首页> 外文期刊>Acta crystallographica. Section F, Structural biology communications >Enhancement of the thermostability of mouse claudin-3 on complex formation with the carboxylterminal region of Clostridium perfringens enterotoxin improves crystal quality
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Enhancement of the thermostability of mouse claudin-3 on complex formation with the carboxylterminal region of Clostridium perfringens enterotoxin improves crystal quality

机译:利用腹肠毒素的羧基肿瘤区域对小鼠克劳德蛋白-3对小鼠克劳德蛋白-3的热稳定性提高了晶体质量

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摘要

Tight junctions regulate substance permeation through intercellular spaces as a physical barrier or a paracellular pathway, and play an important role in maintaining the internal environment. Claudins, which are tetraspan-transmembrane proteins, are pivotal components of tight junctions. In mammals 27 claudin subtypes have been identified, each of which interacts with specific subtypes. Although the crystal structures of several subtypes have been determined, the molecular mechanisms underlying subtype specificity remain unclear. Here, mouse claudin-3 (mCldn3) was crystallized in complex with the C-terminal region of Clostridium perfringens enterotoxin (C-CPE) for the structural analysis of an additional claudin subtype. mCldn3 alone was difficult to crystallize, but complex formation with C-CPE enhanced the thermostability of mCldn3 and facilitated its crystallization. The introduction of an S313A mutation into C-CPE further improved its thermostability, and the resolution limits of the diffraction data sets improved from 8 ? for the wild-type complex to 4.7 ? for the S313A mutant complex.
机译:紧密的连接调节通过细胞间隙作为物理屏障或肺静脉途径的物质渗透,并在维持内部环境方面发挥重要作用。克劳德林是四甘蓝 - 跨膜蛋白,是紧密连接的枢转分量。在哺乳动物中,已经鉴定了27个Claudin亚型,每个亚型与特定亚型相互作用。尽管已经确定了几种亚型的晶体结构,但下面的亚型特异性的分子机制仍然不清楚。这里,小鼠克劳丁蛋白-3(MCLDN3)与梭菌的C末端区域的复合物结晶,其流量肠毒素(C-CPE)用于额外的克劳德蛋白亚型的结构分析。单独的MCLDN3难以结晶,但具有C-CPE的复杂形成增强了MCLDN3的热稳定性,并促进了其结晶。将S313A突变引入C-CPE进一步提高了其热稳定性,并且衍射数据集的分辨率限制从8提高?对于野生型复杂到4.7?对于S313A突变体复合物。

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