Rohrbeck Astrid, von Elsner Leonie, Hagemann Sandra, Just Ingo
Institute of Toxicology, Hannover Medical School, Carl-Neuberg-Str. 1, Hannover D-30625, Germany.
Toxins (Basel). 2015 Feb 2;7(2):380-95. doi: 10.3390/toxins7020380.
The Clostridium botulinum C3 exoenzyme selectively ADP-ribosylates low molecular weight GTP-binding proteins RhoA, B and C. This covalent modification inhibits Rho signaling activity, resulting in distinct actin cytoskeleton changes. Although C3 exoenzyme has no binding, the translocation domain assures that C3 enters cells and acts intracellularly. C3 uptake is thought to occur due to the high concentration of the C3 enzyme. However, recent work indicates that C3 is selectively endocytosed, suggesting a specific endocytotic pathway, which is not yet understood. In this study, we show that the C3 exoenzyme binds to cell surfaces and is internalized in a time-dependent manner. We show that the intermediate filament, vimentin, is involved in C3 uptake, as indicated by the inhibition of C3 internalization by acrylamide, a known vimentin disruption agent. Inhibition of C3 internalization was not observed by chemical inhibitors, like bafilomycin A, methyl-β-cyclodextrin, nocodazole or latrunculin B. Furthermore, the internalization of C3 exoenzyme was markedly inhibited in dynasore-treated HT22 cells. Our results indicate that C3 internalization depends on vimentin and does not depend strictly on both clathrin and caveolae.
肉毒梭菌C3外切酶可选择性地将小分子GTP结合蛋白RhoA、RhoB和RhoC进行ADP核糖基化。这种共价修饰会抑制Rho信号活性,导致肌动蛋白细胞骨架发生明显变化。尽管C3外切酶没有结合位点,但其易位结构域可确保C3进入细胞并在细胞内发挥作用。C3的摄取被认为是由于C3酶的高浓度所致。然而,最近的研究表明C3是被选择性内吞的,这提示存在一种尚未被理解的特定内吞途径。在本研究中,我们发现C3外切酶可与细胞表面结合并以时间依赖性方式被内化。我们发现中间丝波形蛋白参与了C3的摄取,这一点可通过已知的波形蛋白破坏剂丙烯酰胺对C3内化的抑制作用得到证明。化学抑制剂如巴弗洛霉素A、甲基-β-环糊精、诺考达唑或拉特罗毒素B并未观察到对C3内化的抑制作用。此外,在经dynasore处理的HT22细胞中,C3外切酶的内化明显受到抑制。我们的结果表明,C3的内化依赖于波形蛋白,并不严格依赖于网格蛋白和小窝。
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