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裂化可卡因对贻贝 Perna perna 的解毒、氧化应激和细胞遗传毒性。

Detoxification, oxidative stress, and cytogenotoxicity of crack cocaine in the brown mussel Perna perna.

机构信息

Departamento de Ciências do Mar, Universidade Federal de São Paulo, Rua Maria Máximo, 168, Santos, 11030-100, Brazil.

Laboratório de Ecotoxicologia, Universidade Santa Cecília, Rua Oswaldo Cruz 266, Santos, 11045-907, Brazil.

出版信息

Environ Sci Pollut Res Int. 2019 Sep;26(27):27569-27578. doi: 10.1007/s11356-018-1600-7. Epub 2018 Mar 8.

Abstract

The presence of cocaine and its metabolites and by-products has been identified in different aquatic matrices, making crack cocaine the target of recent studies. The aim of this study was to evaluate the sublethal effects of crack on the brown mussel Perna perna. Mussels were exposed to three concentrations of crack cocaine (0.5, 5.0, and 50.0 μg L) for 168 h. Gills, digestive glands, and hemolymph were extracted and analyzed after three different exposure times using a suite of biomarkers (EROD, DBF, GST, GPX, LPO, DNA damage, ChE, and lysosomal membrane stability [LMS]). After 48 and 96 h of exposure, EROD, DBF, GST, GPX activities and DNA strand breaks in the gills increased significantly after 48 and 96 h of exposure. Alterations in LMS were also observed in the mussels exposed to all crack concentrations after 96 and 168 h. Our results demonstrated that crack cocaine is metabolized by CYP-like and GST activities in the gills. GPX was not able to prevent primary genetic damage, and cytotoxic effects in the hemocytes were also observed in a dose- and time-dependent response. Our study shows that the introduction of illicit drugs into coastal ecosystems must be considered a threat to marine organisms.

摘要

可卡因及其代谢物和副产物已在不同的水生基质中被发现,这使得快克可卡因成为最近研究的目标。本研究旨在评估快克可卡因对贻贝(Perna perna)的亚致死效应。贻贝在 0.5、5.0 和 50.0μg/L 三种浓度的快克可卡因中暴露 168 小时。在三个不同的暴露时间后,使用一系列生物标志物(EROD、DBF、GST、GPX、LPO、DNA 损伤、ChE 和溶酶体膜稳定性 [LMS])提取和分析了贻贝的鳃、消化腺和血淋巴。暴露 48 和 96 小时后,贻贝鳃中的 EROD、DBF、GST 和 GPX 活性以及 DNA 链断裂在暴露 48 和 96 小时后显著增加。在暴露 96 和 168 小时后,所有快克浓度暴露的贻贝的 LMS 也发生了改变。我们的结果表明,快克可卡因在贻贝的鳃中被 CYP 样和 GST 活性代谢。GPX 未能预防原发性遗传损伤,并且在血细胞中也观察到了时间和剂量依赖性的细胞毒性效应。我们的研究表明,将非法药物引入沿海生态系统必须被视为对海洋生物的威胁。

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