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暴露后生物样本中神经毒剂生物标志物回顾性鉴定的当前进展

Current Progress for Retrospective Identification of Nerve Agent Biomarkers in Biological Samples after Exposure.

作者信息

Wang Jin, Lu Xiaogang, Gao Runli, Pei Chengxin, Wang Hongmei

机构信息

State Key Laboratory of NBC Protection for Civilian, Beijing 102205, China.

出版信息

Toxics. 2022 Aug 1;10(8):439. doi: 10.3390/toxics10080439.

Abstract

Organophosphorus neurotoxic agents (OPNAs) seriously damage the nervous system, inhibiting AChE activity and threatening human health and life. Timely and accurate detection of biomarkers in biomedical samples is an important means for identifying OPNA exposure, helping to recognize and clarify its characteristics and providing unambiguous forensic evidence for retrospective research. It is therefore necessary to summarize the varieties of biomarkers, recognize their various characteristics, and understand the principal research methods for these biomarkers in the retrospective detection of OPNA exposure. Common biomarkers include mainly intact agents, degradation products and protein adducts. Direct agent identification in basic experimental research was successfully applied to the detection of free OPNAs, however, this method is not applicable to actual biomedical samples because the high reactivity of OPNAs promotes rapid metabolism. Stepwise degradation products are important targets for retrospective research and are usually analyzed using a GC-MS, or an LC-MS system after derivatization. The smaller window of detection time requires that sampling be accomplished within 48 h, increasing the obstacles to determining OPNA exposure. For this reason, the focus of retrospective identification of OPNA exposure has shifted to protein adducts with a longer lifetime. Compared to the fluoride-induced reactivation method, which cannot be used for aged adducts, digestive peptide analysis is the more elegant method for detecting various adducts, identifying more active sites, exploring potential biomarkers and excavating characteristic ions. Retrospective identification of biomarkers after OPNA poisoning is of primary importance, providing unambiguous evidence for forensic analysis in actual cases and judgment of chemical accidents. At present, degradation products, the nonapeptide from BChE adducts and Y411 from human serum adducts are used successfully in actual cases of OPNA exposure. However, more potential biomarkers are still in the discovery stage, which may prove inconclusive. Therefore, there is an urgent need for research that screens biomarker candidates with high reactivity and good reliability from the potential candidates. In addition, mass spectrometry detection with high resolution and reactivity and an accurate data processing system in the scanning mode must also be further improved for the retrospective identification of unknown agents.

摘要

有机磷神经毒剂(OPNAs)严重损害神经系统,抑制乙酰胆碱酯酶(AChE)活性,威胁人类健康和生命。及时、准确地检测生物医学样本中的生物标志物是识别OPNA暴露的重要手段,有助于认识和阐明其特征,并为回顾性研究提供明确的法医证据。因此,有必要总结生物标志物的种类,认识其各种特征,并了解这些生物标志物在OPNA暴露回顾性检测中的主要研究方法。常见的生物标志物主要包括完整的毒剂、降解产物和蛋白质加合物。在基础实验研究中,直接鉴定毒剂成功应用于游离OPNAs的检测,然而,由于OPNAs的高反应性促进了快速代谢,这种方法不适用于实际的生物医学样本。逐步降解产物是回顾性研究的重要目标,通常在衍生化后使用气相色谱-质谱联用仪(GC-MS)或液相色谱-质谱联用仪(LC-MS)系统进行分析。检测时间窗口较小,要求在48小时内完成采样,这增加了确定OPNA暴露的障碍。因此,OPNA暴露回顾性鉴定的重点已转向寿命更长的蛋白质加合物。与不能用于老化加合物的氟化物诱导再活化方法相比,消化肽分析是检测各种加合物、识别更多活性位点、探索潜在生物标志物和挖掘特征离子的更优方法。OPNA中毒后生物标志物的回顾性鉴定至关重要,为实际案件的法医分析和化学事故的判断提供明确证据。目前,降解产物、丁酰胆碱酯酶(BChE)加合物中的九肽和人血清加合物中的Y411已成功应用于OPNA暴露的实际案例中。然而,更多潜在的生物标志物仍处于发现阶段,可能尚无定论。因此,迫切需要开展相关研究,从潜在候选物中筛选出具有高反应性和良好可靠性的生物标志物候选物。此外,还必须进一步改进具有高分辨率和反应性的质谱检测以及扫描模式下准确的数据处理系统,以用于未知毒剂的回顾性鉴定。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fa17/9416412/5131dc46377e/toxics-10-00439-g001.jpg

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