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H-ras的表达与转移潜能相关:10T1/2和NIH 3T3细胞中转移表型直接调控的证据。

Expression of H-ras correlates with metastatic potential: evidence for direct regulation of the metastatic phenotype in 10T1/2 and NIH 3T3 cells.

作者信息

Egan S E, McClarty G A, Jarolim L, Wright J A, Spiro I, Hager G, Greenberg A H

出版信息

Mol Cell Biol. 1987 Feb;7(2):830-7. doi: 10.1128/mcb.7.2.830-837.1987.

Abstract

Using three independent approaches, we studied the effects of H-ras on metastasis formation. Analysis of five in vitro-ras-transfected 10T1/2 clones with either flat or refractile morphologies revealed a relationship between metastatic potential, H-ras expression, and anchorage-independent growth. Four metastatic variants derived from a poorly metastatic, low-H-ras-expressing line all expressed high levels of H-ras RNA and grew efficiently in soft agar. Activation of H-ras expression in the metastatic tumors had occurred through amplification and rearrangement of H-ras sequences. In addition, preinduction of p21 synthesis in NIH 3T3 line 433, which contains v-H-ras under transcriptional control of the glucocorticoid-sensitive mouse mammary tumor virus long terminal repeat, significantly increased metastatic efficiency. Glucocorticoid treatment of normal or pEJ-transformed NIH 3T3 cells did not affect metastatic potential. These data reveal a direct relationship between ras expression and metastasis formation and suggest that metastatic and transformed phenotypes may be coregulated in ras-transformed 10T1/2 and NIH 3T3 cells.

摘要

我们采用三种独立的方法研究了H-ras对转移形成的影响。对五个具有扁平或折光形态的体外ras转染10T1/2克隆进行分析,揭示了转移潜能、H-ras表达和不依赖贴壁生长之间的关系。从一个低转移性、低H-ras表达系衍生出的四个转移变体均表达高水平的H-ras RNA,并能在软琼脂中高效生长。转移瘤中H-ras表达的激活是通过H-ras序列的扩增和重排实现的。此外,在含有受糖皮质激素敏感的小鼠乳腺肿瘤病毒长末端重复序列转录控制的v-H-ras的NIH 3T3 433细胞系中,预先诱导p21合成可显著提高转移效率。对正常或pEJ转化的NIH 3T3细胞进行糖皮质激素处理并不影响转移潜能。这些数据揭示了ras表达与转移形成之间的直接关系,并表明在ras转化的10T1/2和NIH 3T3细胞中,转移表型和转化表型可能受到共同调控。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f6bb/365141/8055ad3d541c/molcellb00074-0276-a.jpg

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