Large-scale sequencing of human influenza reveals the dynamic nature of viral genome evolution

Elodie Ghedin; Naomi A. Sengamalay; Martin Shumway; Jennifer Zaborsky; Tamara Feldblyum; Vik Subbu; David J. Spiro; Jeff Sitz; Hean Koo; Pavel Bolotov; Dmitry Dernovoy; Tatiana Tatusova; Yiming Bao; Kirsten St George; Jill Taylor; David J. Lipman; Claire M. Fraser; Jeffery K. Taubenberger; Steven L. Salzberg

doi:10.1038/nature04239

Large-scale sequencing of human influenza reveals the dynamic nature of viral genome evolution

Elodie Ghedin, Naomi A. Sengamalay, Martin Shumway, Jennifer Zaborsky, Tamara Feldblyum, Vik Subbu, David J. Spiro, Jeff Sitz, Hean Koo, Pavel Bolotov, Dmitry Dernovoy, Tatiana Tatusova, Yiming Bao, Kirsten St George, Jill Taylor, David J. Lipman, Claire M. Fraser, Jeffery K. Taubenberger, Steven L. Salzberg

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Abstract

Influenza viruses are remarkably adept at surviving in the human population over a long timescale. The human influenza A virus continues to thrive even among populations with widespread access to vaccines, and continues to be a major cause of morbidity and mortality. The virus mutates from year to year, making the existing vaccines ineffective on a regular basis, and requiring that new strains be chosen for a new vaccine. Less-frequent major changes, known as antigenic shift, create new strains against which the human population has little protective immunity, thereby causing worldwide pandemics. The most recent pandemics include the 1918 'Spanish' flu, one of the most deadly outbreaks in recorded history, which killed 30-50 million people worldwide, the 1957 'Asian' flu, and the 1968 'Hong Kong' flu. Motivated by the need for a better understanding of influenza evolution, we have developed flexible protocols that make it possible to apply large-scale sequencing techniques to the highly variable influenza genome. Here we report the results of sequencing 209 complete genomes of the human influenza A virus, encompassing a total of 2,821,103 nucleotides. In addition to increasing markedly the number of publicly available, complete influenza virus genomes, we have discovered several anomalies in these first 209 genomes that demonstrate the dynamic nature of influenza transmission and evolution. This new, large-scale sequencing effort promises to provide a more comprehensive picture of the evolution of influenza viruses and of their pattern of transmission through human and animal populations. All data from this project are being deposited, without delay, in public archives.

Original language	English (US)
Pages (from-to)	1162-1166
Number of pages	5
Journal	Nature
Volume	437
Issue number	7062
DOIs	https://doi.org/10.1038/nature04239
State	Published - Oct 20 2005
Externally published	Yes

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10.1038/nature04239

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Ghedin, E., Sengamalay, N. A., Shumway, M., Zaborsky, J., Feldblyum, T., Subbu, V., Spiro, D. J., Sitz, J., Koo, H., Bolotov, P., Dernovoy, D., Tatusova, T., Bao, Y., St George, K., Taylor, J., Lipman, D. J., Fraser, C. M., Taubenberger, J. K., & Salzberg, S. L. (2005). Large-scale sequencing of human influenza reveals the dynamic nature of viral genome evolution. Nature, 437(7062), 1162-1166. https://doi.org/10.1038/nature04239

Ghedin, E, Sengamalay, NA, Shumway, M, Zaborsky, J, Feldblyum, T, Subbu, V, Spiro, DJ, Sitz, J, Koo, H, Bolotov, P, Dernovoy, D, Tatusova, T, Bao, Y, St George, K, Taylor, J, Lipman, DJ, Fraser, CM, Taubenberger, JK & Salzberg, SL 2005, 'Large-scale sequencing of human influenza reveals the dynamic nature of viral genome evolution', Nature, vol. 437, no. 7062, pp. 1162-1166. https://doi.org/10.1038/nature04239

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title = "Large-scale sequencing of human influenza reveals the dynamic nature of viral genome evolution",

abstract = "Influenza viruses are remarkably adept at surviving in the human population over a long timescale. The human influenza A virus continues to thrive even among populations with widespread access to vaccines, and continues to be a major cause of morbidity and mortality. The virus mutates from year to year, making the existing vaccines ineffective on a regular basis, and requiring that new strains be chosen for a new vaccine. Less-frequent major changes, known as antigenic shift, create new strains against which the human population has little protective immunity, thereby causing worldwide pandemics. The most recent pandemics include the 1918 'Spanish' flu, one of the most deadly outbreaks in recorded history, which killed 30-50 million people worldwide, the 1957 'Asian' flu, and the 1968 'Hong Kong' flu. Motivated by the need for a better understanding of influenza evolution, we have developed flexible protocols that make it possible to apply large-scale sequencing techniques to the highly variable influenza genome. Here we report the results of sequencing 209 complete genomes of the human influenza A virus, encompassing a total of 2,821,103 nucleotides. In addition to increasing markedly the number of publicly available, complete influenza virus genomes, we have discovered several anomalies in these first 209 genomes that demonstrate the dynamic nature of influenza transmission and evolution. This new, large-scale sequencing effort promises to provide a more comprehensive picture of the evolution of influenza viruses and of their pattern of transmission through human and animal populations. All data from this project are being deposited, without delay, in public archives.",

author = "Elodie Ghedin and Sengamalay, {Naomi A.} and Martin Shumway and Jennifer Zaborsky and Tamara Feldblyum and Vik Subbu and Spiro, {David J.} and Jeff Sitz and Hean Koo and Pavel Bolotov and Dmitry Dernovoy and Tatiana Tatusova and Yiming Bao and {St George}, Kirsten and Jill Taylor and Lipman, {David J.} and Fraser, {Claire M.} and Taubenberger, {Jeffery K.} and Salzberg, {Steven L.}",

note = "Funding Information: Acknowledgements The authors acknowledge the laboratory and bioinformatics assistance provided by D. Kosack, C. Hauser, L. Groveman, R. Halpin, A. Phillippy and J. Sparenborg at TIGR, and S. Griesemer, M. Kleabonas and R. Bennett at the Wadsworth Center. We also thank M. Giovanni for help with project oversight and direction. This work was supported in part by the US National Institute of Allergy and Infectious Diseases. Viruses described in this study include some isolates collected as part of the Sentinel Physician Influenza Surveillance Program, which is supported by the US Centers for Disease Control and Prevention.",

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doi = "10.1038/nature04239",

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AU - Shumway, Martin

AU - Zaborsky, Jennifer

AU - Feldblyum, Tamara

AU - Subbu, Vik

AU - Spiro, David J.

AU - Sitz, Jeff

AU - Koo, Hean

AU - Bolotov, Pavel

AU - Dernovoy, Dmitry

AU - Tatusova, Tatiana

AU - Bao, Yiming

AU - St George, Kirsten

AU - Taylor, Jill

AU - Lipman, David J.

AU - Fraser, Claire M.

AU - Taubenberger, Jeffery K.

AU - Salzberg, Steven L.

N1 - Funding Information: Acknowledgements The authors acknowledge the laboratory and bioinformatics assistance provided by D. Kosack, C. Hauser, L. Groveman, R. Halpin, A. Phillippy and J. Sparenborg at TIGR, and S. Griesemer, M. Kleabonas and R. Bennett at the Wadsworth Center. We also thank M. Giovanni for help with project oversight and direction. This work was supported in part by the US National Institute of Allergy and Infectious Diseases. Viruses described in this study include some isolates collected as part of the Sentinel Physician Influenza Surveillance Program, which is supported by the US Centers for Disease Control and Prevention.

PY - 2005/10/20

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N2 - Influenza viruses are remarkably adept at surviving in the human population over a long timescale. The human influenza A virus continues to thrive even among populations with widespread access to vaccines, and continues to be a major cause of morbidity and mortality. The virus mutates from year to year, making the existing vaccines ineffective on a regular basis, and requiring that new strains be chosen for a new vaccine. Less-frequent major changes, known as antigenic shift, create new strains against which the human population has little protective immunity, thereby causing worldwide pandemics. The most recent pandemics include the 1918 'Spanish' flu, one of the most deadly outbreaks in recorded history, which killed 30-50 million people worldwide, the 1957 'Asian' flu, and the 1968 'Hong Kong' flu. Motivated by the need for a better understanding of influenza evolution, we have developed flexible protocols that make it possible to apply large-scale sequencing techniques to the highly variable influenza genome. Here we report the results of sequencing 209 complete genomes of the human influenza A virus, encompassing a total of 2,821,103 nucleotides. In addition to increasing markedly the number of publicly available, complete influenza virus genomes, we have discovered several anomalies in these first 209 genomes that demonstrate the dynamic nature of influenza transmission and evolution. This new, large-scale sequencing effort promises to provide a more comprehensive picture of the evolution of influenza viruses and of their pattern of transmission through human and animal populations. All data from this project are being deposited, without delay, in public archives.

AB - Influenza viruses are remarkably adept at surviving in the human population over a long timescale. The human influenza A virus continues to thrive even among populations with widespread access to vaccines, and continues to be a major cause of morbidity and mortality. The virus mutates from year to year, making the existing vaccines ineffective on a regular basis, and requiring that new strains be chosen for a new vaccine. Less-frequent major changes, known as antigenic shift, create new strains against which the human population has little protective immunity, thereby causing worldwide pandemics. The most recent pandemics include the 1918 'Spanish' flu, one of the most deadly outbreaks in recorded history, which killed 30-50 million people worldwide, the 1957 'Asian' flu, and the 1968 'Hong Kong' flu. Motivated by the need for a better understanding of influenza evolution, we have developed flexible protocols that make it possible to apply large-scale sequencing techniques to the highly variable influenza genome. Here we report the results of sequencing 209 complete genomes of the human influenza A virus, encompassing a total of 2,821,103 nucleotides. In addition to increasing markedly the number of publicly available, complete influenza virus genomes, we have discovered several anomalies in these first 209 genomes that demonstrate the dynamic nature of influenza transmission and evolution. This new, large-scale sequencing effort promises to provide a more comprehensive picture of the evolution of influenza viruses and of their pattern of transmission through human and animal populations. All data from this project are being deposited, without delay, in public archives.

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Large-scale sequencing of human influenza reveals the dynamic nature of viral genome evolution

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