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在大鼠结肠细胞介导的诱变试验中结肠致癌物1,2 - 二甲基肼的活化作用。

Activation of the colon carcinogen 1,2-dimethylhydrazine in a rat colon cell-mediated mutagenesis assay.

作者信息

Oravec C T, Jones C A, Huberman E

出版信息

Cancer Res. 1986 Oct;46(10):5068-71.

PMID:3756864
Abstract

Suspensions of rat colon epithelial cells metabolized the potent colon carcinogen, 1,2-[14C]dimethylhydrazine (DMH), into 14C-labeled, alkali-soluble volatile products, presumably CO2. The colon cell suspensions, however, were less effective than rat hepatocyte suspensions. In addition, we used a cell-mediated mutagenesis assay to test rat colon epithelial cells grown from tissue explants for their ability to metabolize DMH into products mutagenic for human P3 teratoma cells. Mutagenesis in the P3 cells was indicated by an acquired resistance to 6-thioguanine. Cocultivation of the colon cells with the P3 cells in the cell-mediated assay resulted in mutagenesis, whereas in the absence of the colon cells, no mutagenesis by DMH was observed. Similar results were obtained in a hepatocyte-mediated mutagenesis assay. Colon cells were also able to activate another carcinogen, benzo(a)pyrene, into products mutagenic for the P3 cells. Individual epithelial clonal populations isolated from the colon cultures grown from tissue explants, however, expressed different capacities to activate DMH and benzo(a)pyrene into mutagens, and a high degree of DMH activation by cells from a colon clone was not necessarily associated with a similar degree of benzo(a)pyrene activation. Our results indicate that the colon itself contains epithelial cell types capable of effectively converting DMH into mutagenic (and presumably carcinogenic) products without necessarily involving intermediary metabolism by hepatocytes as previously thought.

摘要

大鼠结肠上皮细胞悬液可将强效结肠致癌物1,2-[¹⁴C]二甲基肼(DMH)代谢为¹⁴C标记的、碱溶性挥发性产物,推测为二氧化碳。然而,结肠细胞悬液的代谢效率低于大鼠肝细胞悬液。此外,我们使用细胞介导的诱变试验来检测从组织外植体生长而来的大鼠结肠上皮细胞将DMH代谢为对人P3畸胎瘤细胞具有致突变性产物的能力。P3细胞中的诱变通过对6-硫鸟嘌呤获得性抗性来指示。在细胞介导的试验中,结肠细胞与P3细胞共培养导致诱变,而在没有结肠细胞的情况下,未观察到DMH引起的诱变。在肝细胞介导的诱变试验中也获得了类似结果。结肠细胞还能够将另一种致癌物苯并(a)芘激活为对P3细胞具有致突变性的产物。然而,从组织外植体生长的结肠培养物中分离出的单个上皮克隆群体,在将DMH和苯并(a)芘激活为诱变剂方面表现出不同的能力,并且结肠克隆的细胞对DMH的高度激活不一定与对苯并(a)芘的类似激活程度相关。我们的结果表明,结肠本身含有能够有效将DMH转化为诱变(可能致癌)产物的上皮细胞类型,而不一定如先前认为的那样涉及肝细胞的中间代谢。

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