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表没食子儿茶素没食子酸酯(eGCG)作为蓖麻毒素生物相容性抑制剂的体外评估

An in vitro evaluation of epigallocatechin gallate (eGCG) as a biocompatible inhibitor of ricin toxin.

作者信息

Dyer Paul D R, Kotha Arun K, Gollings Alex S, Shorter Susan A, Shepherd Thomas R, Pettit Marie W, Alexander Bruce D, Getti Giulia T M, El-Daher Samer, Baillie Les, Richardson Simon C W

机构信息

Department of Life and Sports Science, University of Greenwich, Central Avenue, Chatham, Kent ME4 4TB, UK.

Department of Pharmaceutical, Chemical and Environmental Science, University of Greenwich, Central Avenue, Chatham, Kent ME4 4TB, UK.

出版信息

Biochim Biophys Acta. 2016 Jul;1860(7):1541-50. doi: 10.1016/j.bbagen.2016.03.024. Epub 2016 Mar 23.

Abstract

The catechin, epigallocatechin gallate (eGCG), found in green tea, has inhibitory activity against a number of protein toxins and was investigated in relation to its impact upon ricin toxin (RT) in vitro. The IC(50) for RT was 0.08±0.004 ng/mL whereas the IC(50) for RT+100 μM eGCG was 3.02±0.572 ng/mL, indicating that eGCG mediated a significant (p<0.0001) reduction in ricin toxicity. This experiment was repeated in the human macrophage cell line THP-1 and IC(50) values were obtained for RT (0.54±0.024 ng/mL) and RT+100 μM eGCG (0.68±0.235 ng/mL) again using 100 μM eGCG and was significant (p=0.0013). The documented reduction in ricin toxicity mediated by eGCG was found to be eGCG concentration dependent, with 80 and 100 μg/mL (i.e. 178 and 223 μM respectively) of eGCG mediating a significant (p=0.0472 and 0.0232) reduction in ricin toxicity at 20 and 4 ng/ml of RT in Vero and THP-1 cells (respectively). When viability was measured in THP-1 cells by propidium iodide exclusion (as opposed to the MTT assays used previously) 10 ng/mL and 5 ng/mL of RT was used. The addition of 1000 μM and 100 μM eGCG mediated a significant (p=0.0015 and <0.0001 respectively) reduction in ricin toxicity relative to an identical concentration of ricin with 1 μg eGCG. Further, eGCG (100 μM) was found to reduce the binding of RT B chain to lactose-conjugated Sepharose as well as significantly (p=0.0039) reduce the uptake of RT B chain in Vero cells. This data suggests that eGCG may provide a starting point to refine biocompatible substances that can reduce the lethality of ricin.

摘要

绿茶中的儿茶素,表没食子儿茶素没食子酸酯(eGCG),对多种蛋白质毒素具有抑制活性,并对其在体外对蓖麻毒素(RT)的影响进行了研究。RT的IC(50)为0.08±0.004 ng/mL,而RT + 100 μM eGCG的IC(50)为3.02±0.572 ng/mL,表明eGCG介导蓖麻毒素毒性显著降低(p<0.0001)。该实验在人巨噬细胞系THP-1中重复进行,再次使用100 μM eGCG获得RT(0.54±0.024 ng/mL)和RT + 100 μM eGCG(0.68±0.235 ng/mL)的IC(50)值,差异显著(p = 0.0013)。已证明eGCG介导的蓖麻毒素毒性降低与eGCG浓度有关,在Vero和THP-1细胞中,80和100 μg/mL(分别为178和223 μM)的eGCG在20和4 ng/ml的RT作用下介导蓖麻毒素毒性显著降低(分别为p = 0.0472和0.0232)。当通过碘化丙啶排除法(与之前使用的MTT法相反)在THP-1细胞中测量活力时,使用了10 ng/mL和5 ng/mL的RT。相对于相同浓度的蓖麻毒素加1 μg eGCG,添加1000 μM和100 μM eGCG介导蓖麻毒素毒性显著降低(分别为p = 0.0015和<0.0001)。此外,发现eGCG(100 μM)可减少RT B链与乳糖偶联琼脂糖的结合,并显著(p = 0.0039)减少Vero细胞中RT B链的摄取。该数据表明eGCG可能为优化可降低蓖麻毒素致死性的生物相容性物质提供一个起点。

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