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  4. The FDA-Approved Drug Nelfinavir Inhibits Lytic Cell-Free but Not Cell-Associated Nonlytic Transmission of Human Adenovirus
 
research article

The FDA-Approved Drug Nelfinavir Inhibits Lytic Cell-Free but Not Cell-Associated Nonlytic Transmission of Human Adenovirus

Georgi, Fanny
•
Andriasyan, Vardan
•
Witte, Robert
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August 20, 2020
Antimicrobial Agents and Chemotherapy

Adenoviruses (AdVs) are prevalent and give rise to chronic and re-current disease. Human AdV (HAdV) species B and C, such as HAdV-C2, -C5, and-B14, cause respiratory disease and constitute a health threat for immunocom-promised individuals. HAdV-Cs are well known for lysing cells owing to the E3CR1--encoded adenovirus death protein (ADP). We previously reported a high-throughput image-based screening framework and identified an inhibitor ofHAdV-C2 multiround infection, nelfinavir mesylate. Nelfinavir is the active ingre-dient of Viracept, an FDA-approved inhibitor of human immunodeficiency virus(HIV) aspartyl protease that is used to treat AIDS. It is not effective againstsingle-round HAdV infections. Here, we show that nelfinavir inhibits lytic cell-freetransmission of HAdV, indicated by the suppression of comet-shaped infectionfoci in cell culture. Comet-shaped foci occur upon convection-based transmissionof cell-free viral particles from an infected cell to neighboring uninfected cells.HAdV lacking ADP was insensitive to nelfinavir but gave rise to comet-shapedfoci, indicating that ADP enhances but is not required for cell lysis. This was sup-ported by the notion that HAdV-B14 and -B14p1 lacking ADP were highly sensi-tive to nelfinavir, although HAdV-A31, -B3, -B7, -B11, -B16, -B21, -D8, -D30, and-D37 were less sensitive. Conspicuously, nelfinavir uncovered slow-growinground HAdV-C2 foci, independent of neutralizing antibodies in the medium, in-dicative of nonlytic cell-to-cell transmission. Our study demonstrates the repur-posing potential of nelfinavir with postexposure efficacy against different HAdVsand describes an alternative nonlytic cell-to-cell transmission mode of HAdV.

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Type
research article
DOI
10.1128/AAC.01002-20
Author(s)
Georgi, Fanny
Andriasyan, Vardan
Witte, Robert
Murer, Luca
Hemmi, Silvio
Yu, Lisa
Grove, Melanie
Meili, Nicole
Kuttler, Fabien  
Yakimovich, Artur
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Date Issued

2020-08-20

Published in
Antimicrobial Agents and Chemotherapy
Volume

64

Issue

9

Start page

e01002

End page

20

Subjects

adenovirus death protein

•

antiviral agents

•

cell lysis

•

compound screening

•

drug repurposing

•

fluorescence imaging

•

membrane rupture

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oncolyticvirus

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plaque assay

•

virus transmission

Note

This article is licensed under a Creative Commons Attribution 4.0 International License

Editorial or Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
PTCB  
Available on Infoscience
October 22, 2020
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/172679
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