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轮胎颗粒和抗生素对斑马鱼的毒理学机制和分子影响。

Toxicological mechanisms and molecular impacts of tire particles and antibiotics on zebrafish.

机构信息

College of Environmental Science and Engineering, North China Electric Power University, Beijing, 102206, China; MOE Key Laboratory of Resources and Environmental System Optimization, North China Electric Power University, Beijing, 102206, China.

School of Climate Change and Adaptation, University of Prince Edward Island, Charlottetown, Canada.

出版信息

Environ Pollut. 2024 Dec 1;362:124912. doi: 10.1016/j.envpol.2024.124912. Epub 2024 Sep 7.

Abstract

Tire microplastics (TMPs) and antibiotics are emerging pollutants that widely exist in water environments. The coexistence of these pollutants poses severe threats to aquatic organisms. However, the toxicity characteristics and key molecular factors of the combined exposure to TMPs in aquatic organisms remain unknown. Therefore, the joint toxicity of styrene-butadiene rubber TMPs (SBR-TMPs) and 32 antibiotics (macrolides, fluoroquinolones, β-lactams, sulfonamides, tetracyclines, nitroimidazoles, highly toxic antibiotics, high-content antibiotics, and common antibiotics) in zebrafish was investigated using a full factorial design, molecular docking, and molecular dynamics simulation. Sixty-four combinations of antibiotics were designed to investigate the hepatotoxicity of the coexistence of SBR-TMPs additives and antibiotics in zebrafish. Results indicated that low-order effects of antibiotics (e.g., enoxacin-lomefloxacin and ofloxacin-enoxacin-lomefloxacin) had relatively notable toxicity. The van der Waals interaction between additives and zebrafish cytochrome P450 enzymes primarily affected zebrafish hepatotoxicity. Zebrafish hepatotoxicity was also affected by the ability of SBR-TMPs to adsorb antibiotics, the relation between antibiotics, the affinity of antibiotics docking to zebrafish cytochrome P450 enzymes, electronegativity, atomic mass, and the hydrophobicity of the antibiotic molecules. This study aimed to eliminate the joint toxicity of TMPs and antibiotics and provide more environmentally friendly instructions for using different chemicals.

摘要

轮胎微塑料(TMPs)和抗生素是新兴的污染物,广泛存在于水环境中。这些污染物的共存对水生生物构成了严重威胁。然而,TMPs 在水生生物中联合暴露的毒性特征和关键分子因素尚不清楚。因此,采用完全因子设计、分子对接和分子动力学模拟的方法,研究了苯乙烯-丁二烯橡胶 TMPs(SBR-TMPs)和 32 种抗生素(大环内酯类、氟喹诺酮类、β-内酰胺类、磺胺类、四环素类、硝基咪唑类、高毒性抗生素、高含量抗生素和常见抗生素)对斑马鱼的联合毒性。设计了 64 种抗生素组合,以研究 SBR-TMPs 添加剂和抗生素共存对斑马鱼的肝毒性。结果表明,抗生素的低阶效应(如恩诺沙星-洛美沙星和氧氟沙星-恩诺沙星-洛美沙星)具有相对显著的毒性。添加剂和斑马鱼细胞色素 P450 酶之间的范德华相互作用主要影响斑马鱼的肝毒性。SBR-TMPs 吸附抗生素的能力、抗生素之间的关系、抗生素与斑马鱼细胞色素 P450 酶的结合亲和力、电负性、原子质量和抗生素分子的疏水性也会影响斑马鱼的肝毒性。本研究旨在消除 TMPs 和抗生素的联合毒性,并为使用不同化学品提供更环保的指导。

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