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首页> 外文期刊>Biochemistry >The pertussis toxin S1 subunit is a thermally unstable protein susceptible to degradation by the 20S proteasome
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The pertussis toxin S1 subunit is a thermally unstable protein susceptible to degradation by the 20S proteasome

机译:百日咳毒素S1亚基是一种热不稳定蛋白,易于被20S蛋白酶体降解

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Pertussis toxin ( PT) is an AB-type protein toxin that consists of a catalytic A subunit ( PT S1) and an oligomeric, cell-binding B subunit. It belongs to a subset of AB toxins that move from the cell surface to the endoplasmic reticulum ( ER) before the A chain passes into the cytosol. Toxin translocation is thought to involve A chain unfolding in the ER and the quality control mechanism of ER-associated degradation ( ERAD). The absence of lysine residues in PT S1 may allow the translocated toxin to avoid ubiquitin-dependent degradation by the 26S proteasome, which is the usual fate of exported ERAD substrates. As the conformation of PT S1 appears to play an important role in toxin translocation, we used biophysical and biochemical methods to examine the structural properties of PT S1. Our in vitro studies found that the isolated PT S1 subunit is a thermally unstable protein that can be degraded in a ubiquitin-independent fashion by the core 20S proteasome. The thermal denaturation of PT S1 was inhibited by its interaction with NAD, a donor molecule used by PT S1 for the ADP ribosylation of target G proteins. These observations support a model of intoxication in which toxin translocation, degradation, and activity are all influenced by the heat-labile nature of the isolated toxin A chain.
机译:百日咳毒素(PT)是一种AB型蛋白质毒素,由催化性A亚基(PT S1)和与细胞结合的B寡聚体组成。它属于AB毒素的一个子集,该毒素在A链进入细胞质之前从细胞表面移动到内质网(ER)。毒素易位被认为与ER中的A链展开以及与ER相关的降解(ERAD)的质量控制机制有关。 PT S1中不存在赖氨酸残基可能使易位毒素避免了26S蛋白酶体的泛素依赖性降解,这是出口ERAD底物的常见命运。由于PT S1的构象似乎在毒素转运中起着重要作用,因此我们使用了生物物理和生化方法来检查PT S1的结构特性。我们的体外研究发现,分离出的PT S1亚基是一种热不稳定蛋白,可以被核心20S蛋白酶体以泛素非依赖性方式降解。 PT S1与NAD的相互作用抑制了PT S1的热变性,NAD是PT S1用于靶G蛋白的ADP核糖基化的供体分子。这些观察结果支持了一种中毒模型,其中毒素的易位,降解和活性都受分离的毒素A链的热不稳定特性影响。

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