Antibody-Dependent Dengue Virus Entry Modulates Cell Intrinsic Responses for Enhanced Infection

Dengue is caused by infection with any one of four dengue viruses (DENV); the risk of severe disease appears to be enhanced by the cross-reactive or subneutralizing levels of antibody from a prior DENV infection. These antibodies opsonize DENV entry through the activating Fc gamma receptors (FcγR),...

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Bibliographic Details
Published in:mSphere 2019-09, Vol.4 (5)
Main Authors: Chan, Candice Y Y, Low, John Zhong Heng, Gan, Esther Shuyi, Ong, Eugenia Ziying, Zhang, Summer Li-Xin, Tan, Hwee Cheng, Chai, Xiaoran, Ghosh, Sujoy, Ooi, Eng Eong, Chan, Kuan Rong
Format: Article
Language:English
Subjects:
Antibodies
Antibodies, Viral - immunology
Antibody-Dependent Enhancement
Antigens
Antigens, Viral - immunology
Cell Line
Cells, Cultured
Dengue - virology
Dengue fever
Dengue hemorrhagic fever
dengue virus
Dengue Virus - physiology
Electron transport
Endocytosis
Fc receptors
Gene expression
Genetic engineering
Host Microbial Interactions
host response
Host-Microbe Biology
Humans
Immunoglobulins
Infections
Infectious diseases
Kinases
Life cycles
Load
Mitochondria
Monocytes
Monocytes - immunology
Monocytes - virology
Receptors, IgG - immunology
Replication
Ribonucleic acid
RNA
Sequence Analysis, RNA
Software
Splicing
Studies
Transcriptome
Viral infections
Viremia
Virus Internalization
Virus Replication
virus-host interactions
Viruses
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Summary:Dengue is caused by infection with any one of four dengue viruses (DENV); the risk of severe disease appears to be enhanced by the cross-reactive or subneutralizing levels of antibody from a prior DENV infection. These antibodies opsonize DENV entry through the activating Fc gamma receptors (FcγR), instead of infection through canonical receptor-mediated endocytosis, to result in higher levels of DENV replication. However, whether the enhanced replication is solely due to more efficient FcγR-mediated DENV entry or is also through FcγR-mediated alteration of the host transcriptome response to favor DENV infection remains unclear. Indeed, more efficient viral entry through activation of the FcγR can result in an increased viral antigenic load within target cells and confound direct comparisons of the host transcriptome response under antibody-dependent and antibody-independent conditions. Herein, we show that, despite controlling for the viral antigenic load in primary monocytes, the antibody-dependent and non-antibody-dependent routes of DENV entry induce transcriptome responses that are remarkably different. Notably, antibody-dependent DENV entry upregulated DENV host dependency factors associated with RNA splicing, mitochondrial respiratory chain complexes, and vesicle trafficking. Additionally, supporting findings from other studies, antibody-dependent DENV entry impeded the downregulation of ribosomal genes caused by canonical receptor-mediated endocytosis to increase viral translation. Collectively, our findings support the notion that antibody-dependent DENV entry alters host responses that support the viral life cycle and that host responses to DENV need to be defined in the context of its entry pathway. Dengue virus is the most prevalent mosquito-borne viral infection globally, resulting in variable manifestations ranging from asymptomatic viremia to life-threatening shock and multiorgan failure. Previous studies have indicated that the risk of severe dengue in humans can be increased by a specific range of preexisting anti-dengue virus antibody titers, a phenomenon termed antibody-dependent enhancement. There is hence a need to understand how antibodies augment dengue virus infection compared to the alternative canonical receptor-mediated viral entry route. Herein, we show that, besides facilitating viral uptake, antibody-mediated entry increases the expression of early host dependency factors to promote viral infection; these factors include RNA s
ISSN:2379-5042
2379-5042
DOI:10.1128/mSphere.00528-19