Carpenter Jessica M, Brown Kyle A, Veltmaat Lukas, Ludwig Helaina D, Clay Kendall B, Norberg Thomas, Harn Donald A, Wagner John J, Filipov Nikolay M
Department of Physiology and Pharmacology, University of Georgia, Athens, GA, United States.
Neuroscience Program, University of Georgia, Athens, GA, United States.
Brain Behav Immun Health. 2022 Nov 8;26:100553. doi: 10.1016/j.bbih.2022.100553. eCollection 2022 Dec.
Chemical overexposures and war-related stress during the 1990-1991 Gulf War (GW) are implicated in the persisting pathological symptoms that many GW veterans continue to endure. These symptoms culminate into a disease known as Gulf War Illness (GWI) and affect about a third of the GW veteran population. Currently, comprehensive effective GWI treatment options are unavailable. Here, an established GWI mouse model was utilized to explore the (1) long-term behavioral and neuroinflammatory effects of deployment-related GWI chemicals exposure and (2) ability of the immunotherapeutic lacto-N-fucopentaose III (LNFPIII) to improve deficits when given months after the end of exposure. Male C57BL6/J mice (8-9 weeks old) were administered pyridostigmine bromide (PB) and DEET for 14 days along with corticosterone (CORT; latter 7 days) to emulate wartime stress. On day 15, a single injection of the nerve agent surrogate diisopropylfluorophosphate (DFP) was given. LNFPIII treatment began 7 months post GWI chemicals exposure and continued until study completion. A battery of behavioral tests for assessment of cognition/memory, mood, and motor function in rodents was performed beginning 8 months after exposure termination and was then followed by immunohistochemcal evaluation of neuroinflammation and neurogenesis. Within tests of motor function, prior GWI chemical exposure led to hyperactivity, impaired sensorimotor function, and altered gait. LNFPIII attenuated these motor-related deficits and improved overall grip strength. GWI mice also exhibited more anxiety-like behavior that was reduced by LNFPIII; this was test-specific. Short-term, but not long-term memory, was impaired by prior GWI exposure; LNFPIII improved this measure. In the brains of GWI mice, but not in mice treated with LNFPIII, glial activation was increased. Overall, it appears that months after exposure to GWI chemicals, behavioral deficits and neuroinflammation are present. Many of these deficits were attenuated by LNFPIII when treatment began long after GWI chemical exposure termination, highlighting its therapeutic potential for veterans with GWI.
在1990 - 1991年海湾战争(GW)期间,化学物质过度暴露和与战争相关的压力被认为与许多海湾战争退伍军人持续忍受的病理症状有关。这些症状最终发展成一种名为海湾战争综合征(GWI)的疾病,影响了约三分之一的海湾战争退伍军人。目前,尚无全面有效的GWI治疗方案。在此,利用已建立的GWI小鼠模型来探究:(1)与部署相关的GWI化学物质暴露的长期行为和神经炎症影响;(2)免疫治疗性乳糖 - N - 岩藻五糖III(LNFPIII)在暴露结束数月后给予时改善缺陷的能力。将8 - 9周龄的雄性C57BL6/J小鼠用溴化吡啶斯的明(PB)和避蚊胺处理14天,并在最后7天给予皮质酮(CORT)以模拟战时压力。在第15天,单次注射神经毒剂替代物二异丙基氟磷酸酯(DFP)。LNFPIII治疗在GWI化学物质暴露7个月后开始,并持续到研究结束。在暴露终止8个月后,进行了一系列用于评估啮齿动物认知/记忆、情绪和运动功能的行为测试,随后对神经炎症和神经发生进行免疫组织化学评估。在运动功能测试中,先前的GWI化学物质暴露导致多动、感觉运动功能受损和步态改变。LNFPIII减轻了这些与运动相关的缺陷,并提高了整体握力。GWI小鼠还表现出更多的焦虑样行为,而LNFPIII可减少这种行为;这是特定测试的结果。先前的GWI暴露损害了短期记忆,但未损害长期记忆;LNFPIII改善了这一指标。在GWI小鼠的大脑中,而非用LNFPIII处理的小鼠大脑中,神经胶质细胞激活增加。总体而言,在暴露于GWI化学物质数月后,存在行为缺陷和神经炎症。当在GWI化学物质暴露终止很久之后开始治疗时,LNFPIII减轻了许多这些缺陷,突出了其对患有GWI的退伍军人的治疗潜力。
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