Your search keyword '"Andrésdóttir V"' showing total 23 results

1. Lineage-Specific Viral Hijacking of Non-canonical E3Ubiquitin Ligase Cofactors in the Evolution of Vif Anti-APOBEC3 Activity

Author

Kane, JR, Stanley, DJ, Hultquist, JF, Johnson, JR, Mietrach, N, Binning, JM, Jónsson, SR, Barelier, S, Newton, BW, Johnson, TL, Franks-Skiba, KE, Li, M, Brown, WL, Gunnarsson, HI, Adalbjornsdóttir, A, Fraser, JS, Harris, RS, Andrésdóttir, V, Gross, JD, and Krogan, NJ

Subjects

viruses, virus diseases, biochemical phenomena, metabolism, and nutrition

Abstract

© 2015 The Authors. HIV-1 encodes the accessory protein Vif, which hijacks a host Cullin-RING ubiquitin ligase (CRL) complex as well as the non-canonical cofactor CBFβ, to antagonize APOBEC3 antiviral proteins. Non-canonical cofactor recruitment to CRL complexes by viral factors, to date, has only been attributed to HIV-1 Vif. To further study this phenomenon, we employed a comparative approach combining proteomic, biochemical, structural, and virological techniques to investigate Vif complexes across the lentivirus genus, including primate (HIV-1 and simian immunodeficiency virus macaque [SIVmac]) and non-primate (FIV, BIV, and MVV) viruses. We find that CBFβ is completely dispensable for the activity of non-primate lentiviral Vif proteins. Furthermore, we find that BIV Vif requires no cofactor and that MVV Vif requires a novel cofactor, cyclophilin A (CYPA), for stable CRL complex formation and anti-APOBEC3 activity. We propose modular conservation of Vif complexes allows for potential exaptation of functions through the acquisition of non-CRL-associated host cofactors while preserving anti-APOBEC3 activity. How viral proteins evolve functions without compromising ancestral ones is not well understood. Kane etal. now report that the lentiviral protein Vif has evolved to hijack host factors in a lineage-specific manner while conserving an ancestral viral-host complex promoting viral infection.

Published

2014

2. Use of B7 costimulatory molecules as adjuvants in a prime-boost vaccination against Visna/Maedi ovine lentivirus

Author

de Andrés, X, Reina, R, Ciriza, J, Crespo, H, Glaria, I, Ramírez, H, Grilló, Mj, Pérez, Mm, Andrésdóttir, V, Rosati, Sergio, Suzan Monti, M, Luján, L, Blacklaws, Ba, Harkiss, Gd, de Andrés, D, and Amorena, B.

Published

2009

3. Renibacterium salmoninarum, the causative agent of bacterial kidney disease in salmonid fish, detected by nested reverse transcription-PCR of 16S rRNA sequences

Author

Magnússon, H B, primary, Fridjónsson, O H, additional, Andrésson, O S, additional, Benediktsdóttir, E, additional, Gudmundsdóttir, S, additional, and Andrésdóttir, V, additional

Published

1994

4. The effect of maternal immunity on the equine gammaherpesvirus type 2 and 5 viral load and antibody response.

Author

Thorsteinsdóttir L, Jónsdóttir S, Stefánsdóttir SB, Andrésdóttir V, Wagner B, Marti E, Torsteinsdóttir S, and Svansson V

Subjects

Animals, Female, Gammaherpesvirinae immunology, Gammaherpesvirinae pathogenicity, Herpesviridae Infections immunology, Herpesviridae Infections veterinary, Herpesviridae Infections virology, Horse Diseases immunology, Horse Diseases virology, Horses immunology, Immunity, Maternally-Acquired, Viral Load immunology, Viral Load veterinary

Abstract

Two types of gammaherpesviruses (γEHV) are known to infect horses, EHV-2 and EHV-5. Foals become infected early in life, probably via the upper respiratory tract, despite maternal antibodies. In this study, we analyzed samples from a herd of mares and their foals. The foals were followed from birth to 22 months of age and the dams during the first 6 months postpartum. Blood and nasal swab samples were taken regularly for evaluation of antibody responses, virus isolation and viral load by qPCR. EHV-2 was isolated on day 5, and EHV-5 on day 12, earlier than previously reported. γEHV specific antibodies were not detectable in serum of foals before colostrum intake but peaked a few days after colostrum. Overall, EHV-2 viral load peaked in nasal swab at three to four months of age, paralleled with decline in maternal antibodies, but EHV-5 viral load did not peak until month 12. Maternal antibodies had a notable effect on the viral load and induction of endogenous antibody production. Foals were grouped in two groups depending on the mare's γEHV specific total IgG levels in serum at birth, group-high and group-low. Group-high had higher levels of maternal γEHV specific total IgG and IgG4/7 for the first 3 months, but when the endogenous production had superseded maternal antibodies, group-low was higher. The maternal antibodies had an effect on the γEHV viral load. Group-low peaked in EHV-2 viral load one month earlier than group-high. These effects were more evident for EHV-5, as there were seven months between the viral load peaks for the groups. The study provides information on how maternal antibody transfer affects γEHV shedding and antibody production in offspring. It also extends our knowledge on the occurrence of EHV-2 and EHV-5 infection in foals during the first two years of life., Competing Interests: The authors have declared that no competing interests exist.

Published

2019

5. Characterization of Ovine A3Z1 Restriction Properties against Small Ruminant Lentiviruses (SRLVs).

Author

de Pablo-Maiso L, Glaria I, Crespo H, Nistal-Villán E, Andrésdóttir V, de Andrés D, Amorena B, and Reina R

Subjects

Alternative Splicing genetics, Animals, Cytosine Deaminase chemistry, Cytosine Deaminase metabolism, Gene Expression Regulation, Haplorhini, Humans, Interferon-gamma pharmacology, Macrophages drug effects, Macrophages virology, Nucleotide Motifs genetics, Protein Isoforms genetics, Sheep, Cytosine Deaminase genetics, Lentivirus physiology, Virus Replication

Abstract

Intrinsic factors of the innate immune system include the apolipoprotein B editing enzyme catalytic polypeptide-like 3 (APOBEC3) protein family. APOBEC3 inhibits replication of different virus families by cytosine deamination of viral DNA and a not fully characterized cytosine deamination-independent mechanism. Sheep are susceptible to small ruminant lentivirus (SRLVs) infection and contain three APOBEC3 genes encoding four proteins (A3Z1, Z2, Z3 and Z2-Z3) with yet not deeply described antiviral properties. Using sheep blood monocytes and in vitro-derived macrophages, we found that A3Z1 expression is associated with lower viral replication in this cellular type. A3Z1 transcripts may also contain spliced variants (A3Z1Tr) lacking the cytidine deaminase motif. A3Z1 exogenous expression in fully permissive fibroblast-like cells restricted SRLVs infection while A3Z1Tr allowed infection. A3Z1Tr was induced after SRLVs infection or stimulation of blood-derived macrophages with interferon gamma (IFN-γ). Interaction between truncated isoform and native A3Z1 protein was detected as well as incorporation of both proteins into virions. A3Z1 and A3Z1Tr interacted with SRLVs Vif, but this interaction was not associated with degradative properties. Similar A3Z1 truncated isoforms were also present in human and monkey cells suggesting a conserved alternative splicing regulation in primates. A3Z1-mediated retroviral restriction could be constrained by different means, including gene expression and specific alternative splicing regulation, leading to truncated protein isoforms lacking a cytidine-deaminase motif., Competing Interests: The authors declare no conflict of interest.

Published

2017

6. Two mutations in the vif gene of maedi-visna virus have different phenotypes, indicating more than one function of Vif.

Author

Franzdóttir SR, Ólafsdóttir K, Jónsson SR, Strobel H, Andrésson ÓS, and Andrésdóttir V

Subjects

Capsid Proteins genetics, Phenotype, Visna-maedi virus genetics, Gene Products, vif genetics, Mutation, Missense, Point Mutation, Virus Replication, Visna-maedi virus physiology

Abstract

Like most other lentiviruses, maedi-visna virus (MVV) requires Vif for replication in natural target cells and in vivo. Here, we show that Vif-deficient MVV accumulates G-A mutations in the sequence context characteristic of ovine APOBEC3, consistent with a role of MVV Vif in neutralizing APOBEC3. We studied two point mutations in the vif gene of MVV. One was a tryptophan to arginine mutation that affects the interaction with APOBEC3 and caused G-A hypermutation. The other mutation was a proline to serine mutation that together with a mutation in the capsid protein caused attenuated replication in fetal ovine synovial (FOS) cells but not in sheep choroid plexus (SCP) cells. There was no hypermutation associated with this mutation. These results suggest that MVV Vif exerts more than one function and that there may be interaction between Vif and the capsid. The results also suggest the involvement of an unknown host factor in MVV Vif function., (Copyright © 2015 Elsevier Inc. All rights reserved.)

Published

2016

7. Lineage-Specific Viral Hijacking of Non-canonical E3 Ubiquitin Ligase Cofactors in the Evolution of Vif Anti-APOBEC3 Activity.

Author

Kane JR, Stanley DJ, Hultquist JF, Johnson JR, Mietrach N, Binning JM, Jónsson SR, Barelier S, Newton BW, Johnson TL, Franks-Skiba KE, Li M, Brown WL, Gunnarsson HI, Adalbjornsdóttir A, Fraser JS, Harris RS, Andrésdóttir V, Gross JD, and Krogan NJ

Subjects

APOBEC Deaminases, Animals, Cytidine Deaminase, Humans, Protein Binding, Sheep, Ubiquitin-Protein Ligases genetics, Cytosine Deaminase antagonists & inhibitors, Gene Products, vif immunology, HIV-1 metabolism, Ubiquitin-Protein Ligases metabolism

Abstract

HIV-1 encodes the accessory protein Vif, which hijacks a host Cullin-RING ubiquitin ligase (CRL) complex as well as the non-canonical cofactor CBFβ, to antagonize APOBEC3 antiviral proteins. Non-canonical cofactor recruitment to CRL complexes by viral factors, to date, has only been attributed to HIV-1 Vif. To further study this phenomenon, we employed a comparative approach combining proteomic, biochemical, structural, and virological techniques to investigate Vif complexes across the lentivirus genus, including primate (HIV-1 and simian immunodeficiency virus macaque [SIVmac]) and non-primate (FIV, BIV, and MVV) viruses. We find that CBFβ is completely dispensable for the activity of non-primate lentiviral Vif proteins. Furthermore, we find that BIV Vif requires no cofactor and that MVV Vif requires a novel cofactor, cyclophilin A (CYPA), for stable CRL complex formation and anti-APOBEC3 activity. We propose modular conservation of Vif complexes allows for potential exaptation of functions through the acquisition of non-CRL-associated host cofactors while preserving anti-APOBEC3 activity., (Copyright © 2015 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2015

8. Host restriction of lentiviruses and viral countermeasures: APOBEC3 and Vif.

Author

Jónsson SR and Andrésdóttir V

Subjects

Animals, Sheep, Sheep Diseases immunology, Sheep Diseases virology, Cytosine Deaminase immunology, Cytosine Deaminase metabolism, Gene Products, vif metabolism, Host-Pathogen Interactions, Virulence Factors metabolism, Visna-maedi virus immunology

Abstract

It is becoming increasingly clear that organisms have developed a variety of mechanisms to fight against viral infection. The viruses have developed means of counteracting these defences in various ways. The APOBEC3 proteins are a mammalian-specific family of nucleic acid cytidine deaminases that block retroviral infection. These inhibitors are counteracted by the Vif proteins encoded by most lentiviruses. In this paper, we will review the interaction of the lentiviral Vif proteins with the APOBEC3 proteins, with an emphasis on sheep APOBEC3 and maedi-visna virus (MVV) Vif.

Published

2013

9. Lentiviral Vif degrades the APOBEC3Z3/APOBEC3H protein of its mammalian host and is capable of cross-species activity.

Author

Larue RS, Lengyel J, Jónsson SR, Andrésdóttir V, and Harris RS

Subjects

Animals, Cats, Cattle, Humans, Macaca, Sheep, Cytosine Deaminase antagonists & inhibitors, Gene Products, vif metabolism, Lentivirus pathogenicity, Virulence Factors metabolism

Abstract

All lentiviruses except equine infectious anemia virus (EIAV) use the small accessory protein Vif to counteract the restriction activity of the relevant APOBEC3 (A3) proteins of their host species. Prior studies have suggested that the Vif-A3 interaction is species specific. Here, using the APOBEC3H (Z3)-type proteins from five distinct mammals, we report that this is generally not the case: some lentiviral Vif proteins are capable of triggering the degradation of both the A3Z3-type protein of their normal host species and those of several other mammals. For instance, SIV(mac) Vif can mediate the degradation of the human, macaque, and cow A3Z3-type proteins but not of the sheep or cat A3Z3-type proteins. Maedi-visna virus (MVV) Vif is similarly promiscuous, degrading not only sheep A3Z3 but also the A3Z3-type proteins of humans, macaques, cows, and cats. In contrast to the neutralization capacity of these Vif proteins, human immunodeficiency virus (HIV), bovine immunodeficiency virus (BIV), and feline immunodeficiency virus (FIV) Vif appear specific to the A3Z3-type protein of their hosts. We conclude, first, that the Vif-A3Z3 interaction can be promiscuous and, second, despite this tendency, that each lentiviral Vif protein is optimized to degrade the A3Z3 protein of its mammalian host. Our results thereby suggest that the Vif-A3Z3 interaction is relevant to lentivirus biology.

Published

2010

10. Guidelines for naming nonprimate APOBEC3 genes and proteins.

Author

LaRue RS, Andrésdóttir V, Blanchard Y, Conticello SG, Derse D, Emerman M, Greene WC, Jónsson SR, Landau NR, Löchelt M, Malik HS, Malim MH, Münk C, O'Brien SJ, Pathak VK, Strebel K, Wain-Hobson S, Yu XF, Yuhki N, and Harris RS

Subjects

Animals, Mammals, Cytosine Deaminase, Terminology as Topic

Published

2009

11. The artiodactyl APOBEC3 innate immune repertoire shows evidence for a multi-functional domain organization that existed in the ancestor of placental mammals.

Author

LaRue RS, Jónsson SR, Silverstein KA, Lajoie M, Bertrand D, El-Mabrouk N, Hötzel I, Andrésdóttir V, Smith TP, and Harris RS

Subjects

APOBEC Deaminases, Animals, Base Sequence, Catalysis, Cattle, Conserved Sequence, Cytidine Deaminase, Cytosine Deaminase metabolism, Female, Gene Duplication, Genome genetics, Humans, Models, Genetic, Molecular Sequence Data, Promoter Regions, Genetic, Protein Structure, Tertiary, Protein Transport, RNA, Messenger genetics, RNA, Messenger metabolism, Recombination, Genetic genetics, Selection, Genetic, Sheep, Domestic, Swine, Artiodactyla genetics, Artiodactyla immunology, Cytosine Deaminase chemistry, Cytosine Deaminase genetics, Immunity, Innate genetics, Phylogeny, Placenta metabolism

Abstract

Background: APOBEC3 (A3) proteins deaminate DNA cytosines and block the replication of retroviruses and retrotransposons. Each A3 gene encodes a protein with one or two conserved zinc-coordinating motifs (Z1, Z2 or Z3). The presence of one A3 gene in mice (Z2-Z3) and seven in humans, A3A-H (Z1a, Z2a-Z1b, Z2b, Z2c-Z2d, Z2e-Z2f, Z2g-Z1c, Z3), suggests extraordinary evolutionary flexibility. To gain insights into the mechanism and timing of A3 gene expansion and into the functional modularity of these genes, we analyzed the genomic sequences, expressed cDNAs and activities of the full A3 repertoire of three artiodactyl lineages: sheep, cattle and pigs., Results: Sheep and cattle have three A3 genes, A3Z1, A3Z2 and A3Z3, whereas pigs only have two, A3Z2 and A3Z3. A comparison between domestic and wild pigs indicated that A3Z1 was deleted in the pig lineage. In all three species, read-through transcription and alternative splicing also produced a catalytically active double domain A3Z2-Z3 protein that had a distinct cytoplasmic localization. Thus, the three A3 genes of sheep and cattle encode four conserved and active proteins. These data, together with phylogenetic analyses, indicated that a similar, functionally modular A3 repertoire existed in the common ancestor of artiodactyls and primates (i.e., the ancestor of placental mammals). This mammalian ancestor therefore possessed the minimal A3 gene set, Z1-Z2-Z3, required to evolve through a remarkable series of eight recombination events into the present day eleven Z domain human repertoire., Conclusion: The dynamic recombination-filled history of the mammalian A3 genes is consistent with the modular nature of the locus and a model in which most of these events (especially the expansions) were selected by ancient pathogenic retrovirus infections.

Published

2008

12. Mutational analysis of a principal neutralization domain of visna/maedi virus envelope glycoprotein.

Author

Haflidadóttir BS, Matthíasdóttir S, Agnarsdóttir G, Torsteinsdóttir S, Pétursson G, Andrésson ÓS, and Andrésdóttir V

Subjects

Amino Acid Sequence, Animals, Antibodies, Viral blood, Cell Line, Cells, Cultured, Choroid Plexus cytology, Choroid Plexus virology, Glycosylation, Immunodominant Epitopes chemistry, Immunodominant Epitopes genetics, Immunodominant Epitopes immunology, Molecular Sequence Data, Neutralization Tests, Pneumonia, Progressive Interstitial, of Sheep immunology, Pneumonia, Progressive Interstitial, of Sheep virology, Sheep, Viral Envelope Proteins chemistry, Viral Envelope Proteins metabolism, Visna-maedi virus immunology, Antibodies, Viral immunology, Cysteine chemistry, Mutation, Viral Envelope Proteins genetics, Viral Envelope Proteins immunology, Visna-maedi virus genetics

Abstract

We have shown previously that a type-specific neutralization domain is located within a 39 aa sequence in the fourth variable domain of gp135 in visna/maedi virus. We now show that neutralizing antibodies detected early in infection are directed to this epitope, suggesting an immunodominant nature of this domain. Ten antigenic variants were previously analysed for mutations in this region, and all but one were found to be mutated. To assess the importance of these mutations in replication and neutralization, we reconstructed several of the mutations in an infectious molecular clone and tested the resulting viruses for neutralization phenotype and replication. Mutation of a conserved cysteine was shown to alter the neutralization epitope, whilst the replication kinetics in macrophages were unchanged. Mutations modulating potential glycosylation sites were found in seven of the ten antigenic variants. A frequently occurring mutation, removing a potential glycosylation site, had no effect on its own on the neutralization phenotype of the virus. However, adding an extra potential glycosylation site in the region resulted in antigenic escape. The results indicate that the conserved cysteine plays a role in the structure of the epitope and that glycosylation may shield the principal neutralization site.

Published

2008

13. The restriction of zoonotic PERV transmission by human APOBEC3G.

Author

Jónsson SR, LaRue RS, Stenglein MD, Fahrenkrug SC, Andrésdóttir V, and Harris RS

Subjects

APOBEC-3G Deaminase, Animals, Base Sequence, Cell Transformation, Viral, Coculture Techniques, Cytidine Deaminase genetics, Cytidine Deaminase metabolism, DNA Primers, Genetic Variation, Humans, Polymerase Chain Reaction, Subcellular Fractions metabolism, Swine, Cytidine Deaminase physiology, Endogenous Retroviruses pathogenicity, Zoonoses

Abstract

The human APOBEC3G protein is an innate anti-viral factor that can dominantly inhibit the replication of some endogenous and exogenous retroviruses. The prospects of purposefully harnessing such an anti-viral defense are under investigation. Here, long-term co-culture experiments were used to show that porcine endogenous retrovirus (PERV) transmission from pig to human cells is reduced to nearly undetectable levels by expressing human APOBEC3G in virus-producing pig kidney cells. Inhibition occurred by a deamination-independent mechanism, likely after particle production but before the virus could immortalize by integration into human genomic DNA. PERV inhibition did not require the DNA cytosine deaminase activity of APOBEC3G and, correspondingly, APOBEC3G-attributable hypermutations were not detected. In contrast, over-expression of the sole endogenous APOBEC3 protein of pigs failed to interfere significantly with PERV transmission. Together, these data constitute the first proof-of-principle demonstration that APOBEC3 proteins can be used to fortify the innate anti-viral defenses of cells to prevent the zoonotic transmission of an endogenous retrovirus. These studies suggest that human APOBEC3G-transgenic pigs will provide safer, PERV-less xenotransplantation resources and that analogous cross-species APOBEC3-dependent restriction strategies may be useful for thwarting other endogenous as well as exogenous retrovirus infections.

Published

2007

14. Duplicated sequence motif in the long terminal repeat of maedi-visna virus extends cell tropism and is associated with neurovirulence.

Author

Oskarsson T, Hreggvidsdóttir HS, Agnarsdóttir G, Matthíasdóttir S, Ogmundsdóttir MH, Jónsson SR, Georgsson G, Ingvarsson S, Andrésson OS, and Andrésdóttir V

Subjects

Animals, Base Sequence, Cells, Cultured, Choroid Plexus cytology, Molecular Sequence Data, Pneumonia, Progressive Interstitial, of Sheep virology, Sequence Deletion, Sheep, Domestic, Visna virology, Visna-maedi virus genetics, Visna-maedi virus isolation & purification, Choroid Plexus virology, Terminal Repeat Sequences genetics, Visna-maedi virus pathogenicity, Visna-maedi virus physiology

Abstract

Maedi-visna virus (MVV) is a lentivirus of sheep causing chronic inflammatory disease of the lungs (maedi) and the nervous system (visna). We have previously shown that a duplicated sequence in the long terminal repeat (LTR) of MVV is a determinant of cell tropism. Here, we demonstrate that deletion of a CAAAT sequence from either one of the repeats resulted in poor virus growth in sheep choroid plexus cells. A duplication in the LTR encompassing the CAAAT sequence was found in four neurological field cases that were sequenced, but no duplication was present in the LTRs from seven maedi cases; one maedi isolate was mixed. These results indicate that the duplication in the LTR is associated with neurovirulence.

Published

2007

15. Evolutionarily conserved and non-conserved retrovirus restriction activities of artiodactyl APOBEC3F proteins.

Author

Jónsson SR, Haché G, Stenglein MD, Fahrenkrug SC, Andrésdóttir V, and Harris RS

Subjects

Amino Acid Sequence, Animals, Catalysis, Cattle, Cytoplasm enzymology, Cytosine Deaminase genetics, Cytosine Deaminase metabolism, Deamination, Gene Products, vif metabolism, HeLa Cells, Humans, Molecular Sequence Data, Mutation, Phylogeny, Protein Structure, Tertiary, Sequence Alignment, Sheep genetics, Swine genetics, Zinc chemistry, Artiodactyla genetics, Cytosine Deaminase chemistry, Evolution, Molecular, Retroviridae genetics

Abstract

The APOBEC3 proteins are unique to mammals. Many inhibit retrovirus infection through a cDNA cytosine deamination mechanism. HIV-1 neutralizes this host defense through Vif, which triggers APOBEC3 ubiquitination and degradation. Here, we report an APOBEC3F-like, double deaminase domain protein from three artiodactyls: cattle, pigs and sheep. Like their human counterparts, APOBEC3F and APOBEC3G, the artiodactyl APOBEC3F proteins are DNA cytosine deaminases that locate predominantly to the cytosol and can inhibit the replication of HIV-1 and MLV. Retrovirus restriction is attributable to deaminase-dependent and -independent mechanisms, as deaminase-defective mutants retain significant anti-retroviral activity. However, unlike human APOBEC3F and APOBEC3G, the artiodactyl APOBEC3F proteins have an active N-terminal DNA cytosine deaminase domain, which elicits a broader dinucleotide deamination preference, and they are resistant to HIV-1 Vif. These data indicate that DNA cytosine deamination; sub-cellular localization and retrovirus restriction activities are conserved in mammals, whereas active site location, local mutational preferences and Vif susceptibility are not. Together, these studies indicate that some properties of the mammal-specific, APOBEC3-dependent retroelement restriction system are necessary and conserved, but others are simultaneously modular and highly adaptable.

Published

2006

16. Simultaneous mutations in CA and Vif of Maedi-Visna virus cause attenuated replication in macrophages and reduced infectivity in vivo.

Author

Gudmundsson B, Jónsson SR, Olafsson O, Agnarsdóttir G, Matthíasdóttir S, Georgsson G, Torsteinsdóttir S, Svansson V, Kristbjornsdóttir HB, Franzdóttir SR, Andrésson OS, and Andrésdóttir V

Subjects

Animals, DNA, Viral analysis, Gene Products, vif genetics, Genome, Viral, Mutation, Sheep, Sheep Diseases virology, Virus Replication, Visna-maedi virus pathogenicity, Gene Products, vif physiology, Macrophages virology, Visna-maedi virus physiology

Abstract

Maedi-visna virus (MVV) is a lentivirus of sheep sharing several key features with the primate lentiviruses. The virus causes slowly progressive diseases, mainly in the lungs and the central nervous system of sheep. Here, we investigate the molecular basis for the differential growth phenotypes of two MVV isolates. One of the isolates, KV1772, replicates well in a number of cell lines and is highly pathogenic in sheep. The second isolate, KS1, no longer grows on macrophages or causes disease. The two virus isolates differ by 129 nucleotide substitutions and two deletions of 3 and 15 nucleotides in the env gene. To determine the molecular nature of the lesions responsible for the restrictive growth phenotype, chimeric viruses were constructed and used to map the phenotype. An L120R mutation in the CA domain, together with a P205S mutation in Vif (but neither alone), could fully convert KV1772 to the restrictive growth phenotype. These results suggest a functional interaction between CA and Vif in MVV replication, a property that may relate to the innate antiretroviral defense mechanisms in sheep.

Published

2005

17. The vif gene of maedi-visna virus is essential for infectivity in vivo and in vitro.

Author

Kristbjörnsdóttir HB, Andrésdóttir V, Svansson V, Torsteinsdóttir S, Matthíasdóttir S, and Andrésson OS

Subjects

Amino Acid Sequence, Animals, Base Sequence, Cells, Cultured, Choroid Plexus cytology, Choroid Plexus virology, Gene Deletion, Gene Products, vif genetics, Molecular Sequence Data, Pneumonia, Progressive Interstitial, of Sheep virology, Sheep, Sheep Diseases virology, Virus Replication, Gene Products, vif metabolism, Genes, Essential, Pneumonia, Progressive Interstitial, of Sheep physiopathology, Visna-maedi virus pathogenicity

Abstract

We have investigated the role of vif in maedi-visna virus (MVV), a lentivirus of sheep, by studying in vitro replication of vif-deleted MVV in several cell types, and the effects of vif deletion on in vivo infection. By measuring RT activity, we found that in comparison to wild-type MVV, growth of vif-deleted MVV was similar in fetal ovine synovial (FOS) cells, highly attenuated in sheep choroid plexus (SCP) cells, and not detectable in macrophages, natural target cells of MVV. Productive infection by vif-deleted MVV could not be demonstrated in sheep. An increased mutation frequency was observed in DNA produced by endogenous reverse transcription of viral RNA in vif-deleted virions, indicating the existence of a factor comparable in action to human APOBEC3G. These results suggest that the vif gene of MVV is essential for infectivity and that the Vif protein protects the viral genome from enpackaged mutagenic activities.

Published

2004

18. Selection of antigenic variants in maedi-visna virus infection.

Author

Andrésdóttir V, Skraban R, Matthíasdóttir S, Lutley R, Agnarsdóttir G, and Thorsteinsdóttir H

Subjects

Amino Acid Sequence, Animals, Antibodies, Viral immunology, Antigenic Variation immunology, Cell Line, Molecular Sequence Data, Neutralization Tests, Pneumonia, Progressive Interstitial, of Sheep immunology, Sequence Analysis, DNA, Sheep, Time Factors, Virus Replication, Visna-maedi virus immunology, Visna-maedi virus isolation & purification, Visna-maedi virus physiology, Antigenic Variation genetics, Genes, env, Pneumonia, Progressive Interstitial, of Sheep virology, Visna-maedi virus genetics

Abstract

In order to analyse the pattern of sequence variation in maedi-visna virus (MVV) in persistently infected sheep and to answer the question of whether antigenic variants are selected in a long-term MVV infection, an 87 bp variable region in the env gene of ten antigenic variants and 24 non-variants was sequenced. Nine of the ten antigenic variants had mutations in this region, comprising 24 point mutations and a deletion of 3 bp. Twenty-three of the point mutations (96%) were non-synonymous. There was only a single mutation in this region in the 24 non-variants. A type-specific neutralizing antibody response appeared in all the sheep 2-5 months post-infection, and in most sheep more broadly reacting neutralizing antibodies appeared up to 4 years later. All the antigenic variants were neutralized by the broadly reacting sera. It is noteworthy that the antigenic variants were isolated at a time when only the type-specific antibodies were acting, before the broadly reacting antibodies appeared. The same picture emerged when molecularly cloned virus was used for infection. Three sheep were infected with a molecularly cloned virus, and of six virus isolates, one was an antigenic variant. This variant arose in the absence of broadly reacting antibodies. The results indicate that there is selection for mutants that escape neutralization.

Published

2002

19. The long terminal repeat is a determinant of cell tropism of maedi-visna virus.

Author

Agnarsdóttir G, Thorsteinsdóttir H, Óskarsson T, Matthíasdóttir S, St Haflidadóttir B, Andrésson ÓS, and Andrésdóttir V

Subjects

Animals, Base Sequence, Molecular Sequence Data, Polymerase Chain Reaction, Sheep, Visna-maedi virus physiology, Terminal Repeat Sequences, Visna-maedi virus genetics

Abstract

Maedi-visna virus (MVV) is a lentivirus of sheep, mainly affecting the lungs and the central nervous system. Long terminal repeat (LTR) sequence variability is common in tissue culture-derived isolates of MVV as well as those of other lentiviruses. The role of this sequence variation in MVV replication has not been explored. PCR amplification of the LTRs of an MVV isolate revealed two product sizes, the larger containing a 53 bp duplication. PCR products containing the two size variants of the LTRs were cloned into an infectious molecular clone of MVV and the resulting chimeric viruses were tested for growth in various cell types. The chimeric virus containing only one copy of the 53 bp sequence was found to grow more slowly in sheep choroid plexus cells, sheep fibroblasts and sheep synovial cells than the virus with the 53 bp duplication. Both viruses grew equally well in macrophages. These results indicate that the LTRs determined the extended cell tropism of MVV.

Published

2000

20. Naturally occurring mutations within 39 amino acids in the envelope glycoprotein of maedi-visna virus alter the neutralization phenotype.

Author

Skraban R, Matthíasdóttir S, Torsteinsdóttir S, Agnarsdóttir G, Gudmundsson B, Georgsson G, Meloen RH, Andrésson OS, Staskus KA, Thormar H, and Andrésdóttir V

Subjects

Amino Acid Sequence, Amino Acids genetics, Animals, Molecular Sequence Data, Phenotype, Sequence Alignment, Visna-maedi virus classification, Visna-maedi virus isolation & purification, Point Mutation, Viral Envelope Proteins genetics, Visna-maedi virus genetics

Abstract

Infectious molecular clones have been isolated from two maedi-visna virus (MVV) strains, one of which (KV1772kv72/67) is an antigenic escape mutant of the other (LV1-1KS1). To map the type-specific neutralization epitope, we constructed viruses containing chimeric envelope genes by using KV1772kv72/67 as a backbone and replacing various parts of the envelope gene with equivalent sequences from LV1-1KS1. The neutralization phenotype was found to map to a region in the envelope gene containing two deletions and four amino acid changes within 39 amino acids (positions 559 to 597 of Env). Serum obtained from a lamb infected with a chimeric virus, VR1, containing only the 39 amino acids from LV1-1KS1 in the KV1772kv72/67 backbone neutralized LV1-1KS1 but not KV1772kv72/67. The region in the envelope gene that we had thus shown to be involved in escape from neutralization was cloned into pGEX-3X expression vectors, and the resulting fusion peptides from both molecular clones were tested in immunoblots for reactivity with the KV1772kv72/67 and VR1 type-specific antisera. The type-specific KV1772kv72/67 antiserum reacted only with the fusion peptide from KV1772kv72/67 and not with that from LV1-1KS1, and the type-specific VR1 antiserum reacted only with the fusion peptide from LV1-1KS1 and not with that from KV1772kv72/67. Pepscan analysis showed that the region contained two linear epitopes, one of which was specific to each of the molecularly cloned viruses. This linear epitope was not bound by all type-specific neutralizing antisera, however, which indicates that it is not by itself the neutralization epitope but may be a part of it. These findings show that mutations within amino acids 559 to 597 in the envelope gene of MVV virus result in escape from neutralization. Furthermore, the region contains one or more parts of a discontinuous neutralization epitope.

Published

1999

21. Visna virus dUTPase is dispensable for neuropathogenicity.

Author

Pétursson G, Turelli P, Matthíasdóttir S, Georgsson G, Andrésson OS, Torsteinsdóttir S, Vigne R, Andrésdóttir V, Gunnarsson E, Agnarsdóttir G, and Quérat G

Subjects

Animals, Gene Deletion, Nervous System pathology, Sheep, Virulence genetics, Visna-maedi virus pathogenicity, Nervous System virology, Pyrophosphatases genetics, Visna virology, Visna-maedi virus genetics

Abstract

The major part of the dUTPase-encoding region of the visna virus genome was deleted. Intracerebral injection of the mutant virus resulted in a somewhat reduced viral load compared to that resulting from injection of the wild type, especially in the lungs, but the neuropathogenic effects were comparable. The dUTPase gene is dispensable for induction of lesions in the brain.

Published

1998

22. In vivo and in vitro infection with two different molecular clones of visna virus.

Author

Torsteinsdóttir S, Agnarsdóttir G, Matthíasdóttir S, Rafnar B, Andrésdóttir V, Andrésson OS, Staskus K, Pétursson G, Pálsson PA, and Georgsson G

Subjects

Animals, Antibodies, Viral blood, Cell Line, Macrophages cytology, Sheep, Visna immunology, Visna pathology, Visna-maedi virus immunology, Visna-maedi virus isolation & purification, Macrophages virology, Visna virology, Visna-maedi virus pathogenicity

Abstract

The behavior of two genetically different molecular clones of visna virus KV1772-kv72/67 and LV1-1KS1 was compared in vivo and in vitro. On intracerebral inoculation, clone KV1772-kv72/67 induced a similar response in five sheep as has already been reported with neurovirulent derivates of visna virus. Virus was frequently isolated from blood, cerebrospinal fluid (CSF), and lymphoid organs and induced characteristic central nervous system (CNS) lesions. A strong humoral immune response was detected by ELISA, immunoblotting, and neutralization. Six sheep infected with clone LV1-1KS1 showed a completely different picture. No virus could be isolated from blood or CSF during 6 months of infection. At sacrifice all organs were virus-negative except the CNS of one sheep. None of the six sheep developed significant neutralizing antibodies and only low titer antibodies were detected by ELISA and immunoblotting. Minimal CNS lesions were present in one sheep. The molecular clones were also tested in sheep choroid plexus cells (SCP) and macrophages. In macrophages LV1-1KS1 replicated to a significantly lower titer but induced much more cell fusion than KV1772-kv72/67. The clones replicated equally well in SCP cells. Thus, these molecular clones of visna virus, which differ only by 1% in nucleotide sequence, showed a profound difference in replication and pathogenicity both in vitro and in vivo. These results can be used to map viral genetic determinants important for host-lentivirus interactions.

Published

1997

23. Subclasses of IgG from whales.

Author

Andrésdóttir V, Magnadóttir B, Andrésson OS, and Pétursson G

Subjects

Animals, Chromatography, Ion Exchange, Immunodiffusion, Immunoglobulin G isolation & purification, Molecular Weight, Papain, Pepsin A, Species Specificity, Cetacea immunology, Immunoglobulin G classification, Whales immunology

Published

1987