Evdokimov Artem G, Tropea Joseph E, Routzahn Karen M, Waugh David S
Protein Engineering Section, Macromolecular Crystallography Laboratory, National Cancer Institute at Frederick, Frederick, Maryland 21702-1201, USA.
Protein Sci. 2002 Feb;11(2):401-8. doi: 10.1110/ps.34102.
Yersinia pestis, the causative agent of bubonic plague, evades the immune response of the infected organism by using a type III (contact-dependent) secretion system to deliver effector proteins into the cytosol of mammalian cells, where they interfere with signaling pathways that regulate inflammation and cytoskeleton dynamics. The cytotoxic effector YopE functions as a potent GTPase-activating protein (GAP) for Rho family GTP-binding proteins, including RhoA, Rac1, and Cdc42. Down-regulation of these molecular switches results in the loss of cell motility and inhibition of phagocytosis, enabling Y. pestis to thrive on the surface of macrophages. We have determined the crystal structure of the GAP domain of YopE (YopE(GAP); residues 90-219) at 2.2-A resolution. Apart from the fact that it is composed almost entirely of alpha-helices, YopE(GAP) shows no obvious structural similarity with eukaryotic RhoGAP domains. Moreover, unlike the catalytically equivalent arginine fingers of the eukaryotic GAPs, which are invariably contained within flexible loops, the critical arginine in YopE(GAP) (Arg144) is part of an alpha-helix. The structure of YopE(GAP) is strikingly similar to the GAP domains from Pseudomonas aeruginosa (ExoS(GAP)) and Salmonella enterica (SptP(GAP)), despite the fact that the three amino acid sequences are not highly conserved. A comparison of the YopE(GAP) structure with those of the Rac1-ExoS(GAP) and Rac1-SptP complexes indicates that few, if any, significant conformational changes occur in YopE(GAP) when it interacts with its G protein targets. The structure of YopE(GAP) may provide an avenue for the development of novel therapeutic agents to combat plague.
鼠疫耶尔森菌是腺鼠疫的病原体,它通过III型(接触依赖性)分泌系统将效应蛋白输送到哺乳动物细胞的胞质溶胶中,从而逃避受感染机体的免疫反应,这些效应蛋白在胞质溶胶中干扰调节炎症和细胞骨架动态的信号通路。细胞毒性效应蛋白YopE作为Rho家族GTP结合蛋白(包括RhoA、Rac1和Cdc42)的有效GTP酶激活蛋白(GAP)发挥作用。这些分子开关的下调导致细胞运动性丧失和吞噬作用受到抑制,使鼠疫耶尔森菌能够在巨噬细胞表面存活。我们已经确定了YopE的GAP结构域(YopE(GAP);第90 - 219位氨基酸残基)的晶体结构,分辨率为2.2 Å。除了它几乎完全由α螺旋组成外,YopE(GAP)与真核RhoGAP结构域没有明显的结构相似性。此外,与真核GAP中具有催化等效性的精氨酸指不同,真核GAP的精氨酸指总是包含在柔性环内,而YopE(GAP)中的关键精氨酸(Arg144)是α螺旋的一部分。尽管这三个氨基酸序列的保守性不高,但YopE(GAP)的结构与铜绿假单胞菌的GAP结构域(ExoS(GAP))和肠炎沙门氏菌的GAP结构域(SptP(GAP))惊人地相似。将YopE(GAP)的结构与Rac1-ExoS(GAP)和Rac1-SptP复合物的结构进行比较表明,YopE(GAP)与它的G蛋白靶点相互作用时,几乎没有发生显著的构象变化。YopE(GAP)的结构可能为开发对抗鼠疫的新型治疗药物提供一条途径。