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通过微核试验评估的十种模型诱变剂。

Ten model mutagens evaluated by the micronucleus test.

作者信息

Maier P, Schmid W

出版信息

Mutat Res. 1976 Nov;40(4):325-37. doi: 10.1016/0165-1218(76)90031-8.

Abstract

The following ten mutagenic compounds were subjected to the micronucleus bone marrow test (MNT) in the mouse: cyclophosphamide (CTX), thiotepa (TT), vincristin (VCR), colcemid (COLC), adriamycin (AM), bleomycin (BM), cytosin arabinoside (ARA C), 6-mercaptopurine (6-MP), methotrexate (MTX) and 5-fluorouracil (5-FU). Dose-effect curves were established for all compounds. With the exception of CTX, COLC and AM, the drugs also were subjected to chromosome analyses on Chinese hamster fibroblasts in vitro. The MNT revealed loss of chromatin due to chromosome breakage and rearrangements by CTX, TT and AM, to breakage by ARA C, 6-MP, MTX and 5-FU, as well as loss of entire chromosomes caused by impairment of the spindle by VCR and COLC. With the exception of BM, the effects were demonstrable in the therapeutic dose range. The MNT, provided it is carried out by the methodology of the authors, not only reveals chromatin loss but permits important conclusions in regard to the proliferative state of the bone marrow and the specific time of action of the mutagens in the cell cycle. If arrest of the cell cycle occurs, as in the case of anti-metabolites MTX and 5-FU particularly, the routine scheme of investigation needs to be modified since micronucleated cells appear only after release of the metabolic block, i.e. after a delay of 24 h. The negative bone marrow results obtained with BM emphasize the importance of combining in vivo and in vitro tests.

摘要

以下十种诱变化合物在小鼠身上进行了骨髓微核试验(MNT):环磷酰胺(CTX)、噻替派(TT)、长春新碱(VCR)、秋水仙酰胺(COLC)、阿霉素(AM)、博来霉素(BM)、阿糖胞苷(ARA C)、6-巯基嘌呤(6-MP)、甲氨蝶呤(MTX)和5-氟尿嘧啶(5-FU)。为所有化合物建立了剂量效应曲线。除CTX、COLC和AM外,这些药物还在体外对中国仓鼠成纤维细胞进行了染色体分析。骨髓微核试验显示,CTX、TT和AM导致染色体断裂和重排,从而使染色质丢失;ARA C、6-MP、MTX和5-FU导致染色体断裂;VCR和COLC使纺锤体受损,导致整条染色体丢失。除BM外,在治疗剂量范围内均可观察到这些效应。如果按照作者的方法进行骨髓微核试验,不仅可以揭示染色质丢失,还可以就骨髓的增殖状态以及诱变剂在细胞周期中的具体作用时间得出重要结论。如果像抗代谢物MTX和5-FU那样出现细胞周期停滞,常规的研究方案就需要修改,因为微核细胞仅在代谢阻滞解除后才出现,即延迟24小时后出现。用BM得到的阴性骨髓结果强调了体内和体外试验相结合的重要性。

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