Department of Microbiology, Immunobiology, Harvard Medical School, Boston, Massachusetts, USA.
mBio. 2012 Apr 3;3(2). doi: 10.1128/mBio.00291-11. Print 2012.
The Escherichia coli membrane protein DsbD functions as an electron hub that dispatches electrons received from the cytoplasmic thioredoxin system to periplasmic oxidoreductases involved in protein disulfide isomerization, cytochrome c biogenesis, and sulfenic acid reduction. Here, we describe a new class of DsbD proteins, named ScsB, whose members are found in proteobacteria and Chlamydia. ScsB has a domain organization similar to that of DsbD, but its amino-terminal domain differs significantly. In DsbD, this domain directly interacts with substrates to reduce them, which suggests that ScsB acts on a different array of substrates. Using Caulobacter crescentus as a model organism, we searched for the substrates of ScsB. We discovered that ScsB provides electrons to the first peroxide reduction pathway identified in the bacterial cell envelope. The reduction pathway comprises a thioredoxin-like protein, TlpA, and a peroxiredoxin, PprX. We show that PprX is a thiol-dependent peroxidase that efficiently reduces both hydrogen peroxide and organic peroxides. Moreover, we identified two additional proteins that depend on ScsB for reduction, a peroxiredoxin-like protein, PrxL, and a novel protein disulfide isomerase, ScsC. Altogether, our results reveal that the array of proteins involved in reductive pathways in the oxidative cell envelope is significantly broader than was previously thought. Moreover, the identification of a new periplasmic peroxiredoxin indicates that in some bacteria, it is important to directly scavenge peroxides in the cell envelope even before they reach the cytoplasm.
Peroxides are reactive oxygen species (ROS) that damage cellular components such as lipids, proteins, and nucleic acids. The presence of protection mechanisms against ROS is essential for cell survival. Bacteria express cytoplasmic catalases and thiol-dependent peroxidases to directly scavenge harmful peroxides. We report the identification of a peroxide reduction pathway active in the periplasm of Caulobacter crescentus, which reveals that, in some bacteria, it is important to directly scavenge peroxides in the cell envelope even before they reach the cytoplasm. The electrons required for peroxide reduction are delivered to this pathway by ScsB, a new type of membrane electron transporter. We also identified two additional likely ScsB substrates, including a novel protein disulfide isomerase. Our results reveal that the array of proteins involved in reductive pathways in the oxidative environment of the cell envelope is significantly broader than was previously thought.
大肠杆菌膜蛋白 DsbD 作为一个电子枢纽,将细胞质硫氧还蛋白系统接收的电子分配给参与蛋白质二硫键异构化、细胞色素 c 生物发生和亚磺酸还原的周质氧化还原酶。在这里,我们描述了一类新的 DsbD 蛋白,命名为 ScsB,其成员存在于变形菌门和衣原体中。ScsB 具有与 DsbD 相似的结构域组织,但它的氨基端结构域有很大的不同。在 DsbD 中,这个结构域直接与底物相互作用以还原它们,这表明 ScsB 作用于不同的底物。我们以新月柄杆菌为模型生物,搜索 ScsB 的底物。我们发现 ScsB 为细菌细胞包膜中鉴定的第一个过氧化物还原途径提供电子。该还原途径包括一种硫氧还蛋白样蛋白 TlpA 和一种过氧化物酶 PprX。我们表明 PprX 是一种依赖于巯基的过氧化物酶,可有效还原过氧化氢和有机过氧化物。此外,我们还鉴定了另外两种依赖于 ScsB 还原的蛋白质,一种过氧化物酶样蛋白 PrxL 和一种新型蛋白二硫键异构酶 ScsC。总之,我们的结果表明,参与氧化细胞包膜中还原途径的蛋白质阵列比以前认为的要广泛得多。此外,一种新的周质过氧化物酶的鉴定表明,在某些细菌中,即使在过氧化氢到达细胞质之前,直接清除细胞包膜中的过氧化物也很重要。
过氧化物是一种活性氧 (ROS),会破坏脂质、蛋白质和核酸等细胞成分。存在针对 ROS 的保护机制对于细胞存活至关重要。细菌表达细胞质过氧化氢酶和依赖巯基的过氧化物酶以直接清除有害的过氧化物。我们报告了新月柄杆菌周质中活性过氧化物还原途径的鉴定,这表明在某些细菌中,即使在过氧化氢到达细胞质之前,直接清除细胞包膜中的过氧化物也很重要。该途径所需的电子由 ScsB 提供,ScsB 是一种新型的膜电子转运蛋白。我们还鉴定了另外两种可能的 ScsB 底物,包括一种新型蛋白二硫键异构酶。我们的结果表明,参与细胞包膜氧化环境中还原途径的蛋白质阵列比以前认为的要广泛得多。
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