Selecting the Most Relevant Mouse Strains for Evaluating Radiation-Induced Multiple Tissue Injury after Leg-Shielded Partial-Body Gamma Irradiation.

IF 2.5 3区 医学 Q2 BIOLOGY
Julian D Down, Milton R Cornwall-Brady, Wei Huang, Martina Hurwitz, Scott R Floyd, Omer H Yilmaz
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引用次数: 0

Abstract

Animal studies are needed that best simulate a large-scale, inhomogeneous body exposure after a radiological or nuclear incident and that provides a platform for future development of medical countermeasures. A partial-body irradiation (PBI) model using 137Cs gamma rays with hind limb (tibia) shielding was developed and assessed for the sequalae of radiation injuries to gastrointestinal tract, bone marrow (BM) and lung and among different genetic mouse strains (C57BL/6J, C57L/J, CBA/J and FVB/NJ). In this case, a marginal level of BM shielding (∼2%) provided adequate protection against lethality from infection and hemorrhage and enabled escalation of radiation doses with evaluation of both acute and delayed radiation syndromes. A steep radiation dose-dependent body weight loss was observed over the first 5 days attributed to enteritis with C57BL/6J mice appearing to be the most sensitive strain. Peripheral blood cell analysis revealed significant depression and recovery of leukocytes and platelets over the first month after PBI and were comparable among the four different mouse strains. Latent pulmonary injury was observed on micro-CT imaging at 4 months in C57L/J mice and confirmed histologically as severe pneumonitis that was lethal at 12 Gy. The lethality and radiological densitometry (HUs) dose responses were comparable to previous studies on C57L/J mice after total-body irradiation (TBI) and BM transplant rescue as well as after localized whole-thorax irradiation (WTI). Indeed, the lethal radiation doses and latency appeared similar for pneumonitis appearing in rhesus macaques after WTI or PBI as well as predicted for patients given systemic radiotherapy. In contrast, PBI treatment of C57BL/6 mice at a higher dose of 14 Gy had far longer survival times and developed extreme and debilitating pIeural effusions; an anomaly as similarly reported in previous thorax irradiation studies on this mouse strain. In summary, a radiation exposure model that delivers PBI to unanesthetized mice in a device that provides consistent shielding of the hind limb BM was developed for 137Cs gamma rays with physical characteristics and relevance to relatively high photon energies expected from the detonation of a nuclear device or accidental release of ionizing radiation. Standard strains such as C57BL/6J mice may be used reliably for early GI or hematological radiation syndromes while the C57L/J mouse strain stands out as the most appropriate for evaluating the delayed pulmonary effects of acute radiation exposure and recapitulating this disease in humans.

选择最相关的小鼠品系,用于评估腿部屏蔽部分全身伽马辐照后辐射诱发的多组织损伤。
需要进行动物研究,以最好地模拟辐射或核事件发生后大规模、不均匀的人体辐照,并为未来医疗对策的开发提供一个平台。利用 137Cs γ 射线和后肢(胫骨)屏蔽,建立了一个局部全身辐照(PBI)模型,并对不同基因小鼠品系(C57BL/6J、C57L/J、CBA/J 和 FVB/NJ)的胃肠道、骨髓(BM)和肺部的辐射损伤后果进行了评估。在这种情况下,边际水平的骨髓屏蔽(∼2%)可提供足够的保护,防止感染和出血导致的死亡,并使辐射剂量的升级与急性和延迟辐射综合征的评估成为可能。在最初的 5 天内,观察到了与辐射剂量相关的体重急剧下降,这是由于肠炎引起的,C57BL/6J 小鼠似乎是最敏感的品系。外周血细胞分析表明,PBI 后的第一个月,白细胞和血小板明显减少和恢复,四种不同品系的小鼠具有可比性。C57L/J 小鼠在 4 个月时通过显微 CT 成像观察到潜伏性肺损伤,组织学证实为严重的肺炎,12 Gy 时致死。致死率和放射密度计(HUs)剂量反应与之前对全身辐照(TBI)和骨髓移植救治以及局部全胸辐照(WTI)后的C57L/J小鼠进行的研究结果相当。事实上,猕猴在接受 WTI 或 PBI 治疗后出现肺炎的致死辐射剂量和潜伏期与接受全身放疗的患者的预测相似。与此相反,C57BL/6小鼠在接受14Gy的高剂量PBI治疗后,存活时间更长,并出现极度衰弱的硬膜外积液;这一反常现象在以前对该小鼠品系进行的胸部照射研究中也有类似报道。总之,针对 137Cs γ 射线开发了一种辐照模型,该模型通过一种可持续屏蔽后肢 BM 的装置向未麻醉的小鼠提供 PBI,其物理特性与核装置爆炸或电离辐射意外释放所产生的相对较高的光子能量相关。C57BL/6J 小鼠等标准品系可以可靠地用于早期消化道或血液辐射综合征的研究,而 C57L/J 小鼠品系则最适合用于评估急性辐照对肺部的延迟影响和重现人类的这种疾病。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Radiation research
Radiation research 医学-核医学
CiteScore
5.10
自引率
8.80%
发文量
179
审稿时长
1 months
期刊介绍: Radiation Research publishes original articles dealing with radiation effects and related subjects in the areas of physics, chemistry, biology and medicine, including epidemiology and translational research. The term radiation is used in its broadest sense and includes specifically ionizing radiation and ultraviolet, visible and infrared light as well as microwaves, ultrasound and heat. Effects may be physical, chemical or biological. Related subjects include (but are not limited to) dosimetry methods and instrumentation, isotope techniques and studies with chemical agents contributing to the understanding of radiation effects.
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