人类白细胞检测系统。7微核源性染色体过早凝聚的进一步研究。

Humangenetik Pub Date : 1975-11-06 DOI:10.1007/BF00291947
G Obe, B Beek
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引用次数: 38

摘要

体外x射线诱导的人白细胞过早染色体凝聚(PCC)显示出剂量效应关系。在不同的培养时间下,未经colcolide处理的制备显示出微核频率和PCC与固定时间相关的复杂变化。PCC斑块在中期板中的位置和不同PCC类型(S型和G2型)的频率与x射线剂量无关。后者表明,微核在细胞周期中的减慢,这是PCC形成的原因,可能是一种调节现象的结果,而不是微核中染色质的非特异性生理损伤的结果。这一点在氚化胸苷标记实验中尤为明显,表明主核和微核之间的不同步程度与x射线剂量无关。氚化尿苷标记实验揭示了x射线剂量依赖性抑制主核和微核细胞的RNA合成。“粉末状”PCC贴片的s相性质可以通过约50%的氚化胸苷的掺入来验证。微核中着丝粒异染色质染色显示微核中有着丝粒异染色质的频率与有丝分裂中发现的g2期PCC的频率相似。
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The human leulocyte test system. VII. Further investigations concerning micronucleus-derived premature chromosome condensation.

Premature chromosome condensation (PCC) from X-ray induced micronuclei shows a dose-effect relationship in human leukocytes in vitro. Preparations at different culture times without colcemide treatment reveal complex variations of the frequencies of micronuclei and PCC correlated with the fixation time. The positions of PCC patches in the metaphase plate and the frequencies of different PCC types (S and G2) ar independent on the X-ray dose. The latter indicates that the slowing down of the micronuclei in the cell cycle, which is the reason for the formation of PCC, may be an outcome rather of a regulatory phenomenon than of an unspecific physiological damage of the chromatin included in the micronuclei. This is especially evident from labeling experiments with tritiated thymidine, showing that the extent of asynchrony between main nuclei and micronuclei is independent on the X-ray dose. Labeling experiments with tritiated uridine reveal a X-ray dose dependent suppression of RNA synthesis in cells with main nuclei and micronuclei. THE S-phase nature of "pulverized" PCC patches could be verified by incorporation of tritiated thymidine in aound 50%. Staining of centromeric heterochromatin in micronuclei reveal a frequency of micronuclei with centromeric heterochromatin resembling the frequency of G2-phase PCC found in mitoses.

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