Islands of linkage in an ocean of pervasive recombination reveals two-speed evolution of human cytomegalovirus genomes

Florent Lassalle; Daniel P. Depledge; Matthew B. Reeves; Amanda C. Brown; Mette T. Christiansen; Helena J. Tutill; Rachel J. Williams; Katja Einer-Jensen; Jolyon Holdstock; Claire Atkinson; Julianne R. Brown; Freek B. Van Loenen; Duncan A. Clark; Paul D. Griffiths; Georges M.G.M. Verjans; Martin Schutten; Richard S.B. Milne; Francois Balloux; Judith Breuer

doi:10.1093/ve/vew017

Islands of linkage in an ocean of pervasive recombination reveals two-speed evolution of human cytomegalovirus genomes

Florent Lassalle, Daniel P. Depledge, Matthew B. Reeves, Amanda C. Brown, Mette T. Christiansen, Helena J. Tutill, Rachel J. Williams, Katja Einer-Jensen, Jolyon Holdstock, Claire Atkinson, Julianne R. Brown, Freek B. Van Loenen, Duncan A. Clark, Paul D. Griffiths, Georges M.G.M. Verjans, Martin Schutten, Richard S.B. Milne, Francois Balloux, Judith Breuer

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Abstract

Human cytomegalovirus (HCMV) infects most of the population worldwide, persisting throughout the host's life in a latent state with periodic episodes of reactivation. While typically asymptomatic, HCMV can cause fatal disease among congenitally infected infants and immunocompromised patients. These clinical issues are compounded by the emergence of antiviral resistance and the absence of an effective vaccine, the development of which is likely complicated by the numerous immune evasins encoded by HCMV to counter the host's adaptive immune responses, a feature that facilitates frequent super-infections. Understanding the evolutionary dynamics of HCMV is essential for the development of effective new drugs and vaccines. By comparing viral genomes fromuncultivated or low-passaged clinical samples of diverse origins, we observe evidence of frequent homologous recombination events, both recent and ancient, and no structure of HCMV genetic diversity at the whole-genome scale. Analysis of individual gene-scale loci reveals a striking dichotomy: while most of the genome is highly conserved, recombines essentially freely and has evolved under purifying selection, 21 genes display extreme diversity, structured into distinct genotypes that do not recombine with each other. Most of these hyper-variable genes encode glycoproteins involved in cell entry or escape of host immunity. Evidence that half of themhave diverged through episodes of intense positive selection suggests that rapid evolution of hyper-variable loci is likely driven by interactions with host immunity. It appears that this process is enabled by recombination unlinking hyper-variable loci from strongly constrained neighboring sites. It is conceivable that viralmechanisms facilitating super-infection have evolved to promote recombination between diverged genotypes, allowing the virus to continuously diversify at key loci to escape immune detection, whilemaintaining a genome optimally adapted to its asymptomatic infectious lifecycle.

Original language	English
Article number	vew017
Journal	Virus Evolution
Volume	2
Issue number	1
DOIs	https://doi.org/10.1093/ve/vew017 https://doi.org/10.1093/ve/vew017
Publication status	Published - 15 Jun 2016
Externally published	Yes

Bibliographical note

Publisher Copyright:
© The Author, 2016.

Keywords

CMV
immune evasion
recombination
viral evolution

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1093/ve/vew017
10.1093/ve/vew017Licence: CC BY 4.0

Vew017 (1)

Cite this

Lassalle, F., Depledge, D. P., Reeves, M. B., Brown, A. C., Christiansen, M. T., Tutill, H. J., Williams, R. J., Einer-Jensen, K., Holdstock, J., Atkinson, C., Brown, J. R., Van Loenen, F. B., Clark, D. A., Griffiths, P. D., Verjans, G. M. G. M., Schutten, M., Milne, R. S. B., Balloux, F., & Breuer, J. (2016). Islands of linkage in an ocean of pervasive recombination reveals two-speed evolution of human cytomegalovirus genomes. Virus Evolution, 2(1), Article vew017. https://doi.org/10.1093/ve/vew017, https://doi.org/10.1093/ve/vew017

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title = "Islands of linkage in an ocean of pervasive recombination reveals two-speed evolution of human cytomegalovirus genomes",

abstract = "Human cytomegalovirus (HCMV) infects most of the population worldwide, persisting throughout the host's life in a latent state with periodic episodes of reactivation. While typically asymptomatic, HCMV can cause fatal disease among congenitally infected infants and immunocompromised patients. These clinical issues are compounded by the emergence of antiviral resistance and the absence of an effective vaccine, the development of which is likely complicated by the numerous immune evasins encoded by HCMV to counter the host's adaptive immune responses, a feature that facilitates frequent super-infections. Understanding the evolutionary dynamics of HCMV is essential for the development of effective new drugs and vaccines. By comparing viral genomes fromuncultivated or low-passaged clinical samples of diverse origins, we observe evidence of frequent homologous recombination events, both recent and ancient, and no structure of HCMV genetic diversity at the whole-genome scale. Analysis of individual gene-scale loci reveals a striking dichotomy: while most of the genome is highly conserved, recombines essentially freely and has evolved under purifying selection, 21 genes display extreme diversity, structured into distinct genotypes that do not recombine with each other. Most of these hyper-variable genes encode glycoproteins involved in cell entry or escape of host immunity. Evidence that half of themhave diverged through episodes of intense positive selection suggests that rapid evolution of hyper-variable loci is likely driven by interactions with host immunity. It appears that this process is enabled by recombination unlinking hyper-variable loci from strongly constrained neighboring sites. It is conceivable that viralmechanisms facilitating super-infection have evolved to promote recombination between diverged genotypes, allowing the virus to continuously diversify at key loci to escape immune detection, whilemaintaining a genome optimally adapted to its asymptomatic infectious lifecycle.",

keywords = "CMV, immune evasion, recombination, viral evolution",

author = "Florent Lassalle and Depledge, {Daniel P.} and Reeves, {Matthew B.} and Brown, {Amanda C.} and Christiansen, {Mette T.} and Tutill, {Helena J.} and Williams, {Rachel J.} and Katja Einer-Jensen and Jolyon Holdstock and Claire Atkinson and Brown, {Julianne R.} and {Van Loenen}, {Freek B.} and Clark, {Duncan A.} and Griffiths, {Paul D.} and Verjans, {Georges M.G.M.} and Martin Schutten and Milne, {Richard S.B.} and Francois Balloux and Judith Breuer",

note = "Publisher Copyright: {\textcopyright} The Author, 2016.",

year = "2016",

month = jun,

day = "15",

doi = "10.1093/ve/vew017",

language = "English",

volume = "2",

journal = "Virus Evolution",

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Lassalle, F, Depledge, DP, Reeves, MB, Brown, AC, Christiansen, MT, Tutill, HJ, Williams, RJ, Einer-Jensen, K, Holdstock, J, Atkinson, C, Brown, JR, Van Loenen, FB, Clark, DA, Griffiths, PD, Verjans, GMGM, Schutten, M, Milne, RSB, Balloux, F & Breuer, J 2016, 'Islands of linkage in an ocean of pervasive recombination reveals two-speed evolution of human cytomegalovirus genomes', Virus Evolution, vol. 2, no. 1, vew017. https://doi.org/10.1093/ve/vew017, https://doi.org/10.1093/ve/vew017

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T1 - Islands of linkage in an ocean of pervasive recombination reveals two-speed evolution of human cytomegalovirus genomes

AU - Lassalle, Florent

AU - Depledge, Daniel P.

AU - Reeves, Matthew B.

AU - Brown, Amanda C.

AU - Christiansen, Mette T.

AU - Tutill, Helena J.

AU - Williams, Rachel J.

AU - Einer-Jensen, Katja

AU - Holdstock, Jolyon

AU - Atkinson, Claire

AU - Brown, Julianne R.

AU - Van Loenen, Freek B.

AU - Clark, Duncan A.

AU - Griffiths, Paul D.

AU - Verjans, Georges M.G.M.

AU - Schutten, Martin

AU - Milne, Richard S.B.

AU - Balloux, Francois

AU - Breuer, Judith

PY - 2016/6/15

Y1 - 2016/6/15

N2 - Human cytomegalovirus (HCMV) infects most of the population worldwide, persisting throughout the host's life in a latent state with periodic episodes of reactivation. While typically asymptomatic, HCMV can cause fatal disease among congenitally infected infants and immunocompromised patients. These clinical issues are compounded by the emergence of antiviral resistance and the absence of an effective vaccine, the development of which is likely complicated by the numerous immune evasins encoded by HCMV to counter the host's adaptive immune responses, a feature that facilitates frequent super-infections. Understanding the evolutionary dynamics of HCMV is essential for the development of effective new drugs and vaccines. By comparing viral genomes fromuncultivated or low-passaged clinical samples of diverse origins, we observe evidence of frequent homologous recombination events, both recent and ancient, and no structure of HCMV genetic diversity at the whole-genome scale. Analysis of individual gene-scale loci reveals a striking dichotomy: while most of the genome is highly conserved, recombines essentially freely and has evolved under purifying selection, 21 genes display extreme diversity, structured into distinct genotypes that do not recombine with each other. Most of these hyper-variable genes encode glycoproteins involved in cell entry or escape of host immunity. Evidence that half of themhave diverged through episodes of intense positive selection suggests that rapid evolution of hyper-variable loci is likely driven by interactions with host immunity. It appears that this process is enabled by recombination unlinking hyper-variable loci from strongly constrained neighboring sites. It is conceivable that viralmechanisms facilitating super-infection have evolved to promote recombination between diverged genotypes, allowing the virus to continuously diversify at key loci to escape immune detection, whilemaintaining a genome optimally adapted to its asymptomatic infectious lifecycle.

AB - Human cytomegalovirus (HCMV) infects most of the population worldwide, persisting throughout the host's life in a latent state with periodic episodes of reactivation. While typically asymptomatic, HCMV can cause fatal disease among congenitally infected infants and immunocompromised patients. These clinical issues are compounded by the emergence of antiviral resistance and the absence of an effective vaccine, the development of which is likely complicated by the numerous immune evasins encoded by HCMV to counter the host's adaptive immune responses, a feature that facilitates frequent super-infections. Understanding the evolutionary dynamics of HCMV is essential for the development of effective new drugs and vaccines. By comparing viral genomes fromuncultivated or low-passaged clinical samples of diverse origins, we observe evidence of frequent homologous recombination events, both recent and ancient, and no structure of HCMV genetic diversity at the whole-genome scale. Analysis of individual gene-scale loci reveals a striking dichotomy: while most of the genome is highly conserved, recombines essentially freely and has evolved under purifying selection, 21 genes display extreme diversity, structured into distinct genotypes that do not recombine with each other. Most of these hyper-variable genes encode glycoproteins involved in cell entry or escape of host immunity. Evidence that half of themhave diverged through episodes of intense positive selection suggests that rapid evolution of hyper-variable loci is likely driven by interactions with host immunity. It appears that this process is enabled by recombination unlinking hyper-variable loci from strongly constrained neighboring sites. It is conceivable that viralmechanisms facilitating super-infection have evolved to promote recombination between diverged genotypes, allowing the virus to continuously diversify at key loci to escape immune detection, whilemaintaining a genome optimally adapted to its asymptomatic infectious lifecycle.

KW - CMV

KW - immune evasion

KW - recombination

KW - viral evolution

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U2 - 10.1093/ve/vew017

DO - 10.1093/ve/vew017

M3 - Article

SN - 2057-1577

VL - 2

JO - Virus Evolution

JF - Virus Evolution

IS - 1

M1 - vew017

ER -

Islands of linkage in an ocean of pervasive recombination reveals two-speed evolution of human cytomegalovirus genomes

Abstract

Bibliographical note

Keywords

UN SDGs

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