Jung Garyn L, McDaniel Katherine L, LoPachin Richard M, Geohagen Brian C, Smith Alicia, Huffstickler Mitchell, Herr David W
Center for Public Health and Environmental Assessment, US Environmental Protection Agency, Research Triangle Park, NC 27711, USA.
Professor Emeritus in the Department of Anesthesiology, Albert Einstein College of Medicine, 111 E. 210th St, Bronx, NY 10467, USA.
Neurotoxicology. 2022 May;90:48-61. doi: 10.1016/j.neuro.2022.02.008. Epub 2022 Feb 25.
Neurotoxicants may be widespread in the environment and can produce serious health impacts in the human population. Screening programs that use in vitro methods have generated data for thousands of chemicals. However, these methods often do not evaluate repeated or prolonged exposures, which are required for many neurotoxic outcomes. Additionally, the data produced by such screening methods may not include mechanisms which play critical biological roles necessary for in vivo neurotoxicity. The Hard and Soft Acids and Bases (HSAB) in silico model focuses on chemical structure and electrophilic properties which are important to the formation of protein adducts. A group of structurally diverse chemicals have been evaluated with an in silico screening approach incorporating HSAB parameters. However, the predictions from the expanded chemical space have not been evaluated using in vivo methods. Three chemicals predicted to be cumulative toxicants were selected for in vivo neurotoxicological testing. Adult male Long-Evans rats were treated orally with citronellal (CIT), 3,4-dichloro-1-butene (DCB), or benzyl bromoacetate (BBA) for 8 weeks. Behavioral observations were recorded weekly to assess motor function. Peripheral neurophysiological measurements were derived from nerve excitability (NE) tests which involved compound muscle action potentials (CMAPs) in the tail and foot, and mixed nerve action potentials (MNAPs) in the tail. Compound nerve action potentials (CNAPs) and nerve conduction velocity (NCV) in the tail were also quantified. Peripheral inputs into the central nervous system were examined using somatosensory evoked potentials recorded from the cortex (SEP) and cerebellum (SEP). CIT or BBA did not result in significant alterations to peripheral nerve or somatosensory function. DCB reduced grip-strength and altered peripheral nerve function. The MNAPs required less current to reach 50% amplitude and had a lower calculated rheobase, suggesting increased excitability. Increased CNAP amplitudes and greater NCV were also observed. Novel changes were found in the SEP with an abnormal peak forming in the early portion of the waveforms of treated rats, and decreased latencies and increased amplitudes were observed in SEP recordings. These data contribute to testing an expanded chemical space from an in silico HSAB model for predicting cumulative neurotoxicity and may assist with prioritizing chemicals to protect human health.
神经毒剂可能在环境中广泛存在,并会对人类健康产生严重影响。使用体外方法的筛选项目已生成了数千种化学物质的数据。然而,这些方法通常不评估重复或长期接触情况,而这是许多神经毒性结果所必需的。此外,此类筛选方法产生的数据可能不包括对体内神经毒性起关键生物学作用的机制。软硬酸碱(HSAB)计算机模拟模型关注对蛋白质加合物形成很重要的化学结构和亲电性质。一组结构多样的化学物质已通过纳入HSAB参数的计算机模拟筛选方法进行了评估。然而,来自扩展化学空间的预测尚未使用体内方法进行评估。选择了三种预计为累积性毒剂的化学物质进行体内神经毒理学测试。成年雄性长 Evans 大鼠口服香茅醛(CIT)、3,4-二氯-1-丁烯(DCB)或溴乙酸苄酯(BBA)8周。每周记录行为观察结果以评估运动功能。外周神经生理学测量来自神经兴奋性(NE)测试,该测试涉及尾部和足部的复合肌肉动作电位(CMAP)以及尾部的混合神经动作电位(MNAP)。还对尾部的复合神经动作电位(CNAP)和神经传导速度(NCV)进行了量化。使用从皮质(SEP)和小脑(SEP)记录的体感诱发电位检查进入中枢神经系统的外周输入。CIT 或 BBA 未导致外周神经或体感功能发生显著改变。DCB 降低了握力并改变了外周神经功能。MNAP 达到 50%振幅所需的电流较小,计算出的基强度较低,表明兴奋性增加。还观察到 CNAP 振幅增加和 NCV 增大。在 SEP 中发现了新的变化,在处理大鼠的波形早期形成了异常峰值,并且在 SEP 记录中观察到潜伏期缩短和振幅增加。这些数据有助于测试来自计算机模拟 HSAB 模型的扩展化学空间以预测累积神经毒性,并可能有助于确定保护人类健康的化学物质优先级。
