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  3. Biochemistry and Molecular Biology / 生物化學暨分子生物學研究所
  4. Bloodmeals fuel dengue virus replication in the female mosquito Aedes aegypti
 
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Bloodmeals fuel dengue virus replication in the female mosquito Aedes aegypti

Journal
Journal of virology
Journal Volume
98
Journal Issue
7
Start Page
e0070124
ISSN
1098-5514
Date Issued
2024-07-23
Author(s)
Huang, Yu-Ning
Lee, Kuan-Ying
SHIN-HONG SHIAO  
Chen, Chun-Hong
Yu, Guann-Yi
MING-JIUN YU  
DOI
10.1128/jvi.00701-24
URI
https://scholars.lib.ntu.edu.tw/handle/123456789/720782
Abstract
Vector competence defines the ability of a vector to acquire, host, and transmit a pathogen. Understanding the molecular determinants of the mosquitos' competence to host dengue virus (DENV) holds promise to prevent its transmission. To this end, we employed RNA-seq to profile mRNA transcripts of the female mosquitos feeding on naïve vs viremic mouse. While most transcripts (12,634) did not change their abundances, 360 transcripts showed decreases. Biological pathway analysis revealed representatives of the decreased transcripts involved in the wnt signaling pathway and hippo signaling pathway. One thousand three hundred fourteen transcripts showed increases in abundance and participate in 21 biological pathways including amino acid metabolism, carbon metabolism, fatty acid metabolism, and oxidative phosphorylation. Inhibition of oxidative phosphorylation with antimycin A reduced oxidative phosphorylation activity and ATP concentration associated with reduced DENV replication in the cells. Antimycin A did not affect the amounts of the non-structural proteins 3 and 5, two major components of the replication complex. Ribavirin, an agent that reduces GTP concentration, recapitulated the effects of reduced ATP concentration on DENV replication. Knocking down one of the oxidative phosphorylation components, ATP synthase subunit β, reduced DENV replication in the mosquitos. In summary, our results suggest that DENV enhances metabolic pathways in the female mosquitos to supply nutrients and energy for virus replication. ATP synthase subunit β knockdown might be exploited to reduce the mosquitos' competence to host and transmit DENV. Through evolution, the mosquito-borne viruses have adapted to the blood-feeding behaviors of their opportunist hosts to fulfill a complete lifecycle in humans and mosquitos. Disruption in the mosquitos' ability to host these viruses offers strategies to prevent diseases caused by them. With the advent of genomic tools, we discovered that dengue virus (DENV) benefited from the female mosquitos' bloodmeals for metabolic and energetic supplies for replication. Chemical or genetic disruption in these supplies reduced DENV replication in the female mosquitos. Our discovery can be exploited to produce genetically modified mosquitos, in which DENV infection leads to disruption in the supplies and thereby reduces replication and transmission. Our discovery might be extrapolated to prevent mosquito-borne virus transmission and the diseases they cause.
Subjects
dengue fever
oxidative phosphorylation
public health
vector competence
yellow fever mosquito
SDGs

[SDGs]SDG3

Type
journal article

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