首页> 美国卫生研究院文献>The Journal of Biological Chemistry >The Structure of the Elicitor Cerato-platanin (CP) the First Member of the CP Fungal Protein Family Reveals a Double ψβ-Barrel Fold and Carbohydrate Binding
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The Structure of the Elicitor Cerato-platanin (CP) the First Member of the CP Fungal Protein Family Reveals a Double ψβ-Barrel Fold and Carbohydrate Binding

机译:CP真菌蛋白家族的第一个成员激肽Cerato-Platanin(CP)的结构揭示了双ψβ-桶折叠和碳水化合物结合

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摘要

Cerato-platanin (CP) is a secretion protein produced by the fungal pathogen Ceratocystis platani, the causal agent of the plane canker disease and the first member of the CP family. CP is considered a pathogen-associated molecular pattern because it induces various defense responses in the host, including production of phytoalexins and cell death. Although much is known about the properties of CP and related proteins as elicitors of plant defense mechanisms, its biochemical activity and host target(s) remain elusive. Here, we present the three-dimensional structure of CP. The protein, which exhibits a remarkable pH and thermal stability, has a double ψβ-barrel fold quite similar to those found in expansins, endoglucanases, and the plant defense protein barwin. Interestingly, although CP lacks lytic activity against a variety of carbohydrates, it binds oligosaccharides. We identified the CP region responsible for binding as a shallow surface located at one side of the β-barrel. Chemical shift perturbation of the protein amide protons, induced by oligo-N-acetylglucosamines of various size, showed that all the residues involved in oligosaccharide binding are conserved among the members of the CP family. Overall, the results suggest that CP might be involved in polysaccharide recognition and that the double ψβ-barrel fold is widespread in distantly related organisms, where it is often involved in host-microbe interactions.
机译:ceratoplatanin(CP)是由真菌病原体Ceratocystis platani产生的分泌蛋白,Ceratocystis platani是平面溃疡病的病因,也是CP家族的第一个成员。 CP被认为是病原体相关的分子模式,因为它在宿主中诱导各种防御反应,包括植物抗毒素的产生和细胞死亡。尽管关于CP和相关蛋白作为植物防御机制的引发剂的特性已广为人知,但其生化活性和宿主靶标仍然难以捉摸。在这里,我们介绍CP的三维结构。该蛋白质具有出色的pH值和热稳定性,其双ψβ-桶形折叠倍数与在扩展酶,内切葡聚糖酶和植物防御蛋白barwin中发现的非常相似。有趣的是,尽管CP缺乏针对多种碳水化合物的裂解活性,但它结合了寡糖。我们将负责结合的CP区域确定为位于β-桶一侧的浅表面。由各种大小的寡-N-乙酰氨基葡糖胺引起的蛋白质酰胺质子的化学位移扰动表明,参与寡糖结合的所有残基在CP家族成员中均保守。总的来说,结果表明CP可能参与了多糖的识别,并且ψ-桶的双倍折叠在远缘的生物中很普遍,而后者通常参与宿主-微生物的相互作用。

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