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非人类灵长类动物的急性辐射综合征:7.2 Gy 全身照射后全球血清代谢组学研究的结果。

Nonhuman Primates with Acute Radiation Syndrome: Results from a Global Serum Metabolomics Study after 7.2 Gy Total-Body Irradiation.

机构信息

Departments of Oncology.

Biochemistry and Molecular & Cellular Biology, Georgetown University Medical Center, Washington, DC.

出版信息

Radiat Res. 2018 Dec;190(6):576-583. doi: 10.1667/RR15167.1. Epub 2018 Sep 5.

Abstract

Threats of nuclear terrorism coupled with potential unintentional ionizing radiation exposures have necessitated the need for large-scale response efforts of such events, including high-throughput biodosimetry for medical triage. Global metabolomics utilizing mass spectrometry (MS) platforms has proven an ideal tool for generating large compound databases with relative quantification and structural information in a short amount of time. Determining metabolite panels for biodosimetry requires experimentation to evaluate the many factors associated with compound concentrations in biofluids after radiation exposures, including temporal changes, pre-existing conditions, dietary intake, partial- vs. total-body irradiation (TBI), among others. Here, we utilize a nonhuman primate (NHP) model and identify metabolites perturbed in serum after 7.2 Gy TBI without supportive care [LD, hematologic (hematopoietic) acute radiation syndrome (HARS) level H3] at 24, 36, 48 and 96 h compared to preirradiation samples with an ultra-performance liquid chromatography quadrupole time-of-flight (UPLC-QTOF) MS platform. Additionally, we document changes in cytokine levels. Temporal changes observed in serum carnitine, acylcarnitines, amino acids, lipids, deaminated purines and increases in pro-inflammatory cytokines indicate clear metabolic dysfunction after radiation exposure. Multivariate data analysis shows distinct separation from preirradiation groups and receiver operator characteristic curve analysis indicates high specificity and sensitivity based on area under the curve at all time points after 7.2 Gy irradiation. Finally, a comparison to a 6.5 Gy (LD, HARS level H2) cohort after 24 h postirradiation revealed distinctly increased separations from the 7.2 Gy cohort based on multivariate data models and higher compound fold changes. These results highlight the utility of MS platforms to differentiate time and absorbed dose after a potential radiation exposure that may aid in assigning specific medical interventions and contribute as additional biodosimetry tools.

摘要

核恐怖主义的威胁加上潜在的非故意电离辐射暴露,使得此类事件需要进行大规模的应对工作,包括用于医疗分诊的高通量生物剂量测定。利用质谱 (MS) 平台进行的全球代谢组学已被证明是一种理想的工具,可在短时间内生成具有相对定量和结构信息的大型化合物数据库。确定生物剂量测定的代谢物组需要进行实验,以评估与辐射暴露后生物流体中化合物浓度相关的许多因素,包括时间变化、预先存在的条件、饮食摄入、局部与全身照射 (TBI) 等。在这里,我们利用非人类灵长类动物 (NHP) 模型,并在没有支持性护理的情况下,确定了 TBI 后 7.2 Gy 时血清中受到干扰的代谢物[LD,血液学(造血)急性辐射综合征 (HARS) 水平 H3],与照射前样本相比,在 24、36、48 和 96 小时使用超高效液相色谱四极杆飞行时间 (UPLC-QTOF) MS 平台。此外,我们记录了细胞因子水平的变化。血清肉碱、酰基肉碱、氨基酸、脂质、脱氨基嘌呤和促炎细胞因子水平的时间变化表明辐射暴露后明显存在代谢功能障碍。多元数据分析显示与照射前组明显分离,基于曲线下面积的接收器操作特征曲线分析表明,在 7.2 Gy 照射后所有时间点均具有高特异性和敏感性。最后,与照射后 24 小时的 6.5 Gy(LD,HARS 水平 H2)队列进行比较,基于多元数据分析模型,发现与 7.2 Gy 队列的分离明显增加,化合物倍数变化更高。这些结果突出了 MS 平台在潜在辐射暴露后区分时间和吸收剂量的效用,这可能有助于指定特定的医疗干预措施,并作为额外的生物剂量测定工具做出贡献。

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