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低剂量暴露于遗传毒性化合物双酚A和鱼藤酮的机制研究。

Mechanistic investigations of low dose exposures to the genotoxic compounds bisphenol-A and rotenone.

作者信息

Johnson George E, Parry Elizabeth M

机构信息

Institute of Life Science, School of Medicine, Swansea University, Singleton Park, Swansea SA2 8PP, Wales, UK.

出版信息

Mutat Res. 2008 Mar 12;651(1-2):56-63. doi: 10.1016/j.mrgentox.2007.10.019. Epub 2007 Nov 12.

Abstract

A complete hazard and risk assessment of any known genotoxin requires the evaluation of the mutagenic, clastogenic and aneugenic potential of the compound. In the case of aneugenic chemicals, mechanism of action (MOA) and quantitative responses may be investigated by studying their effects upon the fidelity of functioning of components of the cell cycle. These present studies have demonstrated that the plastics component bisphenol-A (BPA) and the natural pesticide rotenone induce micronuclei and modify the functioning of the microtubule organising centres (MTOCs) of the mitotic spindles of cultured mammalian cells in a dose-dependent manner. BPA and rotenone were used as model compounds in an investigation of dose response relationships for the hazard/risk assessment of aneugens. Thresholds of action for the induction of aneuploidy have been predicted for spindle poisons on the basis of the multiple targets, which may need disabling before a quantitative response can be detected. The cytokinesis blocked micronucleus assay (CBMA) methodology was utilised in the human lymphoblastoid cell lines AHH-1, MCL-5 and Chinese hamster V79 cell lines. A no observable effect level (NOEL) at 10.8 microg/ml BPA was observed for MN induction. Rotenone showed a small increase in MN induction with the first significant effect at 0.25 ng/ml in V79 cells but there was no significant effect in the metabolically competent cell line, MCL-5. For a mechanistic evaluation of the aneugenic effects of BPA and rotenone, fluorescently labelled antibodies were used to visualise microtubules (alpha-tubulin) and MTOCs (gamma-tubulin). The NOELs for tripolar mitotic spindle induction in V79 cells were 7 microg/ml for BPA and 80 pg/ml for rotenone (concentrations which produced similar changes to mitotic index (M.I.)). Interestingly there was close proximity to the NOEL of 10.8 microg/ml BPA for micronucleus (MN) induction in the human lymphoblastoid AHH-1 cell. Multiple MTOCs can therefore be predicted as a possible mechanism for MN induction. The similarity in concentration inducing tripolar mitosis, M.I. and MN changes suggests immunofluorescence analysis to be a useful dose setting assay with emphasis on the mechanism.

摘要

对任何已知基因毒素进行全面的危害和风险评估,都需要评估该化合物的致突变性、染色体断裂性和非整倍体诱导性。对于具有非整倍体诱导性的化学物质,可通过研究其对细胞周期组成部分功能保真度的影响,来探究其作用机制(MOA)和定量反应。目前的这些研究表明,塑料成分双酚A(BPA)和天然杀虫剂鱼藤酮可诱导微核,并以剂量依赖的方式改变培养的哺乳动物细胞有丝分裂纺锤体微管组织中心(MTOC)的功能。在一项关于非整倍体诱导剂危害/风险评估的剂量反应关系研究中,BPA和鱼藤酮被用作模型化合物。基于多个靶点,已经预测了纺锤体毒物诱导非整倍体的作用阈值,在检测到定量反应之前,这些靶点可能需要被破坏。在人淋巴母细胞系AHH-1、MCL-5和中国仓鼠V79细胞系中采用了胞质分裂阻断微核试验(CBMA)方法。观察到BPA在10.8微克/毫升时对微核诱导无明显影响水平(NOEL)。鱼藤酮在V79细胞中微核诱导有小幅增加,在0.25纳克/毫升时首次出现显著影响,但在代谢活性细胞系MCL-5中无显著影响。为了对BPA和鱼藤酮的非整倍体诱导作用进行机制评估,使用荧光标记抗体来观察微管(α-微管蛋白)和MTOC(γ-微管蛋白)。在V79细胞中,BPA诱导三极有丝分裂纺锤体的NOEL为7微克/毫升,鱼藤酮为80皮克/毫升(这些浓度对有丝分裂指数(M.I.)产生了类似变化)。有趣的是,在人淋巴母细胞AHH-1中,诱导微核(MN)的BPA的NOEL与10.8微克/毫升非常接近。因此,可以预测多个MTOC是微核诱导的一种可能机制。诱导三极有丝分裂、M.I.和MN变化的浓度相似性表明,免疫荧光分析是一种有用的剂量设定试验,重点在于作用机制。

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