Identification of adipocyte plasma membrane-associated protein as a novel modulator of human cytomegalovirus infection

鉴定脂肪细胞质膜相关蛋白作为人类巨细胞病毒感染的新型调节剂

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作者:Xiaohua Ye, Xun Gui, Daniel C Freed, Zhiqiang Ku, Leike Li, Yuanzhi Chen, Wei Xiong, Xuejun Fan, Hang Su, Xi He, Richard R Rustandi, John W Loughney, Ningning Ma, Amy S Espeseth, Jian Liu, Hua Zhu, Dai Wang, Ningyan Zhang, Tong-Ming Fu, Zhiqiang An

Abstract

Human cytomegalovirus (HCMV) is a ubiquitous pathogen that can cause disability in newborns and serious clinical diseases in immunocompromised patients. HCMV has a large genome with enormous coding potential; its viral particles are equipped with complicated glycoprotein complexes and can infect a wide range of human cells. Although multiple host cellular receptors interacting with viral glycoproteins have been reported, the mechanism of HCMV infection remains a mystery. Here we report identification of adipocyte plasma membrane-associated protein (APMAP) as a novel modulator active in the early stage of HCMV infection. APMAP is necessary for HCMV infection in both epithelial cells and fibroblasts; knockdown of APMAP expression significantly reduced HCMV infection of these cells. Interestingly, ectopic expression of human APMAP in cells refractory to HCMV infection, such as canine MDCK and murine NIH/3T3 cells, promoted HCMV infection. Furthermore, reduction in viral immediate early (IE) gene transcription at 6 h post infection and delayed nucleus translocation of tegument delivered pp65 at 4 h post infection were detected in APMAP-deficient cells but not in the wildtype cells. These results suggest that APMAP plays a role in the early stage of HCMV infection. Results from biochemical studies of APMAP and HCMV proteins suggest that APMAP could participate in HCMV infection through interaction with gH/gL containing glycoprotein complexes at low pH and mediate nucleus translocation of tegument pp65. Taken together, our results suggest that APMAP functions as a modulator promoting HCMV infection in multiple cell types and is an important player in the complex HCMV infection mechanism.

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