Department of Microbiology, University of Iowa, Iowa City, Iowa, USA.
J Virol. 2013 Aug;87(15):8327-41. doi: 10.1128/JVI.01025-13. Epub 2013 May 22.
The cell surface receptor T cell immunoglobulin mucin domain 1 (TIM-1) dramatically enhances filovirus infection of epithelial cells. Here, we showed that key phosphatidylserine (PtdSer) binding residues of the TIM-1 IgV domain are critical for Ebola virus (EBOV) entry through direct interaction with PtdSer on the viral envelope. PtdSer liposomes but not phosphatidylcholine liposomes competed with TIM-1 for EBOV pseudovirion binding and transduction. Further, annexin V (AnxV) substituted for the TIM-1 IgV domain, supporting a PtdSer-dependent mechanism. Our findings suggest that TIM-1-dependent uptake of EBOV occurs by apoptotic mimicry. Additionally, TIM-1 enhanced infection of a wide range of enveloped viruses, including alphaviruses and a baculovirus. As further evidence of the critical role of enveloped-virion-associated PtdSer in TIM-1-mediated uptake, TIM-1 enhanced internalization of pseudovirions and virus-like proteins (VLPs) lacking a glycoprotein, providing evidence that TIM-1 and PtdSer-binding receptors can mediate virus uptake independent of a glycoprotein. These results provide evidence for a broad role of TIM-1 as a PtdSer-binding receptor that mediates enveloped-virus uptake. Utilization of PtdSer-binding receptors may explain the wide tropism of many of these viruses and provide new avenues for controlling their virulence.
细胞表面受体 T 细胞免疫球蛋白粘蛋白结构域 1(TIM-1)显著增强了丝状病毒属对上皮细胞的感染。在这里,我们表明 TIM-1 IgV 结构域的关键磷脂酰丝氨酸(PtdSer)结合残基对于通过与病毒包膜上的 PtdSer 直接相互作用,埃博拉病毒(EBOV)进入细胞是至关重要的。PtdSer 脂质体而非磷脂酰胆碱脂质体可与 TIM-1 竞争 EBOV 假病毒结合和转导。此外,膜联蛋白 V(AnxV)替代了 TIM-1 IgV 结构域,支持 PtdSer 依赖性机制。我们的研究结果表明,TIM-1 依赖性摄取 EBOV 通过凋亡模拟发生。此外,TIM-1 增强了广泛包膜病毒的感染,包括甲病毒和杆状病毒。作为包膜病毒相关 PtdSer 在 TIM-1 介导摄取中的关键作用的进一步证据,TIM-1 增强了假病毒和缺乏糖蛋白的病毒样蛋白(VLPs)的内化,这表明 TIM-1 和 PtdSer 结合受体可以介导病毒摄取,而不依赖于糖蛋白。这些结果为 TIM-1 作为介导包膜病毒摄取的 PtdSer 结合受体的广泛作用提供了证据。利用 PtdSer 结合受体可能解释了这些病毒的广泛嗜性,并为控制其毒力提供了新的途径。
