Influenza virus reassortment occurs with high frequency in the absence of segment mismatch.

Reassortment is fundamental to the evolution of influenza viruses and plays a key role in the generation of epidemiologically significant strains. Previous studies indicate that reassortment is restricted by segment mismatch, arising from functional incompatibilities among components of two viruses....

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Main Authors: Nicolle Marshall, Lalita Priyamvada, Zachary Ende, John Steel, Anice C Lowen
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS Pathogens
Online Access:http://europepmc.org/articles/PMC3681746?pdf=render
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spelling doaj-fb7cbfa061b64a568f34a245529a53a82020-11-25T00:12:00ZengPublic Library of Science (PLoS)PLoS Pathogens1553-73661553-73742013-01-0196e100342110.1371/journal.ppat.1003421Influenza virus reassortment occurs with high frequency in the absence of segment mismatch.Nicolle MarshallLalita PriyamvadaZachary EndeJohn SteelAnice C LowenReassortment is fundamental to the evolution of influenza viruses and plays a key role in the generation of epidemiologically significant strains. Previous studies indicate that reassortment is restricted by segment mismatch, arising from functional incompatibilities among components of two viruses. Additional factors that dictate the efficiency of reassortment remain poorly characterized. Thus, it is unclear what conditions are favorable for reassortment and therefore under what circumstances novel influenza A viruses might arise in nature. Herein, we describe a system for studying reassortment in the absence of segment mismatch and exploit this system to determine the baseline efficiency of reassortment and the effects of infection dose and timing. Silent mutations were introduced into A/Panama/2007/99 virus such that high-resolution melt analysis could be used to differentiate all eight segments of the wild-type and the silently mutated variant virus. The use of phenotypically identical parent viruses ensured that all progeny were equally fit, allowing reassortment to be measured without selection bias. Using this system, we found that reassortment occurred efficiently (88.4%) following high multiplicity infection, suggesting the process is not appreciably limited by intracellular compartmentalization. That co-infection is the major determinant of reassortment efficiency in the absence of segment mismatch was confirmed with the observation that the proportion of viruses with reassortant genotypes increased exponentially with the proportion of cells co-infected. The number of reassortants shed from co-infected guinea pigs was likewise dependent on dose. With 10⁶ PFU inocula, 46%-86% of viruses isolated from guinea pigs were reassortants. The introduction of a delay between infections also had a strong impact on reassortment and allowed definition of time windows during which super-infection led to reassortment in culture and in vivo. Overall, our results indicate that reassortment between two like influenza viruses is efficient but also strongly dependent on dose and timing of the infections.http://europepmc.org/articles/PMC3681746?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Nicolle Marshall
Lalita Priyamvada
Zachary Ende
John Steel
Anice C Lowen
spellingShingle Nicolle Marshall
Lalita Priyamvada
Zachary Ende
John Steel
Anice C Lowen
Influenza virus reassortment occurs with high frequency in the absence of segment mismatch.
PLoS Pathogens
author_facet Nicolle Marshall
Lalita Priyamvada
Zachary Ende
John Steel
Anice C Lowen
author_sort Nicolle Marshall
title Influenza virus reassortment occurs with high frequency in the absence of segment mismatch.
title_short Influenza virus reassortment occurs with high frequency in the absence of segment mismatch.
title_full Influenza virus reassortment occurs with high frequency in the absence of segment mismatch.
title_fullStr Influenza virus reassortment occurs with high frequency in the absence of segment mismatch.
title_full_unstemmed Influenza virus reassortment occurs with high frequency in the absence of segment mismatch.
title_sort influenza virus reassortment occurs with high frequency in the absence of segment mismatch.
publisher Public Library of Science (PLoS)
series PLoS Pathogens
issn 1553-7366
1553-7374
publishDate 2013-01-01
description Reassortment is fundamental to the evolution of influenza viruses and plays a key role in the generation of epidemiologically significant strains. Previous studies indicate that reassortment is restricted by segment mismatch, arising from functional incompatibilities among components of two viruses. Additional factors that dictate the efficiency of reassortment remain poorly characterized. Thus, it is unclear what conditions are favorable for reassortment and therefore under what circumstances novel influenza A viruses might arise in nature. Herein, we describe a system for studying reassortment in the absence of segment mismatch and exploit this system to determine the baseline efficiency of reassortment and the effects of infection dose and timing. Silent mutations were introduced into A/Panama/2007/99 virus such that high-resolution melt analysis could be used to differentiate all eight segments of the wild-type and the silently mutated variant virus. The use of phenotypically identical parent viruses ensured that all progeny were equally fit, allowing reassortment to be measured without selection bias. Using this system, we found that reassortment occurred efficiently (88.4%) following high multiplicity infection, suggesting the process is not appreciably limited by intracellular compartmentalization. That co-infection is the major determinant of reassortment efficiency in the absence of segment mismatch was confirmed with the observation that the proportion of viruses with reassortant genotypes increased exponentially with the proportion of cells co-infected. The number of reassortants shed from co-infected guinea pigs was likewise dependent on dose. With 10⁶ PFU inocula, 46%-86% of viruses isolated from guinea pigs were reassortants. The introduction of a delay between infections also had a strong impact on reassortment and allowed definition of time windows during which super-infection led to reassortment in culture and in vivo. Overall, our results indicate that reassortment between two like influenza viruses is efficient but also strongly dependent on dose and timing of the infections.
url http://europepmc.org/articles/PMC3681746?pdf=render
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