Interaction of tetanus toxin derived hybrid proteins with neuronal cells.

Journal of natural toxins Pub Date : 2000-11-01
D M Figueiredo, C C Matthews, D A Parks, N F Fairweather, G Dougan, S G Wilt, P S Fishman
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Abstract

The non-toxic ganglioside binding domain of tetanus toxin (Hc fragment C or TTC) has been studied as a vector for delivering therapeutic proteins to neurons. There is little information on the cellular processing of proteins delivered by linkage to TTC. We have evaluated the cellular handling of a multi-domain hybrid protein containing TTC and both the human enzyme superoxide dismutase and the maltose binding protein from E. coli. Binding, internalization, and cleavage of this protein during prolonged incubation with fetal cortical neurons or cells of the N18-RE-105 line was evaluated by immunoblot analysis, ELISA, and immunocytochemistry. Hybrid proteins were bound and internalized in a manner very similar to TTC. Internalized proteins showed long-term stability within cells, and were degraded into predictable large protein fragments in both cell types. Fragments that were cleaved away from the TTC domain were released into extracellular fluid after internalization. Proteins coupled to TTC share its long-term stability after cellular internalization. After internalization, dissociation of proteins linked to TTC facilitates their release from the cell, but not into other cellular compartments such as the cytosol. TTC linked proteins are probably enclosed within a stable endosomal compartment throughout their cellular lifetime.

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破伤风毒素衍生的杂交蛋白与神经细胞的相互作用。
研究了破伤风毒素(Hc片段C或TTC)的无毒神经节苷结合域作为向神经元传递治疗蛋白的载体。关于通过TTC连接传递的蛋白质的细胞加工的信息很少。我们评估了一种含有TTC和人类超氧化物歧化酶以及来自大肠杆菌的麦芽糖结合蛋白的多域杂交蛋白的细胞处理。通过免疫印迹分析、ELISA和免疫细胞化学评估该蛋白与胎儿皮质神经元或N18-RE-105细胞系长时间孵育期间的结合、内化和裂解情况。杂交蛋白以与TTC非常相似的方式结合和内化。内化蛋白在细胞内表现出长期的稳定性,并在两种细胞类型中降解为可预测的大蛋白片段。从TTC结构域切割出来的片段在内化后被释放到细胞外液中。与TTC偶联的蛋白质在细胞内化后具有长期稳定性。内化后,与TTC相关的蛋白质解离有助于它们从细胞中释放出来,但不会进入细胞质等其他细胞区室。TTC连接蛋白可能在其整个细胞寿命中被封闭在一个稳定的内体隔室中。
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