Mitotic Evolution of Plasmodium falciparum Shows a Stable Core Genome but Recombination in Antigen Families

Malaria parasites elude eradication attempts both within the human host and across nations. At the individual level, parasites evade the host immune responses through antigenic variation. At the global level, parasites escape drug pressure through single nucleotide variants and gene copy amplificati...

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Autores principales: Bopp, Selina E. R., Manary, Micah J., Bright, A. Taylor, Johnston, Geoffrey L., Dharia, Neekesh V., Luna, Fabio L., McCormack, Susan, Plouffe, David, McNamara, Case W., Walker, John R., Fidock, David A., Denchi, Eros Lazzerini, Winzeler, Elizabeth A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3567157/
https://www.ncbi.nlm.nih.gov/pubmed/23408914
http://dx.doi.org/10.1371/journal.pgen.1003293
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author Bopp, Selina E. R.
Manary, Micah J.
Bright, A. Taylor
Johnston, Geoffrey L.
Dharia, Neekesh V.
Luna, Fabio L.
McCormack, Susan
Plouffe, David
McNamara, Case W.
Walker, John R.
Fidock, David A.
Denchi, Eros Lazzerini
Winzeler, Elizabeth A.
author_facet Bopp, Selina E. R.
Manary, Micah J.
Bright, A. Taylor
Johnston, Geoffrey L.
Dharia, Neekesh V.
Luna, Fabio L.
McCormack, Susan
Plouffe, David
McNamara, Case W.
Walker, John R.
Fidock, David A.
Denchi, Eros Lazzerini
Winzeler, Elizabeth A.
author_sort Bopp, Selina E. R.
collection PubMed
description Malaria parasites elude eradication attempts both within the human host and across nations. At the individual level, parasites evade the host immune responses through antigenic variation. At the global level, parasites escape drug pressure through single nucleotide variants and gene copy amplification events conferring drug resistance. Despite their importance to global health, the rates at which these genomic alterations emerge have not been determined. We studied the complete genomes of different Plasmodium falciparum clones that had been propagated asexually over one year in the presence and absence of drug pressure. A combination of whole-genome microarray analysis and next-generation deep resequencing (totaling 14 terabases) revealed a stable core genome with only 38 novel single nucleotide variants appearing in seventeen evolved clones (avg. 5.4 per clone). In clones exposed to atovaquone, we found cytochrome b mutations as well as an amplification event encompassing the P. falciparum multidrug resistance associated protein (mrp1) on chromosome 1. We observed 18 large-scale (>1 kb on average) deletions of telomere-proximal regions encoding multigene families, involved in immune evasion (9.5×10(−6) structural variants per base pair per generation). Six of these deletions were associated with chromosomal crossovers generated during mitosis. We found only minor differences in rates between genetically distinct strains and between parasites cultured in the presence or absence of drug. Using these derived mutation rates for P. falciparum (1.0–9.7×10(−9) mutations per base pair per generation), we can now model the frequency at which drug or immune resistance alleles will emerge under a well-defined set of assumptions. Further, the detection of mitotic recombination events in var gene families illustrates how multigene families can arise and change over time in P. falciparum. These results will help improve our understanding of how P. falciparum evolves to evade control efforts within both the individual hosts and large populations.
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spelling pubmed-35671572013-02-13 Mitotic Evolution of Plasmodium falciparum Shows a Stable Core Genome but Recombination in Antigen Families Bopp, Selina E. R. Manary, Micah J. Bright, A. Taylor Johnston, Geoffrey L. Dharia, Neekesh V. Luna, Fabio L. McCormack, Susan Plouffe, David McNamara, Case W. Walker, John R. Fidock, David A. Denchi, Eros Lazzerini Winzeler, Elizabeth A. PLoS Genet Research Article Malaria parasites elude eradication attempts both within the human host and across nations. At the individual level, parasites evade the host immune responses through antigenic variation. At the global level, parasites escape drug pressure through single nucleotide variants and gene copy amplification events conferring drug resistance. Despite their importance to global health, the rates at which these genomic alterations emerge have not been determined. We studied the complete genomes of different Plasmodium falciparum clones that had been propagated asexually over one year in the presence and absence of drug pressure. A combination of whole-genome microarray analysis and next-generation deep resequencing (totaling 14 terabases) revealed a stable core genome with only 38 novel single nucleotide variants appearing in seventeen evolved clones (avg. 5.4 per clone). In clones exposed to atovaquone, we found cytochrome b mutations as well as an amplification event encompassing the P. falciparum multidrug resistance associated protein (mrp1) on chromosome 1. We observed 18 large-scale (>1 kb on average) deletions of telomere-proximal regions encoding multigene families, involved in immune evasion (9.5×10(−6) structural variants per base pair per generation). Six of these deletions were associated with chromosomal crossovers generated during mitosis. We found only minor differences in rates between genetically distinct strains and between parasites cultured in the presence or absence of drug. Using these derived mutation rates for P. falciparum (1.0–9.7×10(−9) mutations per base pair per generation), we can now model the frequency at which drug or immune resistance alleles will emerge under a well-defined set of assumptions. Further, the detection of mitotic recombination events in var gene families illustrates how multigene families can arise and change over time in P. falciparum. These results will help improve our understanding of how P. falciparum evolves to evade control efforts within both the individual hosts and large populations. Public Library of Science 2013-02-07 /pmc/articles/PMC3567157/ /pubmed/23408914 http://dx.doi.org/10.1371/journal.pgen.1003293 Text en © 2013 Bopp et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Bopp, Selina E. R.
Manary, Micah J.
Bright, A. Taylor
Johnston, Geoffrey L.
Dharia, Neekesh V.
Luna, Fabio L.
McCormack, Susan
Plouffe, David
McNamara, Case W.
Walker, John R.
Fidock, David A.
Denchi, Eros Lazzerini
Winzeler, Elizabeth A.
Mitotic Evolution of Plasmodium falciparum Shows a Stable Core Genome but Recombination in Antigen Families
title Mitotic Evolution of Plasmodium falciparum Shows a Stable Core Genome but Recombination in Antigen Families
title_full Mitotic Evolution of Plasmodium falciparum Shows a Stable Core Genome but Recombination in Antigen Families
title_fullStr Mitotic Evolution of Plasmodium falciparum Shows a Stable Core Genome but Recombination in Antigen Families
title_full_unstemmed Mitotic Evolution of Plasmodium falciparum Shows a Stable Core Genome but Recombination in Antigen Families
title_short Mitotic Evolution of Plasmodium falciparum Shows a Stable Core Genome but Recombination in Antigen Families
title_sort mitotic evolution of plasmodium falciparum shows a stable core genome but recombination in antigen families
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3567157/
https://www.ncbi.nlm.nih.gov/pubmed/23408914
http://dx.doi.org/10.1371/journal.pgen.1003293
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