优化高剂量和部分体照射染色体剂量测定的显微镜时间安排。

Q4 Biochemistry, Genetics and Molecular Biology
Genome Integrity Pub Date : 2017-01-23 eCollection Date: 2017-01-01 DOI:10.4103/2041-9414.198908
Volodymyr A Vinnikov
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引用次数: 4

摘要

细胞遗传学分类的方法可以通过优化不同暴露场景的显微镜时间表来改进。在体外照射至~2、4和12 Gy急性60Co γ射线的人血液淋巴细胞,与模拟10%、50%、90%和100%暴露的未照射血液混合,并与均匀暴露于~20 Gy的样品一起,用显微镜定量了染色体畸变。生物剂量学工作量进行统计建模,假设0.5、1、5或25小时可用于评分一个病例,或用于分析多达1000个细胞或100个双中心加中心环。在畸变获取率和细胞记录率之间建立了强烈的负相关。计算表明,每个操作人员每天1例的工作量(5小时显微镜评分)允许对90%-100%的2 Gy照射或50%-90%的4-12 Gy照射进行高精度的剂量估计;12 Gy和20 Gy的致死性均质(100%)暴露仅用1小时显微镜即可评估。每例0.5小时评分的分诊分析结果显示,只有局部和全身暴露在4-20 Gy时,才有最低可容忍的准确性。传统生物剂量测定法的时间相关功效主要取决于样品中的像差率,而像差率又取决于辐射剂量及其在患者体内的分布。应针对每个实验室的不同暴露情况制定优化的显微镜评分计划,以提高其对放射紧急情况的准备。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Optimizing the Microscopy Time Schedule for Chromosomal Dosimetry of High-dose and Partial-body Irradiations.

Optimizing the Microscopy Time Schedule for Chromosomal Dosimetry of High-dose and Partial-body Irradiations.

Optimizing the Microscopy Time Schedule for Chromosomal Dosimetry of High-dose and Partial-body Irradiations.

Optimizing the Microscopy Time Schedule for Chromosomal Dosimetry of High-dose and Partial-body Irradiations.

The methodology of cytogenetic triage can be improved by optimizing a schedule of microscopy for different exposure scenarios. Chromosome aberrations were quantified by microscopy in human blood lymphocytes irradiated in vitro to ~2, 4, and 12 Gy acute 60Co γ-rays mixed with the unirradiated blood simulating 10%, 50%, 90%, and 100% exposure and in along with a sample from a homogeneous exposure to ~20 Gy. Biodosimetry workload was statistically modeled assuming that 0.5, 1, 5, or 25 h was available for scoring one case or for analysis of up to 1000 cells or 100 dicentrics plus centric rings by one operator. A strong negative correlation was established between the rates of aberration acquisition and cell recording. Calculations showed that the workload of 1 case per operator per·day (5 h of scoring by microscopy) allows dose estimates with high accuracy for either 90%-100% irradiations of 2 Gy or 50%-90% irradiations of 4-12 Gy; lethal homogeneous (100%) exposures of 12 and 20 Gy can be evaluated with just 1 h of microscopy. Triage analysis of 0.5 h scoring per case results in the minimum tolerable accuracy only for partial- and total-body exposure of 4-20 Gy. Time-related efficacy of conventional biodosimetry depends primarily on the aberration yield in the sample, which is dependent on the radiation dose and its distribution in the patient's body. An optimized schedule of microscopy scoring should be developed for different exposure scenarios in each laboratory to increase their preparedness to radiological emergencies.

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来源期刊
Genome Integrity
Genome Integrity Biochemistry, Genetics and Molecular Biology-Genetics
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