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来自 的人类癌细胞活性毒素Cry41Aa与其杀虫同类物作用相似。

The human cancer cell active toxin Cry41Aa from acts like its insecticidal counterparts.

作者信息

Krishnan Vidisha, Domanska Barbara, Elhigazi Alicia, Afolabi Fatai, West Michelle J, Crickmore Neil

机构信息

School of Life Sciences, University of Sussex, Falmer, Brighton BN1 9QG, U.K.

出版信息

Biochem J. 2017 Apr 28;474(10):1591-1602. doi: 10.1042/BCJ20170122.

DOI:10.1042/BCJ20170122
PMID:28341807
Abstract

Understanding how certain protein toxins from the normally insecticidal bacterium () target human cell lines has implications for both the risk assessment of products containing these toxins and potentially for cancer therapy. This understanding requires knowledge of whether the human cell active toxins work by the same mechanism as their insecticidal counterparts or by alternative ones. The Cry41Aa (also known as Parasporin3) toxin is structurally related to the toxins synthesised by commercially produced transgenic insect-resistant plants, with the notable exception of an additional C-terminal β-trefoil ricin domain. To better understand its mechanism of action, we developed an efficient expression system for the toxin and created mutations in regions potentially involved in the toxic mechanism. Deletion of the ricin domain did not significantly affect the activity of the toxin against the human HepG2 cell line, suggesting that this region was not responsible for the mammalian specificity of Cry41Aa. Various biochemical assays suggested that unlike some other human cell active toxins from Cry41Aa did not induce apoptosis, but that its mechanism of action was consistent with that of a pore-forming toxin. The toxin induced a rapid and significant decrease in metabolic activity. Adenosine triphosphate depletion, cell swelling and membrane damage were also observed. An exposed loop region believed to be involved in receptor binding of insecticidal Cry toxins was shown to be important for the activity of Cry41Aa against HepG2 cells.

摘要

了解来自通常具有杀虫作用的苏云金芽孢杆菌()的某些蛋白质毒素如何靶向人类细胞系,对于评估含有这些毒素的产品的风险以及潜在的癌症治疗都具有重要意义。要实现这一理解,需要知道对人类细胞具有活性的毒素是否与其杀虫对应物通过相同机制起作用,还是通过其他机制。Cry41Aa(也称为副孢子蛋白3)毒素在结构上与商业生产的转基因抗虫植物合成的毒素相关,但值得注意的是,它还有一个额外的C端β-三叶蓖麻毒素结构域。为了更好地理解其作用机制,我们开发了一种有效的毒素表达系统,并在可能参与毒性机制的区域引入突变。缺失蓖麻毒素结构域对毒素针对人类HepG2细胞系的活性没有显著影响,这表明该区域与Cry41Aa的哺乳动物特异性无关。各种生化分析表明,与其他一些对人类细胞具有活性的苏云金芽孢杆菌毒素不同,Cry41Aa不会诱导细胞凋亡,但其作用机制与成孔毒素一致。该毒素导致代谢活性迅速且显著降低。还观察到三磷酸腺苷耗竭、细胞肿胀和膜损伤。一个据信参与杀虫Cry毒素受体结合的暴露环区域,对Cry41Aa针对HepG2细胞的活性很重要。

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