首页> 外文期刊>The Journal of biological chemistry >Allosteric Transitions Direct Protein Tagging by PafA, the Prokaryotic Ubiquitin-like Protein (Pup) Ligase
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Allosteric Transitions Direct Protein Tagging by PafA, the Prokaryotic Ubiquitin-like Protein (Pup) Ligase

机译:BAFA的颠跃于PAFA的直接蛋白质标记,原核泛素样蛋白(幼崽)连接酶

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Protein degradation via prokaryotic ubiquitin-like protein (Pup) tagging is conserved in bacteria belonging to the phyla Actinobacteria and Nitrospira. The physiological role of this novel proteolytic pathway is not yet clear, although in Mycobacterium tuberculosis, the world's most threatening bacterial pathogen, Pup tagging is important for virulence. PafA, the Pup ligase, couples ATP hydrolysis with Pup conjugation to lysine side chains of protein substrates. PafA is the sole Pup ligase in M. tuberculosis and apparently, in other bacteria. Thus, whereas PafA is a key player in the Pup tagging (i.e. pupylation) system, control of its activity and interactions with target protein substrates remain poorly understood. In this study, we examined the mechanism of protein pupylation by PafA in Mycobacterium smegmatis, a model mycobacterial organism. We report that PafA is an allosteric enzyme that binds its target substrates cooperatively and find that PafA allostery is controlled by the binding of target protein substrates, yet is unaffected by Pup binding. Analysis of PafA pupylation using engineered substrates differing in the number of pupylation sites points to PafA acting as a dimer. These findings suggest that protein pupylation can be regulated at the level of PafA allostery.
机译:通过原核泛素样蛋白(幼崽)标记的蛋白质降解在属于肌肌肌菌和Nitrospira的细菌中被保守。这种新型蛋白水解途径的生理作用尚不清楚,虽然在结核分枝杆菌中,世界上最威胁的细菌病原体,幼崽标记对于毒力很重要。 PAFA,幼崽酶,用幼瞳叠层与蛋白质底链的瞳孔缀合夫妇。 Pafa是肺结核菌的唯一幼崽酶,显然是在其他细菌中。因此,虽然PAFA是幼崽标记(即蛹)系统中的关键球员,其活性的控制和与靶蛋白质基质的相互作用仍然明显。在这项研究中,我们在分枝杆菌的分枝杆菌生物体中检查了PAFA蛋白蛹化的机制。我们认为PAFA是一种颠覆性酶,其协同结合其靶基质,并发现PAFA仿生体通过靶蛋白质底物的结合来控制,但不受幼崽结合的影响。使用工程基材的PAFA蛹分析在蛹位点数不同的指向作为二聚体的PAFA。这些发现表明,蛋白质捕蛋白可以在PAFA BALLostery的水平下调节。

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