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小鼠乳腺肿瘤细胞亚群的混合接种物会导致器官特异性转移的变化。

Mixed inocula of mouse mammary tumour cell subpopulations result in changes of organ-specific metastasis.

作者信息

Hossain A, Sarkar A, Sarkar N H

机构信息

Department of Immunology and Microbiology, Medical College of Georgia, Augusta 30912-2100.

出版信息

Clin Exp Metastasis. 1991 Nov-Dec;9(6):501-15. doi: 10.1007/BF01768579.

Abstract

Tumour and metastatic phenotypes, the pattern of mouse mammary tumour virus (MMTV) integration and expression, and the expression of a metastasis associated gene, nm23, were examined in three mammary tumour cell subpopulations, 66, 168 and 4526. Tumour growth, host survival, metastatic aggressiveness, and the distribution of different cell types in metastasis resulting from mixed cell inocula were also analysed. The results of these studies indicated that the cell lines were distinguishable from each other both phenotypically and genotypically. However, a rearrangement of the mammary tumour specific protooncogene, int-1, caused by MMTV was found to be a unique characteristic of the cell line 4526. Therefore, int-1 was used as a stable marker to examine the genotype of the metastatic colonies that developed in mice bearing tumours of mixed cell inocula. Highly metastatic 4526 cells influenced the metastatic range of poorly metastatic 66 cells. Line 66 cells that normally colonize only to lungs were also found to colonize liver when inoculated together with the liver-metastasizing 4526 cells. This acquired metastatic phenotype of 66 cells was transient. On the contrary, mixed cell inocula of 4526 and non-metastatic 168 cells did not produce any colony of 168 cells. The metastatic aggressiveness of 4526 cells was inhibited by both 66 and 168 cells. Furthermore, the metastatic behaviour of mixed inocula differed depending on the relative abundance of the component populations in the mixtures. These findings suggest that interaction between cells of different metastatic phenotypes may result in changes of their metastatic behaviour.

摘要

在三个乳腺肿瘤细胞亚群66、168和4526中,检测了肿瘤和转移表型、小鼠乳腺肿瘤病毒(MMTV)整合与表达模式以及转移相关基因nm23的表达。还分析了肿瘤生长、宿主存活、转移侵袭性以及混合细胞接种所导致转移中不同细胞类型的分布。这些研究结果表明,这些细胞系在表型和基因型上彼此可区分。然而,发现由MMTV引起的乳腺肿瘤特异性原癌基因int-1的重排是细胞系4526的独特特征。因此,int-1被用作稳定标记,以检测在接种混合细胞肿瘤的小鼠中形成的转移菌落的基因型。高转移性的4526细胞影响低转移性66细胞的转移范围。通常仅在肺部定植的66细胞系,当与可转移至肝脏的4526细胞一起接种时,也被发现可在肝脏中定植。66细胞这种获得性转移表型是短暂的。相反,4526细胞与非转移性168细胞的混合接种未产生任何168细胞菌落。4526细胞的转移侵袭性受到66和168细胞的抑制。此外,混合接种的转移行为因混合物中各组分群体的相对丰度而异。这些发现表明,不同转移表型的细胞之间的相互作用可能导致其转移行为发生变化。

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