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径迹结构和细胞失活对哺乳动物细胞重离子突变率计算的影响。

Effects of track structure and cell inactivation on the calculation of heavy ion mutation rates in mammalian cells.

作者信息

Cucinotta F A, Wilson J W, Shavers M R, Katz R

机构信息

NASA Langley Research Center, Hampton, VA 23681-0001, USA.

出版信息

Int J Radiat Biol. 1996 May;69(5):593-600. doi: 10.1080/095530096145607.

Abstract

It has long been suggested that inactivation severely effects the probability of mutation by heavy ions in mammalian cells. Heavy ions have observed cross sections of inactivation that approach and sometimes exceed the geometric size of the cell nucleus in mammalian cells. In the track structure model of Katz the inactivation cross section is found by summing an inactivation probability over all impact parameters from the ion to the sensitive sites within the cell nucleus. The inactivation probability is evaluated using the dose-response of the system to gamma-rays and the radial dose of the ions and may be equal to unity at small impact parameters for some ions. We show how the effects of inactivation may be taken into account in the evaluation of the mutation cross sections from heavy ions in the track structure model through correlation of sites for gene mutation and cell inactivation. The model is fit to available data for HPRT mutations in Chinese hamster cells and good agreement is found. The resulting calculations qualitatively show that mutation cross sections for heavy ions display minima at velocities where inactivation cross sections display maxima. Also, calculations show the high probability of mutation by relativistic heavy ions due to the radial extension of ions track from delta-rays in agreement with the microlesion concept. The effects of inactivation on mutations rates make it very unlikely that a single parameter such as LET or Z*2/beta(2) can be used to specify radiation quality for heavy ion bombardment.

摘要

长期以来,人们一直认为失活会严重影响哺乳动物细胞中重离子诱导突变的概率。在哺乳动物细胞中,已观察到重离子的失活截面接近并有时超过细胞核的几何尺寸。在卡茨的径迹结构模型中,失活截面是通过将离子到细胞核内敏感位点的所有碰撞参数的失活概率相加得到的。失活概率是利用系统对γ射线的剂量响应和离子的径向剂量来评估的,对于某些离子,在小碰撞参数下可能等于1。我们展示了如何通过基因突变位点与细胞失活的相关性,在径迹结构模型中评估重离子诱导突变截面时考虑失活的影响。该模型与中国仓鼠细胞中次黄嘌呤磷酸核糖转移酶(HPRT)突变的现有数据拟合良好。所得计算结果定性地表明,重离子的突变截面在失活截面显示最大值的速度处呈现最小值。此外,计算结果表明,相对论性重离子由于δ射线导致的离子径迹径向扩展而具有很高的突变概率,这与微损伤概念一致。失活对突变率的影响使得诸如传能线密度(LET)或Z*2/β(2)等单个参数极不可能用于指定重离子轰击的辐射品质。

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