Deep Sequencing of MHC-Adapted Viral Lines Reveals Complex Recombinational Exchanges With Endogenous Retroviruses Leading to High-Frequency Variants

Deep Sequencing of MHC-Adapted Viral Lines Reveals Complex Recombinational Exchanges With Endogenous Retroviruses Leading to High-Frequency Variants

Experimental evolution (serial passage) of Friend virus complex (FVC) in mice demonstrates phenotypic adaptation to specific host major histocompatibility complex (MHC) genotypes. These evolved viral lines show increased fitness and virulence in their host-genotype-of-passage, but display fitness an...

Full description

Bibliographic Details
Main Authors: Earl A. Middlebrook, Derek L. Stark, Douglas H. Cornwall, Jason L. Kubinak, Wayne K. Potts
Format: Article
Language:English
Published: Frontiers Media S.A. 2021-08-01
Series:Frontiers in Genetics
Subjects:
recombination
ERV
host adaptation
serial passage
Friend virus complex
murine leukemia virus
Online Access:https://www.frontiersin.org/articles/10.3389/fgene.2021.716623/full
id doaj-d8a9aa7cd34b468a9eee35e426af6c09
record_format Article
spelling doaj-d8a9aa7cd34b468a9eee35e426af6c092021-09-03T12:49:44ZengFrontiers Media S.A.Frontiers in Genetics1664-80212021-08-011210.3389/fgene.2021.716623716623Deep Sequencing of MHC-Adapted Viral Lines Reveals Complex Recombinational Exchanges With Endogenous Retroviruses Leading to High-Frequency VariantsEarl A. Middlebrook0Earl A. Middlebrook1Derek L. Stark2Douglas H. Cornwall3Douglas H. Cornwall4Jason L. Kubinak5Wayne K. Potts6School of Biological Sciences, University of Utah, Salt Lake City, UT, United StatesBiosecurity and Public Health, Los Alamos National Laboratory, Los Alamos, NM, United StatesSchool of Biological Sciences, University of Utah, Salt Lake City, UT, United StatesSchool of Biological Sciences, University of Utah, Salt Lake City, UT, United StatesDepartment of Pathology, University of Utah, Salt Lake City, UT, United StatesDepartment of Pathology, Microbiology and Immunology, University of South Carolina School of Medicine, Columbia, SC, United StatesSchool of Biological Sciences, University of Utah, Salt Lake City, UT, United StatesExperimental evolution (serial passage) of Friend virus complex (FVC) in mice demonstrates phenotypic adaptation to specific host major histocompatibility complex (MHC) genotypes. These evolved viral lines show increased fitness and virulence in their host-genotype-of-passage, but display fitness and virulence tradeoffs when infecting unfamiliar host MHC genotypes. Here, we deep sequence these viral lines in an attempt to discover the genetic basis of FVC adaptation. The principal prediction for genotype-specific adaptation is that unique mutations would rise to high frequency in viral lines adapted to each host MHC genotype. This prediction was not supported by our sequencing data as most observed high-frequency variants were present in each of our independently evolved viral lines. However, using a multi-variate approach to measure divergence between viral populations, we show that populations of replicate evolved viral lines from the same MHC congenic mouse strain were more similar to one another than to lines derived from different MHC congenic mouse strains, suggesting that MHC genotype does predictably act on viral evolution in our model. Sequence analysis also revealed rampant recombination with endogenous murine leukemia virus sequences (EnMuLVs) that are encoded within the BALB/c mouse genome. The highest frequency variants in all six lines contained a 12 bp insertion from a recombinant EnMuLV source, suggesting such recombinants were either being favored by selection or were contained in a recombinational hotspot. Interestingly, they did not reach fixation, as if they are low fitness. The amount of background mutations linked to FVC/EnMuLV variable sites indicated that FVC/EnMuLV recombinants had not reached mutation selection equilibrium and thus, that EnMuLV sequences are likely continuously introgressing into the replicating viral population. These discoveries raise the question: is the expression of EnMuLV sequences in mouse splenocytes that permit recombination with exogenous FVC a pathogen or host adaptation?https://www.frontiersin.org/articles/10.3389/fgene.2021.716623/fullrecombinationERVhost adaptationserial passageFriend virus complexmurine leukemia virus
collection DOAJ
language English
format Article
sources DOAJ
author Earl A. Middlebrook
Earl A. Middlebrook
Derek L. Stark
Douglas H. Cornwall
Douglas H. Cornwall
Jason L. Kubinak
Wayne K. Potts
spellingShingle Earl A. Middlebrook
Earl A. Middlebrook
Derek L. Stark
Douglas H. Cornwall
Douglas H. Cornwall
Jason L. Kubinak
Wayne K. Potts
Deep Sequencing of MHC-Adapted Viral Lines Reveals Complex Recombinational Exchanges With Endogenous Retroviruses Leading to High-Frequency Variants
Frontiers in Genetics
recombination
ERV
host adaptation
serial passage
Friend virus complex
murine leukemia virus
author_facet Earl A. Middlebrook
Earl A. Middlebrook
Derek L. Stark
Douglas H. Cornwall
Douglas H. Cornwall
Jason L. Kubinak
Wayne K. Potts
author_sort Earl A. Middlebrook
title Deep Sequencing of MHC-Adapted Viral Lines Reveals Complex Recombinational Exchanges With Endogenous Retroviruses Leading to High-Frequency Variants
title_short Deep Sequencing of MHC-Adapted Viral Lines Reveals Complex Recombinational Exchanges With Endogenous Retroviruses Leading to High-Frequency Variants
title_full Deep Sequencing of MHC-Adapted Viral Lines Reveals Complex Recombinational Exchanges With Endogenous Retroviruses Leading to High-Frequency Variants
title_fullStr Deep Sequencing of MHC-Adapted Viral Lines Reveals Complex Recombinational Exchanges With Endogenous Retroviruses Leading to High-Frequency Variants
title_full_unstemmed Deep Sequencing of MHC-Adapted Viral Lines Reveals Complex Recombinational Exchanges With Endogenous Retroviruses Leading to High-Frequency Variants
title_sort deep sequencing of mhc-adapted viral lines reveals complex recombinational exchanges with endogenous retroviruses leading to high-frequency variants
publisher Frontiers Media S.A.
series Frontiers in Genetics
issn 1664-8021
publishDate 2021-08-01
description Experimental evolution (serial passage) of Friend virus complex (FVC) in mice demonstrates phenotypic adaptation to specific host major histocompatibility complex (MHC) genotypes. These evolved viral lines show increased fitness and virulence in their host-genotype-of-passage, but display fitness and virulence tradeoffs when infecting unfamiliar host MHC genotypes. Here, we deep sequence these viral lines in an attempt to discover the genetic basis of FVC adaptation. The principal prediction for genotype-specific adaptation is that unique mutations would rise to high frequency in viral lines adapted to each host MHC genotype. This prediction was not supported by our sequencing data as most observed high-frequency variants were present in each of our independently evolved viral lines. However, using a multi-variate approach to measure divergence between viral populations, we show that populations of replicate evolved viral lines from the same MHC congenic mouse strain were more similar to one another than to lines derived from different MHC congenic mouse strains, suggesting that MHC genotype does predictably act on viral evolution in our model. Sequence analysis also revealed rampant recombination with endogenous murine leukemia virus sequences (EnMuLVs) that are encoded within the BALB/c mouse genome. The highest frequency variants in all six lines contained a 12 bp insertion from a recombinant EnMuLV source, suggesting such recombinants were either being favored by selection or were contained in a recombinational hotspot. Interestingly, they did not reach fixation, as if they are low fitness. The amount of background mutations linked to FVC/EnMuLV variable sites indicated that FVC/EnMuLV recombinants had not reached mutation selection equilibrium and thus, that EnMuLV sequences are likely continuously introgressing into the replicating viral population. These discoveries raise the question: is the expression of EnMuLV sequences in mouse splenocytes that permit recombination with exogenous FVC a pathogen or host adaptation?
topic recombination
ERV
host adaptation
serial passage
Friend virus complex
murine leukemia virus
url https://www.frontiersin.org/articles/10.3389/fgene.2021.716623/full
work_keys_str_mv AT earlamiddlebrook deepsequencingofmhcadaptedvirallinesrevealscomplexrecombinationalexchangeswithendogenousretrovirusesleadingtohighfrequencyvariants
AT earlamiddlebrook deepsequencingofmhcadaptedvirallinesrevealscomplexrecombinationalexchangeswithendogenousretrovirusesleadingtohighfrequencyvariants
AT dereklstark deepsequencingofmhcadaptedvirallinesrevealscomplexrecombinationalexchangeswithendogenousretrovirusesleadingtohighfrequencyvariants
AT douglashcornwall deepsequencingofmhcadaptedvirallinesrevealscomplexrecombinationalexchangeswithendogenousretrovirusesleadingtohighfrequencyvariants
AT douglashcornwall deepsequencingofmhcadaptedvirallinesrevealscomplexrecombinationalexchangeswithendogenousretrovirusesleadingtohighfrequencyvariants
AT jasonlkubinak deepsequencingofmhcadaptedvirallinesrevealscomplexrecombinationalexchangeswithendogenousretrovirusesleadingtohighfrequencyvariants
AT waynekpotts deepsequencingofmhcadaptedvirallinesrevealscomplexrecombinationalexchangeswithendogenousretrovirusesleadingtohighfrequencyvariants
_version_ 1717817252419469312

Similar Items