锌是接触铝的工人认知功能受损的 ROCK1 通路介质:一项临床和动物研究

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC
ACS Applied Electronic Materials Pub Date : 2024-12-01 Epub Date: 2024-02-26 DOI:10.1007/s12011-024-04119-2
Nan Shang, Xianlin Li, Lan Zhang, ShanShan Wang, Chanting He, Ling Zhang, Qiao Niu, Xiaojun Zheng
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引用次数: 0

摘要

铝(Al)暴露与神经退行性疾病和认知障碍有关,然而锌(Zn)在铝诱导的轻度认知障碍(MCI)中的参与及其机制仍鲜为人知。本研究旨在探讨锌在铝诱导的认知障碍中的作用及其潜在机制。研究人员收集了蒙特利尔认知评估(MoCA)测试得分以及铝业工人血清中的铝、锌含量。进行了中介分析,以评估血清锌在血清铝和 MoCA 测试分数之间的作用。随后,对大鼠模型进行了铝暴露研究,分为对照组、低剂量组、中等剂量组和高浓度组。在进行了莫里斯水迷宫测试和海马中铝、锌含量检测后,对对照组和高剂量组进行了转录组学和蛋白质组学综合分析,以确定差异表达基因(DEPs)、蛋白质(DEPs)和通路。为了证实这些发现,研究人员选择了实时定量聚合酶链反应(qRT-PCR)和免疫印迹(WB)来确定基因和蛋白质的表达结果。锌总体上调解了血清铝与认知功能之间的关系(调解效应为 17.82%,效应值 = - 0.0351)。在暴露于铝的大鼠模型中,高剂量组与对照组之间共鉴定出 734 个 DEGs、18 个 miRNAs、35 个 lncRNAs、64 个 circRNAs 和 113 个 DEPs。其中,ROCK1、DMD和其他4个DEPs被鉴定为与锌指蛋白(ZNF)有关。京都基因与基因组百科全书(KEGG)和基因本体(GO)的共富集分析将这些变化与 RHOA/ROCK1 信号轴联系起来。高剂量组的 ZNF 相关蛋白 Rock1、DMD 和 DHX57 下调(p = 0.006、0.003、0.04),Myl9、Rhoa、miR431 和 miR182 的表达也下调(p = 0.003、0.032、0.032 和 0.046)。这些发现还表明,海马中的 Al、Zn 水平、水迷宫表现与 Myl9、Rhoa、miR431、miR182、DMD、ROCK1 和 DHX57 的表达之间存在负相关和正相关。根据研究结果,我们确定锌参与了铝工人和铝暴露大鼠模型的铝诱导 MCI。miR431、miR182调控RHOA/ROCK1是锌参与铝诱导认知障碍的途径之一。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Zinc as a Mediator Through the ROCK1 Pathway of Cognitive Impairment in Aluminum-Exposed Workers: A Clinical and Animal Study.

Aluminum (Al) exposure was implicated in neurodegenerative diseases and cognitive impairment, yet the involvement of zinc (Zn) and its mechanism in Al-induced mild cognitive impairment (MCI) remains poorly understood. The objective is to explore the role of Zn in Al-induced cognitive impairment and its potential mechanisms. Montreal cognitive assessment (MoCA) test scores and serum Al, Zn from Al industry workers were collected. A mediation analysis was performed to evaluate the role of serum Zn among serum Al and MoCA test scores. Subsequently, an Al-exposure study was conducted on a rat model categorized into control, low-, medium-, and high-dose groups. After a Morris Water Maze test and detection of Al, Zn content in the hippocampus, integrated transcriptomic and proteomic analyses between the control group and the high-dose group were performed to identify the differentially expressed genes (DEPs), proteins (DEPs), and pathways. To corroborate these findings, quantitative real-time polymerase chain reaction (qRT-PCR) and western blotting (WB) were selected to identify the gene and protein results. Zn overall mediates the relationship between serum Al and cognitive function (mediation effect 17.82%, effect value =  - 0.0351). In the Al-exposed rat model, 734 DEGs, 18 miRNAs, 35 lncRNAs, 64 circRNAs, and 113 DEPs were identified between the high-dose group and the control group. Among them, ROCK1, DMD, and other four DEPs were identified as related to zinc finger proteins (ZNF). Co-enrichment analyses of the Kyoto Encyclopedia of Genes and Genomes (KEGG) and Gene Ontology (GO) linked these changes to the RHOA/ROCK1 signaling axis. ZNF-related proteins Rock1, DMD, and DHX57 in the high-dose group were downregulated (p = 0.006, 0.003, 0.04), and the expression of Myl9, Rhoa, miR431, and miR182 was also downregulated (p = 0.003, 0.032, 0.032, and 0.046). These findings also show correlations between Al, Zn levels in the hippocampus, water maze performance, and expressions of Myl9, Rhoa, miR431, miR182, DMD, ROCK1, and DHX57, with both negative and positive associations. Based on the results, we determined that Zn was involved in Al-induced MCI in Al workers and Al-exposed rat models. Al exposure and interaction with Zn could trigger the downregulation of ZNF of ROCK1, DMD, and DHX57. miR431, miR182 regulate RHOA/ROCK1 was one of the Zn-involved pathways in Al-induced cognitive impairment.

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