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基于吖啶酯的雪卡毒素和短裸甲藻毒素发光受体结合分析方法

Chemiluminescent Receptor Binding Assay for Ciguatoxins and Brevetoxins Using Acridinium Brevetoxin-B2.

机构信息

Faculty of Pharmacy, Kindai University, Higashiosaka 577-8502, Japan.

Japan Food Research Laboratories, Tama Laboratory, Nagayama 6-11-10, Tama 206-0025, Japan.

出版信息

Toxins (Basel). 2019 Oct 9;11(10):580. doi: 10.3390/toxins11100580.

Abstract

Ciguatera is the term for poisoning resulting from eating fish from tropical or subtropical regions. The causative toxins collectively named ciguatoxins (CTXs) widely differ in structures depending on their geographic origins, which range from the Pacific Ocean and the Indian Ocean to the Caribbean Sea. Neurotoxic shellfish poisoning (NSP) is caused by the ingestion of bivalve shellfish contaminated with brevetoxins (BTXs). Structurally, both CTXs and BTXs consist of fused ether rings aligned in a ladder shape. Pharmacologically, they bind at the same site (site-5) of voltage-gated sodium channels. However, the great structural diversity and the rare availability of reference toxins hinder LC-MS and ELISA methods, which operate on structure-based recognition. In this study, we prepared a chemiluminescent ligand, acridinium BTXB2 (ABTX), and tested its suitability for use in competitive binding assays to detect CTXs and BTXs. The affinity of ABTX to the rat brain synaptosome estimated by (1.66 pM) was approximately two-fold higher than that of PbTx-3 (BTX3). In addition, the equilibrium dissociation constant () was 0.84 nM, the maximum number of binding was 6.76 pmol toxin/mg protein, and the detection limit was 1.4 amol. The assays performed on samples spiked with CTX3C or BTXB4 (-palmitoylBTXB2) at 0.2-1.0 ng CTX/g fish flesh, and 200-800 ng BTXB4/g shellfish showed a linear relationship between the theoretical and observed toxin amounts.

摘要

雪卡毒素中毒是指食用热带或亚热带地区鱼类而引起的中毒。引起中毒的毒素统称为雪卡毒素(CTXs),根据其地理来源,其结构差异很大,范围从太平洋、印度洋到加勒比海。贝类神经毒素中毒(NSP)是由摄入受短裸甲藻毒素(BTXs)污染的双壳贝类引起的。从结构上看,CTXs 和 BTXs 都由融合的醚环排列成梯形状。从药理学上讲,它们结合在电压门控钠离子通道的相同部位(部位 5)。然而,巨大的结构多样性和罕见的参考毒素可用性阻碍了基于结构识别的 LC-MS 和 ELISA 方法。在这项研究中,我们制备了一种化学发光配体,吖啶 BTXB2(ABTX),并测试了它在竞争性结合测定中检测 CTXs 和 BTXs 的适用性。ABTX 对大鼠脑突触体的亲和力(1.66 pM)估计约为 PbTx-3(BTX3)的两倍。此外,平衡解离常数(Kd)为 0.84 nM,最大结合数为 6.76 pmol 毒素/mg 蛋白,检测限为 1.4 amol。在以 0.2-1.0 ng CTX/g 鱼肉和 200-800 ng BTXB4/g 贝类的 CTX3C 或 BTXB4 (-棕榈酰 BTXB2)加标样品上进行的测定中,理论和观察到的毒素量之间呈线性关系。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d551/6833909/80be99614fac/toxins-11-00580-g001.jpg

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