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正常小鼠细胞降低转化的小鼠膀胱上皮细胞恶性潜能的能力取决于它们的体细胞起源。

The ability of normal mouse cells to reduce the malignant potential of transformed mouse bladder epithelial cells depends on their somatic origin.

作者信息

Cowell J K, Franks L M

出版信息

Int J Cancer. 1984 May 15;33(5):657-67. doi: 10.1002/ijc.2910330517.

Abstract

Somatic cell hybrids have been made between a transformed mouse bladder carcinoma cell line and normal mouse bladder epithelium and mesenchyme. In the epithelial tumour/mesenchyme hybrids the malignant phenotype was expressed dominantly whereas in the carcinoma/normal epithelium hybrids the malignant potential was greatly reduced. In both cases the dominant in vitro and in vivo phenotype was that of the normal parental cells. All hybrid tumours were first palpable after 4-7 days, demonstrating that the tumours had not arisen as a result of in vivo selection of a sub-population of tumorigenic cells. Chromosome analysis showed that the carcinoma/normal epithelium hybrids were all in the hypertetraploid range but the large variation in the karyotypic profile of each hybrid made it impossible to implicate any specific chromosomes in the control of expression of the malignant phenotype. During normal development in bladder epithelium, terminal differentiation is associated with tetraploid formation by cell fusion. The reduction in malignancy of the carcinoma/normal epithelium hybrids may perhaps be due to the expression of genes associated with normal terminal differentiation after cell fusion and tetraploid formation. This is also supported by the more differentiated phenotype of the hybrid tumours. Of the 10 mesenchyme/epithelium hybrids analysed cytogenetically , four were in the hypertetraploid range from which little meaningful data could be obtained about specific chromosome losses. Chromosome analysis of the cells from the near-tetraploid hybrids showed only minor differences from what might have been expected from the input of the two parents; these differences appeared to be due to random chromosome loss. The maximum number of chromosomes lost from any of the hybrids was five, although one, two or three was more usual. The only consistent chromosome loss was of a single copy of chromosome 4, which in two of the hybrids represented the only chromosome change. The possibility that this loss might facilitate re-expression of the malignant phenotype is discussed.

摘要

已在一种转化的小鼠膀胱癌细胞系与正常小鼠膀胱上皮和间充质之间构建了体细胞杂种。在上皮肿瘤/间充质杂种中,恶性表型呈显性表达,而在癌/正常上皮杂种中,恶性潜能大大降低。在这两种情况下,体外和体内的显性表型均为正常亲代细胞的表型。所有杂种肿瘤在4 - 7天后首次可触及,表明这些肿瘤并非因体内致瘤细胞亚群的选择而产生。染色体分析显示,癌/正常上皮杂种均处于超四倍体范围内,但每个杂种的核型图谱差异很大,无法确定任何特定染色体与恶性表型表达的控制有关。在膀胱上皮的正常发育过程中,终末分化与细胞融合导致的四倍体形成相关。癌/正常上皮杂种恶性程度的降低可能是由于细胞融合和四倍体形成后与正常终末分化相关的基因表达。杂种肿瘤更分化的表型也支持了这一点。在经细胞遗传学分析的10个间充质/上皮杂种中,4个处于超四倍体范围内,从中无法获得关于特定染色体丢失的有意义数据。近四倍体杂种细胞的染色体分析显示,与两个亲本输入所预期的情况相比,只有微小差异;这些差异似乎是由于随机染色体丢失所致。任何杂种中丢失的染色体最多为5条,不过通常是丢失1条、2条或3条。唯一一致的染色体丢失是第4号染色体的单拷贝丢失,在其中两个杂种中,这是唯一的染色体变化。文中讨论了这种丢失可能促进恶性表型重新表达的可能性。

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