From the Centre for Molecular Microbiology and Infection, Imperial College London, London SW7 2AZ, United Kingdom.
the Division of Molecular Structure, National Institute for Medical Research, The Ridgeway, London NW7 1AA, United Kingdom, and.
J Biol Chem. 2010 Feb 5;285(6):4087-4098. doi: 10.1074/jbc.M109.071035. Epub 2009 Nov 19.
Pathogenic Yersinia species neutralize innate immune mechanisms by injecting type three secretion effectors into immune cells, altering cell signaling. Our study elucidates how one of these effectors, YopO, blocks phagocytosis. We demonstrate using different phagocytic models that YopO specifically blocks Rac-dependent Fcgamma receptor internalization pathway but not complement receptor 3-dependent uptake, which is controlled by Rho activity. We show that YopO prevents Rac activation but does not affect Rac accumulation at the phagocytic cup. In addition, we show that plasma membrane localization and the guanine-nucleotide dissociation inhibitor (GDI)-like domain of YopO cooperate for maximal anti-phagocytosis. Although YopO has the same affinity for Rac1, Rac2, and RhoA in vitro, it selectively interacts with Rac isoforms in cells. This is due to the differential localization of the Rho family G proteins in resting cells; Rac isoforms partially exist as a GDI-free pool at the membrane of resting cells, whereas RhoA is trapped in the cytosol by RhoGDIalpha. We propose that YopO exploits this basic difference in localization and availability to selectively inhibit Rac-dependent phagocytosis.
致病性耶尔森氏菌通过将三种分泌效应蛋白注入免疫细胞来中和先天免疫机制,从而改变细胞信号转导。我们的研究阐明了其中一种效应蛋白 YopO 如何阻断吞噬作用。我们使用不同的吞噬模型证明,YopO 特异性阻断 Rac 依赖性 Fcγ受体内化途径,但不阻断 Rho 活性控制的补体受体 3 依赖性摄取。我们表明,YopO 可阻止 Rac 激活,但不影响吞噬杯中 Rac 的积累。此外,我们表明,YopO 的质膜定位和鸟嘌呤核苷酸解离抑制剂(GDI)样结构域共同作用以实现最大的抗吞噬作用。尽管 YopO 在体外对 Rac1、Rac2 和 RhoA 具有相同的亲和力,但它在细胞中选择性地与 Rac 同工型相互作用。这是由于 Rho 家族 G 蛋白在静止细胞中的定位不同所致;在静止细胞的膜上,Rac 同工型部分存在作为无 GDI 池,而 RhoA 则被 RhoGDIalpha 困在细胞质中。我们提出,YopO 利用这种在定位和可用性上的基本差异来选择性地抑制 Rac 依赖性吞噬作用。
