Reverse immunodynamics: a new method for identifying targets of protective immunity

Katrina J. Spensley; Paul S. Wikramaratna; Bridget S. Penman; Andrew Walker; Adrian L. Smith; Oliver G. Pybus; Létitia Jean; Sunetra Gupta; José Lourenço

doi:10.1038/s41598-018-37288-x

Reverse immunodynamics: a new method for identifying targets of protective immunity

Katrina J. Spensley
, Paul S. Wikramaratna
, Bridget S. Penman
, Andrew Walker
, Adrian L. Smith
, Oliver G. Pybus
, Létitia Jean
, Sunetra Gupta
, José Lourenço^*

^*Autor correspondente para este trabalho

Resultado de pesquisa › revisão de pares

2 Citações (Scopus)

Resumo

Despite a dramatic increase in our ability to catalogue variation among pathogen genomes, we have made far fewer advances in using this information to identify targets of protective immunity. Epidemiological models predict that strong immune selection can cause antigenic variants to structure into genetically discordant sets of antigenic types (e.g. serotypes). A corollary of this theory is that targets of immunity may be identified by searching for non-overlapping associations of amino acids among co-circulating antigenic variants. We propose a novel population genetics methodology that combines such predictions with phylogenetic analyses to identify genetic loci (epitopes) under strong immune selection. We apply this concept to the AMA-1 protein of the malaria parasite Plasmodium falciparum and find evidence of epitopes among certain regions of low variability which could render them ideal vaccine candidates. The proposed method can be applied to a myriad of multi-strain pathogens for which vast amounts of genetic data has been collected in recent years.

Idioma original	English
Número do artigo	2164
Revista	Scientific Reports
Volume	9
Número de emissão	1
DOIs	https://doi.org/10.1038/s41598-018-37288-x
Estado da publicação	Publicado - 1 dez. 2019
Publicado externamente	Sim

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Reverse immunodynamics: a new method for identifying targets of protective immunity
Spensley, K. J., Wikramaratna, P. S., Penman, B. S., Walker, A., Smith, A. L., Pybus, O. G., Jean, L., Gupta, S. & Lourenço, J., 20 jul. 2017, bioRxiv, 17 p.
Resultado de pesquisa: ???researchoutput.researchoutputtypes.workingpaper.preprint???

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title = "Reverse immunodynamics: a new method for identifying targets of protective immunity",

abstract = "Despite a dramatic increase in our ability to catalogue variation among pathogen genomes, we have made far fewer advances in using this information to identify targets of protective immunity. Epidemiological models predict that strong immune selection can cause antigenic variants to structure into genetically discordant sets of antigenic types (e.g. serotypes). A corollary of this theory is that targets of immunity may be identified by searching for non-overlapping associations of amino acids among co-circulating antigenic variants. We propose a novel population genetics methodology that combines such predictions with phylogenetic analyses to identify genetic loci (epitopes) under strong immune selection. We apply this concept to the AMA-1 protein of the malaria parasite Plasmodium falciparum and find evidence of epitopes among certain regions of low variability which could render them ideal vaccine candidates. The proposed method can be applied to a myriad of multi-strain pathogens for which vast amounts of genetic data has been collected in recent years.",

author = "Spensley, \{Katrina J.\} and Wikramaratna, \{Paul S.\} and Penman, \{Bridget S.\} and Andrew Walker and Smith, \{Adrian L.\} and Pybus, \{Oliver G.\} and L{\'e}titia Jean and Sunetra Gupta and Jos{\'e} Louren{\c c}o",

note = "Funding Information: We thank Dr. CRC Spensley for assistance with data manipulation and programming, and Dr. Pietro Roversi for assistance with generating the structure. JL and SG received funding from the European Research Council under the European Union{\textquoteright}s Seventh Framework Programme (FP7/2007-2013, ERC grant number 268904 - DIVERSITY). Publisher Copyright: {\textcopyright} 2019, The Author(s).",

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AU - Pybus, Oliver G.

AU - Jean, Létitia

AU - Gupta, Sunetra

AU - Lourenço, José

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N2 - Despite a dramatic increase in our ability to catalogue variation among pathogen genomes, we have made far fewer advances in using this information to identify targets of protective immunity. Epidemiological models predict that strong immune selection can cause antigenic variants to structure into genetically discordant sets of antigenic types (e.g. serotypes). A corollary of this theory is that targets of immunity may be identified by searching for non-overlapping associations of amino acids among co-circulating antigenic variants. We propose a novel population genetics methodology that combines such predictions with phylogenetic analyses to identify genetic loci (epitopes) under strong immune selection. We apply this concept to the AMA-1 protein of the malaria parasite Plasmodium falciparum and find evidence of epitopes among certain regions of low variability which could render them ideal vaccine candidates. The proposed method can be applied to a myriad of multi-strain pathogens for which vast amounts of genetic data has been collected in recent years.

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Reverse immunodynamics: a new method for identifying targets of protective immunity

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Reverse immunodynamics: a new method for identifying targets of protective immunity

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