and have shown that cycling cells are more sensitive to ADM and HN2 than are non-cycling cells but somewhat less sensitive for the response to CCNU. Since the response patterns of cells from different regions of spheroids to HN2, treated either before disaggregation (intact spheroid) or after disaggregation (isolated spheroid cells), are similar and the surviving fraction increases from the surface towards the centre of the spheroid, cell cycle distribution is thought to be the only factor involved in the cytotoxicity of HN2 towards cells within the spheroids. Although the patterns of response to ADM of cells within intact spheroids and isolated spheroid cells are similar to those for HN2, the initial slope of the curve for intact spheroids is much steeper than that of the isolated spheroid cells. Therefore, in addition to the factor of cell-cycle distribution, drug penetration also appears to be involved in the action of ADM on spheroids, while the factors of intercellular contact and microenvironment appear to be relatively less important. The reverse pattern was found for the response of cells within different regions of spheroids to CCNU, treated as intact spheroids or as isolated spheroid cells (i.e., greater killing of inner compared with outer cells).(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

EMT6/Ca/VJAC小鼠乳腺肿瘤细胞系的多细胞球体已被用于研究肿瘤几何形状对肿瘤细胞对三种细胞毒性药物阿霉素(ADM)、氮芥(HN2)和环己亚硝脲(CCNU)反应的影响。除了固有的细胞药物反应外,与球体结构相关的因素,即细胞周期分布、细胞间接触、药物渗透和微环境(pH值、氧气、葡萄糖等),被认为会影响球体内细胞对细胞毒性药物的反应。选择性酶解(使用细菌中性蛋白酶)已被用于将大的(直径约800微米)球体内的细胞分离成4个不同的亚群。这些亚群中的细胞已通过其DNA含量、RNA含量、氚标记胸腺嘧啶掺入指数、细胞大小和克隆形成能力进行了表征。结果发现,球体表面的细胞比朝向中心的细胞相对更大且增殖性更强,而它们的克隆形成能力相似。同时对EMT6/Ca/VJAC对数期和平稳期单层细胞的反应进行了研究,结果表明,处于细胞周期的细胞对ADM和HN2比非细胞周期的细胞更敏感,但对CCNU的反应则稍不敏感。由于球体不同区域的细胞对HN2的反应模式,无论是在解离前(完整球体)还是解离后(分离的球体细胞)处理,都是相似的,并且存活分数从球体表面向中心增加,因此细胞周期分布被认为是HN2对球体内细胞细胞毒性的唯一相关因素。尽管完整球体和分离的球体细胞内的细胞对ADM的反应模式与HN2相似,但完整球体曲线的初始斜率比分离的球体细胞陡得多。因此,除了细胞周期分布因素外,药物渗透似乎也参与了ADM对球体的作用,而细胞间接触和微环境因素似乎相对不太重要。对于球体不同区域的细胞对CCNU的反应,作为完整球体或分离的球体细胞处理时发现了相反的模式(即内部细胞比外部细胞杀伤更大)。(摘要截选至400字)

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