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破伤风毒素与神经细胞膜:结合与毒性之间的关系

Tetanus toxin and neuronal membranes: the relationship between binding and toxicity.

作者信息

Bakry N, Kamata Y, Sorensen R, Simpson L L

机构信息

Department of Medicine, Jefferson Medical College, Philadelphia, Pennsylvania.

出版信息

J Pharmacol Exp Ther. 1991 Aug;258(2):613-9.

PMID:1865360
Abstract

Tetanus toxin labeled by the Bolton-Hunter technique possesses high specific activity and retains substantial biological activity. This material can be used to characterize tetanus toxin binding to receptors in brain membrane preparations. In experiments aimed at measuring the absorption of labeled toxin, the displacement of labeled toxin by unlabeled toxin and the on-rate and off-rate constants, the data revealed two binding sites. The high affinity site had a Kd of 0.033 to 0.070 nM and a Bmax of 0.26 to 0.4 pmol/mg of protein; the low affinity site had a Kd of 0.89 to 6.9 nM and a Bmax of 1.55 to 3.0 pmol/mg of protein. The binding of tetanus toxin to brain membranes was enhanced greatly by low pH and ionic strength. Similarly to tetanus toxin, botulinum neurotoxin could be labeled by the Bolton-Hunter technique, and its binding to brain membranes was also enhanced by low pH and ionic strength. In studies with a neutralizing monoclonal antibody against tetanus toxin, the antigen-antibody interaction was not significantly altered by media with low ionic strength and pH. On the other hand, the ability of the antibody to block toxin binding to brain membranes was reduced substantially in nonphysiologic media. In a bioassay aimed at determining the effect of pH and tonicity on tissue association by toxin, low pH and ionic strength did not enhance toxicity. The biological activity of tetanus toxin was unaffected and that of botulinum neurotoxin was greatly diminished. The present findings confirm the widely reported observation that low pH and ionic strength promote tissue association by tetanus toxin, but they challenge the premise that this binding is relevant to the normal process of cell poisoning.

摘要

用博尔顿-亨特技术标记的破伤风毒素具有高比活性,并保留了大量生物活性。这种物质可用于表征破伤风毒素与脑膜制剂中受体的结合。在旨在测量标记毒素的吸收、未标记毒素对标记毒素的置换以及结合和解离速率常数的实验中,数据显示存在两个结合位点。高亲和力位点的解离常数(Kd)为0.033至0.070纳摩尔,最大结合量(Bmax)为0.26至0.4皮摩尔/毫克蛋白质;低亲和力位点的Kd为0.89至6.9纳摩尔,Bmax为1.55至3.0皮摩尔/毫克蛋白质。低pH值和离子强度可大大增强破伤风毒素与脑膜的结合。与破伤风毒素类似,肉毒杆菌神经毒素也可用博尔顿-亨特技术标记,其与脑膜的结合也可被低pH值和离子强度增强。在用抗破伤风毒素的中和单克隆抗体进行的研究中,低离子强度和pH值的培养基不会显著改变抗原-抗体相互作用。另一方面,在非生理培养基中,抗体阻断毒素与脑膜结合的能力会大幅降低。在一项旨在确定pH值和张力对毒素与组织结合影响的生物测定中,低pH值和离子强度不会增强毒性。破伤风毒素的生物活性未受影响,而肉毒杆菌神经毒素的生物活性则大大降低。目前的研究结果证实了广泛报道的观察结果,即低pH值和离子强度促进破伤风毒素与组织的结合,但它们对这种结合与细胞中毒正常过程相关这一前提提出了挑战。

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