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新生儿期暴露于临床相关剂量的电离辐射和氯胺酮对成年后认知功能的影响。

Effects on adult cognitive function after neonatal exposure to clinically relevant doses of ionising radiation and ketamine in mice.

机构信息

Department of Environmental Toxicology, Uppsala University, Uppsala, Sweden.

Department of Immunology, Genetics and Pathology, Uppsala University, Uppsala, Sweden.

出版信息

Br J Anaesth. 2018 Mar;120(3):546-554. doi: 10.1016/j.bja.2017.11.099. Epub 2018 Jan 27.

Abstract

BACKGROUND

Radiological methods for screening, diagnostics and therapy are frequently used in healthcare. In infants and children, anaesthesia/sedation is often used in these situations to relieve the patients' perception of stress or pain. Both ionising radiation (IR) and ketamine have been shown to induce developmental neurotoxic effects and this study aimed to identify the combined effects of these in a murine model.

METHODS

Male mice were exposed to a single dose of ketamine (7.5 mg kg body weight) s.c. on postnatal day 10. One hour after ketamine exposure, mice were whole body irradiated with 50-200 mGy gamma radiation (Cs). Behavioural observations were performed at 2, 4 and 5 months of age. At 6 months of age, cerebral cortex and hippocampus tissue were analysed for neuroprotein levels.

RESULTS

Animals co-exposed to IR and ketamine displayed significant (P≤0.01) lack of habituation in the spontaneous behaviour test, when compared with controls and single agent exposed mice. In the Morris Water Maze test, co-exposed animals showed significant (P≤0.05) impaired learning and memory capacity in both the spatial acquisition task and the relearning test compared with controls and single agent exposed mice. Furthermore, in co-exposed mice a significantly (P≤0.05) elevated level of tau protein in cerebral cortex was observed. Single agent exposure did not cause any significant effects on the investigated endpoints.

CONCLUSION

Co-exposure to IR and ketamine can aggravate developmental neurotoxic effects at doses where the single agent exposure does not impact on the measured variables. These findings show that estimation of risk after paediatric low-dose IR exposure, based upon radiation dose alone, may underestimate the consequences for this vulnerable population.

摘要

背景

放射学方法在医疗保健中常用于筛查、诊断和治疗。在婴儿和儿童中,这些情况下常使用麻醉/镇静来减轻患者对压力或疼痛的感知。电离辐射(IR)和氯胺酮已被证明会引起发育神经毒性作用,本研究旨在鉴定这些物质在一种鼠模型中的联合作用。

方法

雄性小鼠在出生后第 10 天接受单次皮下注射氯胺酮(7.5mg/kg 体重)。在氯胺酮暴露 1 小时后,将小鼠全身照射 50-200 mGy γ 射线(Cs)。在 2、4 和 5 个月大时进行行为观察。在 6 个月大时,分析大脑皮质和海马组织中的神经蛋白水平。

结果

与对照组和单剂暴露组相比,共同暴露于 IR 和氯胺酮的动物在自发行为测试中表现出明显(P≤0.01)的缺乏习惯化。在 Morris 水迷宫测试中,共同暴露的动物在空间获得任务和再学习测试中均表现出明显(P≤0.05)的学习和记忆能力受损,与对照组和单剂暴露组相比。此外,在共同暴露的小鼠中,大脑皮质中的 tau 蛋白水平显著(P≤0.05)升高。单剂暴露在研究终点上没有引起任何显著影响。

结论

IR 和氯胺酮的共同暴露会在单剂暴露不会影响测量变量的剂量下加重发育神经毒性作用。这些发现表明,基于辐射剂量单独评估儿科低剂量 IR 暴露后的风险可能会低估该脆弱人群的后果。

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