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鉴定贻贝(贻贝)中的 21,22-脱水azaspiracids 和azaspiracid-26 的体外毒性

Identification of 21,22-Dehydroazaspiracids in Mussels ( Mytilus edulis) and in Vitro Toxicity of Azaspiracid-26.

机构信息

Marine Institute , Rinville, Oranmore , Co. Galway H91 R673 , Ireland.

Measurement Science and Standards , National Research Council Canada , Halifax , NS B3H 3Z1 , Canada.

出版信息

J Nat Prod. 2018 Apr 27;81(4):885-893. doi: 10.1021/acs.jnatprod.7b00973. Epub 2018 Feb 28.

Abstract

Azaspiracids (AZAs) are marine biotoxins produced by the genera Azadinium and Amphidoma, pelagic marine dinoflagellates that may accumulate in shellfish resulting in human illness following consumption. The complexity of these toxins has been well documented, with more than 40 structural variants reported that are produced by dinoflagellates, result from metabolism in shellfish, or are extraction artifacts. Approximately 34 μg of a new AZA with MW 823 Da (AZA26 (3)) was isolated from blue mussels ( Mytilus edulis), and its structure determined by MS and NMR spectroscopy. AZA26, possibly a bioconversion product of AZA5, lacked the C-20-C-21 diol present in all AZAs reported thus far and had a 21,22-olefin and a keto group at C-23. Toxicological assessment of 3 using an in vitro model system based on Jurkat T lymphocyte cells showed the potency to be ∼30-fold lower than that of AZA1. The corresponding 21,22-dehydro-23-oxo-analogue of AZA10 (AZA28) and 21,22-dehydro analogues of AZA3, -4, -5, -6, -9, and -10 (AZA25, -48 (4), -60, -27, -49, and -61, respectively) were also identified by HRMS/MS, periodate cleavage reactivity, conversion from known analogues, and NMR (for 4 that was present in a partially purified sample of AZA7).

摘要

azaspiracids (AZAs) 是由 azadinium 和 amphidoma 属产生的海洋生物毒素,这些浮游海洋甲藻可能在贝类中积累,导致人类食用后患病。这些毒素的复杂性已有充分记录,已报告了 40 多种结构变体,这些变体由甲藻产生,来自贝类的代谢,或为提取的人工产物。从贻贝( Mytilus edulis )中分离到一种新的 MW 823 Da 的 AZA(AZA26(3)),约 34 μg,其结构通过 MS 和 NMR 光谱确定。AZA26 可能是 AZA5 的生物转化产物,缺乏迄今为止报道的所有 AZAs 中存在的 C-20-C-21 二醇,并且在 C-23 处具有 21,22-烯烃和酮基。使用基于 Jurkat T 淋巴细胞细胞的体外模型系统对 3 进行的毒理学评估表明,其效力比 AZA1 低约 30 倍。AZA10 的相应 21,22-脱氢-23-氧代类似物(AZA28)和 AZA3、-4、-5、-6、-9 和 -10 的 21,22-脱氢类似物(AZA25、-48(4)、-60、-27、-49 和-61)也通过高分辨质谱/质谱(HRMS/MS)、过碘酸盐裂解反应性、从已知类似物的转化以及 NMR(对于存在于部分纯化的 AZA7 样品中的 4)来鉴定。

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