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一种用于检测肿瘤启动子依赖性向肿瘤表型进展的细胞培养分析:肿瘤启动子和促癌抑制剂的检测

A cell culture assay for tumor-promoter-dependent progression toward neoplastic phenotype: detection of tumor promoters and promotion inhibitors.

作者信息

Colburn N H, Koehler B A, Nelson K J

出版信息

Teratog Carcinog Mutagen. 1980;1(1):87-96. doi: 10.1002/tcm.1770010109.

Abstract

Mouse epidermal cell lines have been identified which respond to tumor-promoting (but not nonpromoting) phorbol esters with an irreversible shift in anchorage independence, an in vitro marker of neoplastic phenotype. This response may be analogous to a later stage of tumor promotion in vivo. The shift occurs at TPA concentrations as low as 0.1 ng/ml (1.6 x 10(-10) M). The specificity of the soft agar growth response is not limited to phorbol esters but extends to nonphorbol plant diterpenes such as mezerein, to detergents, to polycyclic hydrocarbons present in cigarette smoke, and to some growth factors. All of the above classes of compounds have been previously shown to have tumor-promoting and/or cocarcinogenic activity in mouse skin in vivo. Clonal heterogeneity for TPA responsiveness has been found. Clones which were highly responsive to phorbol esters were also highly responsive to other classes of promoters, indicating their usefulness both for promoter detection and mechanism studies. The anchorage-independence to response to TPA was inhibited by a series of retinoids whose activity paralleled that for inhibiting tumor promotion in vivo. Both retinoid inhibition and clonal heterogeneity for promoter response are being utilized to study determinants of preneoplastic progression.

摘要

已鉴定出小鼠表皮细胞系,它们对促肿瘤(而非非促肿瘤)佛波酯产生反应,表现为锚定独立性发生不可逆转变,这是肿瘤表型的一种体外标志物。这种反应可能类似于体内肿瘤促进的后期阶段。该转变在佛波酯浓度低至0.1 ng/ml(1.6×10⁻¹⁰ M)时发生。软琼脂生长反应的特异性不仅限于佛波酯,还扩展到非佛波植物二萜类化合物如芫花酯素、去污剂、香烟烟雾中的多环烃以及一些生长因子。上述所有类别的化合物先前已被证明在小鼠皮肤体内具有促肿瘤和/或协同致癌活性。已发现对佛波酯的反应存在克隆异质性。对佛波酯高度反应的克隆对其他类别的启动子也高度反应,表明它们在启动子检测和机制研究中都很有用。一系列类视黄醇抑制了对佛波酯的反应所导致的锚定独立性,其活性与体内抑制肿瘤促进的活性相当。类视黄醇抑制和启动子反应的克隆异质性都被用于研究肿瘤前进展的决定因素。

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