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Physiologically Based Pharmacokinetic Model for the Biotransportation of Arsenic in Marine Medaka (Oryzias melastigma)

机译:生理基于基于药代动力学模型的海洋Medaka(Oryzias MelaStigma)生物传播

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摘要

The toxicity of arsenic (As) targets specific tissues of organisms, while the biotransportation of As among the tissues of fish remains poorly understood. In the present study, radiotracer techniques followed by a physiologically based pharmacokinetic (PBPK) modeling were applied to simulate the biotransportation (absorption, distribution, and elimination) of ~(73)As(Ⅴ) and biotransformation of As(Ⅴ) in the marine medaka Oryzias melastigma after waterborne As exposure. Fish were simulated by a six-compartment model by assuming that blood was the intermediate exchange among different compartments (gill, intestine, liver, head, and carcass). Modeling suggested that intestine and gill were the uptake, exchange, as well as elimination sites of waterborne As, while carcass and head were the main storage sites. Intestine played a vital role in the metabolism of As(Ⅴ) by biotransforming inorganic As into arsenobetaine (AsB), possibly because of the important role of gut microbiota. The correlation between the PBPK model constants and the As speciation (e.g., AsB %, inorganic As %, and methylated As %) indicated that AsB tended to be stored in the tissues rather than being depurated, while inorganic and methylated As were more easily transferred from tissues to the blood and eliminated. Modeling simulation coupling with biotransformation for the first time demonstrated that the fish intestine was the main metabolic site, and synthesis of AsB as mediated by the microbiota in the intestine contributed to the high As bioaccumulation in marine fish.
机译:砷(AS)的毒性(AS)靶向有机体的特定组织,而鱼类组织的生物转向仍然明白。在本研究中,应用了放射性物质技术,然后应用了生理基础的药代动力学(PBPK)建模,用于模拟〜(73)和在海军陆战队中(ⅴ)的生物传播(吸收,分布和消除)和生物转化Medaka Oryzias Melastigma水上被淘水后作为曝光。通过假设血液是不同隔室(鳃,肠,肝,头部和尸体)之间的中间交换来模拟六室模型的鱼。建模表明,肠和鳃是吸收,交换,以及水性的消除位点,而胴体和头部是主储存场所。肠道在Byorransformintointo(ASB)中的Biorroalformintaine(ASB)中的代谢作用了至关重要的作用,可能是因为肠道微生物的重要作用。 PBPK模型常数与作为物质(例如,ASB%,无机AS%和甲基化为%)的相关性表明,ASB倾向于储存在组织中而不是被沉积的,而无机和甲基化,则更容易转移从组织到血液并消除。第一次与生物转化建模耦合表明,鱼肠是主要代谢位点,并且由微生物群中的肠道介导的ASB的合成导致海洋鱼类中的生物累积。

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  • 来源
    《Environmental Science & Technology》 |2020年第12期|7485-7493|共9页
  • 作者单位

    Institute of Environmental Research at Greater Bay Area Key Laboratory for Water Quality and Conservation of the Pearl River Delta Ministry of Education Guangzhou University Guangzhou 510006 China Key Laboratory of Tropical Marine Bio-resources and Ecology Guangdong Provincial Key Laboratory of Applied Marine Biology South China Sea Institute of Oceanology Chinese Academy of Sciences Guangzhou 510301 China;

    Key Laboratory of Tropical Marine Bio-resources and Ecology Guangdong Provincial Key Laboratory of Applied Marine Biology South China Sea Institute of Oceanology Chinese Academy of Sciences Guangzhou 510301 China;

    Key Laboratory of the Coastal and Wetland Ecosystems Ministry of Education College of Environment and Ecology Xiamen University Xiamen 361102 P. R China;

    School of Energy and Environment and State Key Laboratory of Marine Pollution City University of Hong Kong Kowloon 999077 Hong Kong;

    Key Laboratory of Tropical Marine Bio-resources and Ecology Guangdong Provincial Key Laboratory of Applied Marine Biology South China Sea Institute of Oceanology Chinese Academy of Sciences Guangzhou 510301 China;

  • 收录信息 美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
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  • 正文语种 eng
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