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在珍宝蟹中研究软骨藻酸的毒代动力学:深入了解调控生物蓄积机制的新见解。

Domoic acid toxicokinetics in Dungeness crabs: new insights into mechanisms that regulate bioaccumulation.

机构信息

Battelle Pacific NW Division-Marine Sciences Lab, 1529 West Sequim Bay Rd, Sequim, WA 98382, USA.

出版信息

Aquat Toxicol. 2013 Sep 15;140-141:77-88. doi: 10.1016/j.aquatox.2013.04.011. Epub 2013 May 1.

DOI:10.1016/j.aquatox.2013.04.011
PMID:23765030
Abstract

Domoic acid (DA) is an excitatory neurotoxic amino acid produced by several marine algal species and is the causative agent of amnesic shellfish poisoning. Profound differences in the toxicokinetics of DA have been identified in a wide variety of shellfish. We characterized the toxicokinetics of DA in Dungeness crabs (Metacarcinus magister) after oral and intravascular dosing (IV) using a variety of doses ranging from 0.1 to 20mg/kg. After a 1mg/kg oral dose, DA disappeared from the foregut within 2h and largely accumulated in the hepatopancreas, with hemolymph and other tissues having 100-1000 times lower concentrations. After IV dosing, hemolymph concentrations of DA were unexpectedly high and toxicokinetic analysis indicated the steady-state volume of distribution (Vss) was 123-197 ml/kg, which is well below the hemolymph volume of 350 ml/kg for crabs. This indicated only limited extravascular distribution of DA was occurring after IV injection, which is surprising considering the capacity of the hepatopancreas to sequester DA after oral dosing. Additional studies measured the partitioning of DA in hepatopancreas cellular and subcellular fractions. The subcellular distribution of DA was primarily associated with the S8 fraction and could be filtered through a 30,000 MW cut-off filter, indicating DA was not appreciably bound to macromolecules. Interestingly, very little (<0.4%) of the total hepatopancreas DA tissue content was associated with the cellular fraction isolated after dissociation and separation from tissue fragments. The in vivo and in vitro results led us to hypothesize that DA uptake and distribution is regulated by crustacean orthologs of ATP-binding cassette (ABC) type transporters. We tested this hypothesis by co-exposing crabs to DA and known inhibitors of ABC transporters (verapamil, cyclosporine A and MK-571) and through in vitro studies using isolated hepatopancreas tissue and mixed cell suspensions prepared from hepatopancreas tissue. The in vivo results were inconclusive in that the toxicokinetics of DA was not consistently altered by co-administration of the inhibitors. Two exceptions were MK-571, which significantly increased the total body clearance of DA and co-administration of verapamil, which significantly increased the hepatopancreas tissue content of DA 24h after IV injection. Isolated pieces of hepatopancreas tissue were able to readily absorb DA from incubation media, but mixed cell suspensions did not. The absorption of DA or lack thereof was largely unaffected by co-incubation with verapamil although cell suspensions appeared to accumulate small quantities of DA in the presence of verapamil. Collectively, the results of this study suggest DA accumulates in the extracellular spaces of the hepatopancreas, such as the tubular lumen. Under natural circumstances, crabs feeding on contaminated shellfish would be expected to readily absorb DA, which is then stored and slowly eliminated in urine. If the DA exposure level exceeds the storage capacity of the tissue (as occurred with the 20mg/kg dose), breakthrough occurs resulting in much higher systemic exposure and potential for DA toxicity.

摘要

软骨藻酸(DA)是一种兴奋性神经毒素氨基酸,由几种海洋藻类产生,是记忆障碍性贝类中毒的致病因子。在各种贝类中,软骨藻酸的毒代动力学存在明显差异。我们通过口服和血管内给药(IV)的方式,用从 0.1 到 20mg/kg 的各种剂量对 Dungeness 蟹(Metacarcinus magister)进行了软骨藻酸的毒代动力学研究。口服 1mg/kg 剂量后,软骨藻酸在前肠中 2 小时内消失,并主要积累在肝胰腺中,而血淋巴和其他组织的浓度低 100-1000 倍。静脉注射后,血淋巴中的软骨藻酸浓度出人意料地高,毒代动力学分析表明,稳态分布容积(Vss)为 123-197ml/kg,远低于蟹的 350ml/kg 的血淋巴量。这表明,与口服给药后肝胰腺对软骨藻酸的蓄积能力相比,IV 注射后仅发生有限的血管外分布。考虑到这一点,这令人惊讶。进一步的研究测量了肝胰腺细胞和亚细胞部分中软骨藻酸的分配。软骨藻酸的亚细胞分布主要与 S8 部分相关,并且可以通过 30,000MW 的截止过滤器过滤,这表明软骨藻酸与大分子没有明显结合。有趣的是,肝胰腺组织中软骨藻酸的总含量只有很少一部分(<0.4%)与从组织碎片中分离和分离后分离的细胞部分相关。体内和体外的结果使我们假设软骨藻酸的摄取和分布受甲壳类动物 ABC 型转运蛋白的同源物调节。我们通过将螃蟹暴露于软骨藻酸和已知的 ABC 转运蛋白抑制剂(维拉帕米、环孢菌素 A 和 MK-571),以及使用分离的肝胰腺组织和从肝胰腺组织制备的混合细胞悬浮液进行的体外研究来测试这一假设。体内结果不确定,因为抑制剂的共同给药并没有一致改变软骨藻酸的毒代动力学。两个例外是 MK-571,它显著增加了 DA 的全身清除率,而维拉帕米的共同给药则在 IV 注射后 24 小时显著增加了肝胰腺组织中的 DA 含量。从孵育介质中,肝胰腺组织的切片能够轻易地吸收 DA,但混合细胞悬浮液则不能。维拉帕米的共同孵育对 DA 的吸收或缺乏吸收影响不大,尽管细胞悬浮液在维拉帕米存在的情况下似乎在体内积累了少量的 DA。总的来说,这项研究的结果表明,软骨藻酸在肝胰腺的细胞外空间(如管状腔)中积累。在自然情况下,食用受污染贝类的螃蟹会很容易吸收软骨藻酸,然后在尿液中储存并缓慢排出。如果 DA 的暴露水平超过组织的储存能力(如 20mg/kg 剂量),则会出现突破,导致全身暴露水平显著升高,并可能发生 DA 毒性。

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