Flunitrazepam and its metabolites induced brain toxicity: Insights from molecular dynamics simulation and transcriptomic analysis

IF 12.2 1区环境科学与生态学 Q1 ENGINEERING, ENVIRONMENTAL

Journal of Hazardous Materials Pub Date : 2023-11-29 DOI:10.1016/j.jhazmat.2023.133113

Wenting Lin , Yingjun Qin , Yuan Ren

{"title":"Flunitrazepam and its metabolites induced brain toxicity: Insights from molecular dynamics simulation and transcriptomic analysis","authors":"Wenting Lin , Yingjun Qin , Yuan Ren","doi":"10.1016/j.jhazmat.2023.133113","DOIUrl":null,"url":null,"abstract":"<div><p>Psychoactive drugs frequently contaminate aquatic environments after human consumption, raising concerns about their residues and ecological harm. This study investigates the effects of flunitrazepam (FLZ) and its metabolite 7-aminoflunitrazepam (7-FLZ), benzodiazepine-class psychoactive drugs, on brain accumulation, blood-brain barrier (BBB), and neuroinflammation of the model organism zebrafish. Molecular dynamics simulation and transcriptome sequencing were used to uncover their toxic mechanisms. Results demonstrate that both FLZ and 7-FLZ can accumulate in the brain, increasing Evans blue levels by 3.4 and 0.8 times, respectively. This increase results from abnormal expression of tight junction proteins, particularly <em>ZO-1</em> and <em>Occludin</em>, leading to elevated BBB permeability. Furthermore, FLZ and 7-FLZ can also induce neuroinflammation, upregulating <em>TNFα</em><span> by 91% and 39%, respectively, leading to pathological changes and disrupted intracellular ion balance. Molecular dynamics simulation reveals conformational changes in ZO-1 and Occludin proteins, with FLZ exhibiting stronger binding forces and greater toxicity. Weighted gene co-expression network analysis identifies four modules correlated with BBB permeability and neuroinflammation. KEGG enrichment analysis of genes within these modules reveals pathways like protein processing in the endoplasmic reticulum, NOD-like receptor signaling pathway, and arginine and proline metabolism. This study enhances understanding of FLZ and 7-FLZ neurotoxicity and assesses environmental risks of psychoactive substances.</span></p></div><div><h3>Environmental Implication</h3><p>With the increasing prevalence of mental disorders and the discharge of psychoactive drugs into water, even low drug concentrations (ng/L-μg/L) can pose neurological risks. This study, utilizing molecular dynamic (MD) simulations and transcriptome sequencing, investigate the neurotoxicity and mechanisms of flunitrazepam and 7-aminoflunitrazepam. It reveals that they disrupt the blood-brain barrier in zebrafish and induce neuroinflammation primarily by inducing conformational changes in tight junction proteins. MD simulations are valuable for understanding pollutant-protein interactions. This research offers invaluable insights for the environmental risk assessment of psychoactive drugs and informs the development of strategies aimed at prevention and mitigation.</p></div>","PeriodicalId":361,"journal":{"name":"Journal of Hazardous Materials","volume":"465 ","pages":"Article 133113"},"PeriodicalIF":12.2000,"publicationDate":"2023-11-29","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":null,"platform":"Semanticscholar","paperid":null,"PeriodicalName":"Journal of Hazardous Materials","FirstCategoryId":"93","ListUrlMain":"https://www.sciencedirect.com/science/article/pii/S030438942302397X","RegionNum":1,"RegionCategory":"环境科学与生态学","ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"","PubModel":"","JCR":"Q1","JCRName":"ENGINEERING, ENVIRONMENTAL","Score":null,"Total":0}

引用次数: 0

Abstract

Psychoactive drugs frequently contaminate aquatic environments after human consumption, raising concerns about their residues and ecological harm. This study investigates the effects of flunitrazepam (FLZ) and its metabolite 7-aminoflunitrazepam (7-FLZ), benzodiazepine-class psychoactive drugs, on brain accumulation, blood-brain barrier (BBB), and neuroinflammation of the model organism zebrafish. Molecular dynamics simulation and transcriptome sequencing were used to uncover their toxic mechanisms. Results demonstrate that both FLZ and 7-FLZ can accumulate in the brain, increasing Evans blue levels by 3.4 and 0.8 times, respectively. This increase results from abnormal expression of tight junction proteins, particularly ZO-1 and Occludin, leading to elevated BBB permeability. Furthermore, FLZ and 7-FLZ can also induce neuroinflammation, upregulating TNFα by 91% and 39%, respectively, leading to pathological changes and disrupted intracellular ion balance. Molecular dynamics simulation reveals conformational changes in ZO-1 and Occludin proteins, with FLZ exhibiting stronger binding forces and greater toxicity. Weighted gene co-expression network analysis identifies four modules correlated with BBB permeability and neuroinflammation. KEGG enrichment analysis of genes within these modules reveals pathways like protein processing in the endoplasmic reticulum, NOD-like receptor signaling pathway, and arginine and proline metabolism. This study enhances understanding of FLZ and 7-FLZ neurotoxicity and assesses environmental risks of psychoactive substances.

Environmental Implication

With the increasing prevalence of mental disorders and the discharge of psychoactive drugs into water, even low drug concentrations (ng/L-μg/L) can pose neurological risks. This study, utilizing molecular dynamic (MD) simulations and transcriptome sequencing, investigate the neurotoxicity and mechanisms of flunitrazepam and 7-aminoflunitrazepam. It reveals that they disrupt the blood-brain barrier in zebrafish and induce neuroinflammation primarily by inducing conformational changes in tight junction proteins. MD simulations are valuable for understanding pollutant-protein interactions. This research offers invaluable insights for the environmental risk assessment of psychoactive drugs and informs the development of strategies aimed at prevention and mitigation.

Abstract Image

查看原文本刊更多论文

氟硝西泮及其代谢物诱导脑毒性:来自分子动力学模拟和转录组学分析的见解

精神活性药物在人类食用后经常污染水生环境，引起人们对其残留和生态危害的关注。本研究探讨氟硝西泮(FLZ)及其代谢物7-氨基氟硝西泮(7-FLZ)对模式生物斑马鱼脑蓄积、血脑屏障(BBB)和神经炎症的影响。分子动力学模拟和转录组测序揭示了它们的毒性机制。结果表明，FLZ和7-FLZ均可在脑内积累，使埃文斯蓝水平分别提高3.4倍和0.8倍。这种增加是由于紧密连接蛋白的异常表达，特别是ZO-1和Occludin，导致血脑屏障通透性升高。此外，FLZ和7-FLZ还能诱导神经炎症，使TNFα分别上调91%和39%，导致病理改变，破坏细胞内离子平衡。分子动力学模拟显示，ZO-1和Occludin蛋白的构象发生了变化，FLZ表现出更强的结合力和更大的毒性。加权基因共表达网络分析确定了与血脑屏障通透性和神经炎症相关的四个模块。对这些模块内基因的KEGG富集分析揭示了内质网蛋白质加工、nod样受体信号通路以及精氨酸和脯氨酸代谢等途径。本研究提高了对FLZ和7-FLZ神经毒性的认识，并评估了精神活性物质的环境风险。随着精神疾病的日益流行和精神活性药物排放到水中，即使是低浓度(ng/L-μg/L)的药物也可能造成神经系统风险。本研究利用分子动力学(MD)模拟和转录组测序研究氟硝西泮和7-氨基氟硝西泮的神经毒性及其机制。研究表明，它们主要通过诱导紧密连接蛋白的构象改变来破坏斑马鱼的血脑屏障并诱导神经炎症。MD模拟对于理解污染物与蛋白质的相互作用很有价值。这项研究为精神活性药物的环境风险评估提供了宝贵的见解，并为制定预防和减轻风险的战略提供了信息。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

求助全文

约1分钟内获得全文求助全文

来源期刊

Journal of Hazardous Materials 工程技术-工程：环境

CiteScore

25.40

自引率

5.90%

发文量

3059

审稿时长

58 days

期刊介绍： The Journal of Hazardous Materials serves as a global platform for promoting cutting-edge research in the field of Environmental Science and Engineering. Our publication features a wide range of articles, including full-length research papers, review articles, and perspectives, with the aim of enhancing our understanding of the dangers and risks associated with various materials concerning public health and the environment. It is important to note that the term "environmental contaminants" refers specifically to substances that pose hazardous effects through contamination, while excluding those that do not have such impacts on the environment or human health. Moreover, we emphasize the distinction between wastes and hazardous materials in order to provide further clarity on the scope of the journal. We have a keen interest in exploring specific compounds and microbial agents that have adverse effects on the environment.