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Chemogenetic ON and OFF switches for RNA virus replication

Medicine and Health

Chemogenetic ON and OFF switches for RNA virus replication

E. Heilmann, J. Kimpel, et al.

Discover an innovative regulator switch for RNA viruses, offering controlled therapeutic applications in oncology. This groundbreaking research was advanced by authors from the Institute of Virology, Medical University of Innsbruck, and other esteemed institutions, ensuring safety while enhancing viral functions through HIV protease involvement.... show more
Abstract
Therapeutic application of RNA viruses as oncolytic agents or gene vectors requires a tight control of virus activity if toxicity is a concern. Here we present a regulator switch for RNA viruses using a conditional protease approach, in which the function of at least one viral protein essential for transcription and replication is linked to autocatalytical, exogenous human immunodeficiency virus (HIV) protease activity. Virus activity can be en- or disabled by various HIV protease inhibitors. Incorporating the HIV protease dimer in the genome of vesicular stomatitis virus (VSV) into the open reading frame of either the P- or L-protein resulted in an ON switch. Here, virus activity depends on co-application of protease inhibitor in a dose-dependent manner. Conversely, an N-terminal VSV polymerase tag with the HIV protease dimer constitutes an OFF switch, as application of protease inhibitor stops virus activity. This technology may also be applicable to other potentially therapeutic RNA viruses.
Publisher
Nature Communications
Published On
Mar 01, 2021
Authors
E. Heilmann, J. Kimpel, B. Hofer, A. Rössler, I. Blaas, L. Egerer, T. Nolden, C. Urbiola, H. G. Kräusslich, G. Wollmann, D. von Laer
Tags
RNA viruses
oncolytic agents
gene vectors
HIV protease
virus activity control
therapeutic application
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