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TatBC-Independent TatA/Tat Substrate Interactions Contribute to Transport Efficiency

机译:TatBC独立的TatA / Tat底物相互作用有助于提高运输效率

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摘要

The Tat system can transport folded, signal peptide-containing proteins (Tat substrates) across energized membranes of prokaryotes and plant plastids. A twin-arginine motif in the signal peptide of Tat substrates is recognized by TatC-containing complexes, and TatA permits the membrane passage. Often, as in the model Tat systems of Escherichia coli and plant plastids, a third component – TatB – is involved that resembles TatA but has a higher affinity to TatC. It is not known why most TatA dissociates from TatBC complexes in vivo and distributes more evenly in the membrane. Here we show a TatBC-independent substrate-binding to TatA from Escherichia coli, and we provide evidence that this binding enhances Tat transport. First hints came from in vivo cross-linking data, which could be confirmed by affinity co-purification of TatA with the natural Tat substrates HiPIP and NrfC. Two positions on the surface of HiPIP could be identified that are important for the TatA interaction and transport efficiency, indicating physiological relevance of the interaction. Distributed TatA thus may serve to accompany membrane-interacting Tat substrates to the few TatBC spots in the cells.
机译:Tat系统可将折叠的含信号肽的蛋白质(Tat底物)转运到原核生物和植物质体的活化膜上。 Tat底物的信号肽中的双精氨酸基序被含TatC的复合物识别,TatA允许膜通过。通常,就像在大肠杆菌和植物质体的模型Tat系统中一样,涉及到第三种成分-TatB-与TatA类似,但对TatC具有更高的亲和力。尚不清楚为什么大多数TatA在体内从TatBC复合物中解离并在膜中更均匀地分布。在这里,我们显示了独立于TatBC的底物与来自大肠杆菌的TatA结合,并且我们提供了这种结合增强Tat运输的证据。第一个提示来自体内的交联数据,这可以通过TatA与天然Tat底物HiPIP和NrfC的亲和共纯化来证实。可以鉴定出HiPIP表面上的两个位置,这些位置对于TatA相互作用和转运效率很重要,表明了相互作用的生理学意义。因此,分布的TatA可用于与膜相互作用的Tat底物伴随细胞中的少数TatBC点。

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