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体外纺锤体抑制剂诱导人淋巴细胞染色体不分离与染色体落后阈值的指征。

Indication for thresholds of chromosome non-disjunction versus chromosome lagging induced by spindle inhibitors in vitro in human lymphocytes.

作者信息

Elhajouji A, Tibaldi F, Kirsch-Volders M

机构信息

Anthropogenetics Laboratory, Vrije Universiteit Brussel, Belgium.

出版信息

Mutagenesis. 1997 May;12(3):133-40. doi: 10.1093/mutage/12.3.133.

Abstract

Risk assessment from exposure to spindle inhibitors should take into account the possibility of threshold concentration-response curves for aneuploidy induction. We analysed concentration-dependent induction of chromosome non-disjunction by well known spindle poisons (colchicine, carbendazim, mebendazole and nocodazole) and a reference clastogen, methyl methanesulphonate (MMS) in vitro in human lymphocytes; and integrated these findings with earlier results of chromosome loss in micronuclei. Chromosome non-disjunction was estimated on cytokinesis-blocked lymphocytes after simultaneous fluorescent in situ hybridization labelling with two chromosome-specific centromeric probes (chromosomes 1 and 17). The frequencies of spontaneous non-disjunction showed important inter-individual variations and were surprisingly high (7.04-15.39%). Lower concentrations of aneugens did not induce a statistically significant increase of non-disjunction frequencies over the respective control levels, whereas higher concentrations clearly induced a concentration-dependent increase in the non-disjunction frequencies with the four aneugens tested. On the contrary, even at high concentrations, MMS induced a slight increase in the frequency of non-disjunction but without being statistically significant when compared with the control frequencies. We estimated the inflection points, the first statistically significant concentrations, the last non-statistically significant concentrations and the number of events from concentration-response curves of chromosome non-disjunction and chromosome loss. A threshold-type of concentration-response for non-disjunction is highly probable for colchicine and nocodazole. For carbendazim and mebendazole the inflection point fell above the first statistically significant concentrations. But since it is obvious from dose-response curves where the inflection point/threshold lies, it appears that the model might be picking up some irregularities (possibly due to experimental variability in the dose-response curve at concentrations greater than the threshold). For accurate estimation of the threshold, analysis of more concentrations or more cells might be needed. Our data strongly indicate that in cultured human lymphocytes chromosome non-disjunction is a major mechanism of aneuploidy induction by spindle inhibitors and since non-disjunction occurs at lower concentration than chromosome loss, the aneuploidy threshold should be estimated on the basis of non-disjunction rather than on micronuclei frequencies (chromosome loss).

摘要

评估接触纺锤体抑制剂带来的风险时,应考虑非整倍体诱导的阈值浓度-反应曲线的可能性。我们在体外对人淋巴细胞中已知的纺锤体毒物(秋水仙碱、多菌灵、甲苯咪唑和诺考达唑)以及参比断裂剂甲磺酸甲酯(MMS)进行了浓度依赖性染色体不分离诱导分析;并将这些结果与早期微核中染色体丢失的结果相结合。在用两种染色体特异性着丝粒探针(1号和17号染色体)进行同步荧光原位杂交标记后,对胞质分裂阻滞的淋巴细胞进行染色体不分离评估。自发不分离的频率显示出个体间的显著差异,且令人惊讶地高(7.04 - 15.39%)。较低浓度的非整倍体诱导剂并未使不分离频率相较于各自的对照水平有统计学显著增加,而较高浓度明显导致了所测试的四种非整倍体诱导剂的不分离频率呈浓度依赖性增加。相反,即使在高浓度下,MMS也仅使不分离频率略有增加,但与对照频率相比无统计学显著性。我们从染色体不分离和染色体丢失的浓度-反应曲线中估计了拐点、首个具有统计学显著性的浓度、最后一个无统计学显著性的浓度以及事件数量。秋水仙碱和诺考达唑极有可能存在不分离的阈值型浓度-反应。对于多菌灵和甲苯咪唑,拐点高于首个具有统计学显著性的浓度。但由于从剂量-反应曲线中拐点/阈值所在位置明显可知,该模型似乎可能捕捉到了一些不规则性(可能是由于浓度高于阈值时剂量-反应曲线中的实验变异性)。为了准确估计阈值,可能需要分析更多浓度或更多细胞。我们的数据有力地表明,在培养的人淋巴细胞中,染色体不分离是纺锤体抑制剂诱导非整倍体的主要机制,并且由于不分离发生的浓度低于染色体丢失,非整倍体阈值应基于不分离而非微核频率(染色体丢失)来估计。

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