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用于太平洋雪卡毒素(P-CTX-1)的血液中雪卡毒素提取方法的优化。

Optimization of ciguatoxin extraction method from blood for Pacific ciguatoxin (P-CTX-1).

作者信息

Bottein Dechraoui Marie-Yasmine, Wang Zhihong, Ramsdell John S

机构信息

Marine Biotoxins Program, Center for Coastal Environmental Health and Biomolecular Research, NOAA-National Ocean Service, Charleston, SC 29412, USA.

出版信息

Toxicon. 2007 Jan;49(1):100-5. doi: 10.1016/j.toxicon.2006.10.002. Epub 2006 Oct 14.

Abstract

Ciguatera diagnosis relies on clinical observations associated with a recent consumption of fish. Although needed, direct confirmation of exposure in subjects showing ciguatera disease symptoms is currently unavailable. We previously reported that ciguatoxins were measurable in the blood of mice exposed to extracts of Pacific ciguatoxins isolated from Gambierdiscus polynesiensis, and of Indian Ocean or Caribbean Sea ciguatoxins, isolated from fish. Although highly efficient for extracting spiked purified Caribbean-CTX-1, the methanolic extraction method previously described is found here to yield only 6% recovery of spiked Pacific-CTX-1 (P-CTX-1). We report in this short communication a substantially modified method for ciguatoxin extraction from both dried and fresh blood. With this method, toxin measurement is directly accomplished in acetonitrile deproteinated whole fresh blood or phosphate buffer solution (PBS) eluted dried blood using the N2A cell-based assay. Spike studies using increasing concentrations of purified ciguatoxins reveal linear (r2 above 0.87 for all toxins) and overall efficient toxin recoveries (62%, 96%, and 96% from fresh blood and 75%, 90%, and 74% from dried blood, for C-CTX-1, P-CTX-3C, and P-CTX-1, respectively). Comparative blood matrix analysis for P-CTX-1 recovery shows increased recovery of ciguatoxin activity from whole fresh blood than from dried blood, greater by 20% in P-CTX-1 spiked mice blood and by over 85% in P-CTX-1 exposed mouse blood. In conclusion, both Caribbean and Pacific ciguatoxins can be readily extracted from blood using this modified method; however, in the case of P-CTX-1 we find that fresh blood is optimal.

摘要

雪卡毒素中毒的诊断依赖于与近期食用鱼类相关的临床观察。尽管有必要,但目前尚无法对出现雪卡毒素中毒疾病症状的受试者进行暴露的直接确认。我们之前报道过,在暴露于从多氏冈比藻中分离出的太平洋雪卡毒素提取物以及从鱼类中分离出的印度洋或加勒比海雪卡毒素的小鼠血液中,可检测到雪卡毒素。尽管之前描述的甲醇提取法对提取加标的纯化加勒比海 - CTX - 1非常有效,但在此发现该方法对加标的太平洋 - CTX - 1(P - CTX - 1)回收率仅为6%。在本简短通讯中,我们报告了一种从干血和新鲜血液中提取雪卡毒素的大幅改进方法。使用这种方法,可通过基于N2A细胞的检测直接在乙腈脱蛋白的全血新鲜血液或磷酸盐缓冲溶液(PBS)洗脱的干血中完成毒素测量。使用浓度递增的纯化雪卡毒素进行加标研究显示,对于所有毒素,回收率呈线性(所有毒素的r2均高于0.87),且总体毒素回收率较高(对于C - CTX - 1、P - CTX - 3C和P - CTX - 1,从新鲜血液中的回收率分别为62%、96%和96%,从干血中的回收率分别为75%、90%和74%)。对P - CTX - 1回收率的血液基质比较分析表明,从全血新鲜血液中回收的雪卡毒素活性高于干血,在加标P - CTX - 1的小鼠血液中高出20%,在暴露于P - CTX - 1的小鼠血液中高出85%以上。总之,使用这种改进方法可轻松从血液中提取加勒比海和太平洋雪卡毒素;然而,对于P - CTX - 1,我们发现新鲜血液是最佳选择。

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