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Seventeen a-subunit isoforms of paramecium V-ATPase provide high specialization in localization and function.

机译:草履虫V-ATPase的十七种α-亚基同工型在定位和功能上提供了高度专业化的特点。

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摘要

In the Paramecium tetraurelia genome, 17 genes encoding the 100-kDa-subunit (a-subunit) of the vacuolar-proton-ATPase were identified, representing by far the largest number of a-subunit genes encountered in any organism investigated so far. They group into nine clusters, eight pairs with >82% amino acid identity and one single gene. Green fluorescent protein-tagging of representatives of the nine clusters revealed highly specific targeting to at least seven different compartments, among them dense core secretory vesicles (trichocysts), the contractile vacuole complex, and phagosomes. RNA interference for two pairs confirmed their functional specialization in their target compartments: silencing of the trichocyst-specific form affected this secretory pathway, whereas silencing of the contractile vacuole complex-specific form altered organelle structure and functioning. The construction of chimeras between selected a-subunits surprisingly revealed the targeting signal to be located in the C terminus of the protein, in contrast with the N-terminal targeting signal of the a-subunit in yeast. Interestingly, some chimeras provoked deleterious effects, locally in their target compartment, or remotely, in the compartment whose specific a-subunit N terminus was used in the chimera.
机译:在草履虫属草履虫基因组中,鉴定了17个编码液泡质子-ATPase的100-kDa亚基(a-亚基)的基因,代表了迄今为止在所研究的任何生物中遇到的最大数量的a-亚基基因。他们分为九个簇,八对具有> 82%氨基酸同一性的对和一个单一基因。代表这九个簇的绿色荧光蛋白标签显示了高度特异性地靶向至少七个不同的区室,其中包括致密的核心分泌囊泡(毛囊),收缩的液泡复合物和吞噬体。两对RNA的RNA干扰证实了它们在靶标区室中的功能专一性:降低了毛囊的特异性形式影响了该分泌途径,而收缩了的液泡复合物特异性形式的沉默改变了细胞器的结构和功能。与酵母中α-亚基的N-末端靶向信号相反,所选α-亚基之间的嵌合体的构建令人惊讶地揭示了靶向信号位于蛋白质的C末端。有趣的是,一些嵌合体在其靶区室中局部地或在其嵌合体中使用了特定的α-亚基N末端的区室中远程地引起有害作用。

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