Department of Medicine, School of Clinical Medicine, University of Cambridge, Cambridge, United Kingdom.
J Immunol. 2010 Jul 15;185(2):1093-102. doi: 10.4049/jimmunol.1000789. Epub 2010 Jun 7.
Human CMV (HCMV) encodes multiple genes that control NK cell activation and cytotoxicity. Some of these HCMV-encoded gene products modulate NK cell activity as ligands expressed at the cell surface that engage inhibitory NK cell receptors, whereas others prevent the infected cell from upregulating ligands that bind to activating NK cell receptors. A major activating NKR is the homodimeric NKG2D receptor, which has eight distinct natural ligands in humans. It was shown that HCMV is able to prevent the surface expression of five of these ligands (MIC A/B and ULBP1, 2, and 6). In this article, we show that the HCMV gene product UL142 can prevent cell surface expression of ULBP3 during infection. We further show that UL142 interacts with ULBP3 and mediates its intracellular retention in a compartment that colocalizes with markers of the cis-Golgi complex. In doing so, UL142 prevents ULBP3 trafficking to the surface and protects transfected cells from NK-mediated cytotoxicity. This is the first description of a viral gene able to mediate downregulation of ULBP3.
人巨细胞病毒 (HCMV) 编码多种基因,这些基因控制 NK 细胞的激活和细胞毒性。其中一些 HCMV 编码的基因产物作为细胞表面表达的配体调节 NK 细胞的活性,这些配体与抑制性 NK 细胞受体结合,而其他基因产物则阻止被感染的细胞上调与激活 NK 细胞受体结合的配体。主要的激活性 NKR 是二聚体 NKG2D 受体,人类中有 8 种不同的天然配体。研究表明,HCMV 能够阻止其中 5 种配体(MIC A/B 和 ULBP1、2 和 6)的表面表达。在本文中,我们表明 HCMV 基因产物 UL142 可以在感染过程中阻止 ULBP3 的细胞表面表达。我们进一步表明,UL142 与 ULBP3 相互作用,并将其在与顺式高尔基体复合物标志物共定位的细胞内隔室中保留下来。通过这种方式,UL142 阻止了 ULBP3 的转运到表面,并保护转染细胞免受 NK 介导的细胞毒性。这是第一个描述能够介导 ULBP3 下调的病毒基因的文章。
