Your search keyword '"Guy Lemay"' showing total 93 results

1. A newly identified interaction between nucleolar NPM1/B23 and the HTLV-I basic leucine zipper factor in HTLV-1 infected cells

Author

Zhenlong Liu, Émilie Larocque, Yongli Xie, Yong Xiao, Guy Lemay, Jean-Marie Peloponese, Jean-Michel Mesnard, Éric Rassart, Rongtuan Lin, Shuang Zhou, Yiming Zeng, Hongzhi Gao, Shan Cen, and Benoit Barbeau

Subjects

HTLV-1, ATLL, HBZ, NPM1/B23, APH-2, nucleolus, Microbiology, QR1-502

Abstract

Human T-cell leukemia virus type 1 is the causative agent of HTLV-1-associated myelopathy/tropical spastic paraparesis and adult T-cell leukemia-lymphoma (ATL). The HTLV-1 basic leucine zipper factor (HBZ) has been associated to the cancer-inducing properties of this virus, although the exact mechanism is unknown. In this study, we identified nucleophosmin (NPM1/B23) as a new interaction partner of HBZ. We show that sHBZ and the less abundant uHBZ isoform interact with nucleolar NPM1/B23 in infected cells and HTLV-1 positive patient cells, unlike equivalent antisense proteins of related non-leukemogenic HTLV-2, −3 and-4 viruses. We further demonstrate that sHBZ association to NPM1/B23 is sensitive to RNase. Interestingly, sHBZ was shown to interact with its own RNA. Through siRNA and overexpression experiments, we further provide evidence that NPM1/B23 acts negatively on viral gene expression with potential impact on cell transformation. Our results hence provide a new insight over HBZ-binding partners in relation to cellular localization and potential function on cell proliferation and should lead to a better understanding of the link between HBZ and ATL development.

Published

2022

2. U5 snRNP Core Proteins Are Key Components of the Defense Response against Viral Infection through Their Roles in Programmed Cell Death and Interferon Induction

Author

Simon Boudreault, Guy Lemay, and Martin Bisaillon

Subjects

reovirus, spliceosome, U5 snRNP, EFTUD2, PRPF8, SNRNP200, Microbiology, QR1-502

Abstract

The spliceosome is a massive ribonucleoprotein structure composed of five small nuclear ribonucleoprotein (snRNP) complexes that catalyze the removal of introns from pre-mature RNA during constitutive and alternative splicing. EFTUD2, PRPF8, and SNRNP200 are core components of the U5 snRNP, which is crucial for spliceosome function as it coordinates and performs the last steps of the splicing reaction. Several studies have demonstrated U5 snRNP proteins as targeted during viral infection, with a limited understanding of their involvement in virus–host interactions. In the present study, we deciphered the respective impact of EFTUD2, PRPF8, and SNRNP200 on viral replication using mammalian reovirus as a model. Using a combination of RNA silencing, real-time cell analysis, cell death and viral replication assays, we discovered distinct and partially overlapping novel roles for EFTUD2, PRPF8, and SNRNP200 in cell survival, apoptosis, necroptosis, and the induction of the interferon response pathway. For instance, we demonstrated that EFTUD2 and SNRNP200 are required for both apoptosis and necroptosis, whereas EFTUD2 and PRPF8 are required for optimal interferon response against viral infection. Moreover, we demonstrated that EFTUD2 restricts viral replication, both in a single cycle and multiple cycles of viral replication. Altogether, these results establish U5 snRNP core components as key elements of the cellular antiviral response.

Published

2022

3. Reovirus μ2 Protein Impairs Translation to Reduce U5 snRNP Protein Levels

Author

Simon Boudreault, Carole-Anne Martineau, Laurence Faucher-Giguère, Sherif Abou-Elela, Guy Lemay, and Martin Bisaillon

Subjects

reovirus, alternative splicing, U5 SNRNP, polysome profiling, translation inhibition, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Mammalian orthoreovirus (MRV) is a double-stranded RNA virus from the Reoviridae family that infects a large range of mammals, including humans. Recently, studies have shown that MRV alters cellular alternative splicing (AS) during viral infection. The structural protein μ2 appears to be the main determinant of these AS modifications by decreasing the levels of U5 core components EFTUD2, PRPF8, and SNRNP200 during infection. In the present study, we investigated the mechanism by which μ2 exerts this effect on the U5 components. Our results revealed that μ2 has no impact on steady-state mRNA levels, RNA export, and protein stability of these U5 snRNP proteins. However, polysome profiling and metabolic labeling of newly synthesized proteins revealed that μ2 exerts an inhibitory effect on global translation. Moreover, we showed that μ2 mutants unable to accumulate in the nucleus retain most of the ability to reduce PRPF8 protein levels, indicating that the effect of μ2 on U5 snRNP components mainly occurs in the cytoplasm. Finally, co-expression experiments demonstrated that μ2 suppresses the expression of U5 snRNP proteins in a dose-dependent manner, and that the expression of specific U5 snRNP core components have different sensitivities to μ2’s presence. Altogether, these results suggest a novel mechanism by which the μ2 protein reduces the levels of U5 core components through translation inhibition, allowing this viral protein to alter cellular AS during infection.

Published

2022

4. The μ2 and λ1 Proteins of Mammalian Reovirus Modulate Early Events Leading to Induction of the Interferon Signaling Network

Author

Guillaume David Després, Kenny Ngo, and Guy Lemay

Subjects

reovirus, interferon, RIG-I, viral RNA, ISGs, Stat1, Microbiology, QR1-502

Abstract

It has been previously shown that amino acid polymorphisms in reovirus proteins μ2 and λ1 are associated with differing levels of interferon induction. In the present study, viruses carrying these polymorphisms in either or both proteins, were further studied. The two viral determinants exert a synergistic effect on the control of β-interferon induction at the protein and mRNA level, with a concomitant increase in RIG-I. In contrast, levels of phospho-Stat1 and interferon-stimulated genes are increased in singly substituted viruses but with no further increase when both substitutions were present. This suggests that the viral determinants are acting during initial events of viral recognition. Accordingly, difference between viruses was reduced when infection was performed with partially uncoated virions (ISVPs) and transfection of RNA recovered from early-infected cells recapitulates the differences between viruses harboring the different polymorphisms. Altogether, the data are consistent with a redundant or complementary role of μ2 and λ1, affecting either early disassembly or the nature of the viral RNA in the incoming viral particle. Proteins involved in viral RNA synthesis are thus involved in this likely critical aspect of the ability of different reovirus variants to infect various cell types, and to discriminate between parental and transformed/cancer cells.

Published

2022

5. The Jembrana disease virus Rev protein: Identification of nuclear and novel lentiviral nucleolar localization and nuclear export signals.

Author

Claude Marchand, Guy Lemay, and Denis Archambault

Subjects

Medicine, Science

Abstract

The lentiviral Rev protein, which is a regulatory protein essential for virus replication, has been first studied in the human immunodeficiency virus type 1 (HIV-1). The main function of Rev is to mediate the nuclear exportation of viral RNAs. To fulfill its function, Rev shuttles between the cytoplasm and the nucleus. The Jembrana disease virus (JDV), a lentivirus, is the etiologic agent of the Jembrana disease which was first described in Bali cattle in Indonesia in 1964. Despite the high mortality rate associated with JDV, this virus remains poorly studied. Herein the subcellular distribution of JDV Rev, the nuclear and nucleolar localization signals (NLS and NoLS, respectively) and the nuclear export signal (NES) of the protein were examined. JDV Rev fused to the enhanced green fluorescent protein (EGFP) predominantly localized to the cytoplasm and nucleolus of transfected cells, as determined by fluorescence microscopy analyses. Through transfection of a series of deletion mutants of JDV Rev, it was possible to localize the NLS/NoLS region between amino acids (aa) 74 to 105. By substituting basic residues with alanine within this sequence, we demonstrated that the JDV Rev NLS encompasses aa 76 to 86, and is exclusively composed of arginine residues, whereas a bipartite NoLS was observed for the first time in any retroviral Rev/Rev-like proteins. Finally, a NES was identified downstream of the NLS/NoLS and encompasses aa 116 to 128 of the JDV Rev protein. The JDV Rev NES was found to be of the protein kinase A inhibitor (PKI) class instead of the HIV-1 Rev class. It also corresponds to the most optimal consensus sequence of PKI NES and, as such, is novel among lentiviral Rev NES.

Published

2019

6. How Many Mammalian Reovirus Proteins are involved in the Control of the Interferon Response?

Author

Delphine Lanoie, Simon Boudreault, Martin Bisaillon, and Guy Lemay

Subjects

virus, reovirus, interferon, viral proteins, Medicine

Abstract

As with most viruses, mammalian reovirus can be recognized and attacked by the host-cell interferon response network. Similarly, many viruses have developed resistance mechanisms to counteract the host-cell response at different points of this response. Reflecting the complexity of the interferon signaling pathways as well as the resulting antiviral response, viruses can—and often have—evolved many determinants to interfere with this innate immune response and allow viral replication. In the last few years, it has been evidenced that mammalian reovirus encodes many different determinants that are involved in regulating the induction of the interferon response or in interfering with the action of interferon-stimulated gene products. In this brief review, we present our current understanding of the different reovirus proteins known to be involved, introduce their postulated modes of action, and raise current questions that may lead to further investigations.

Published

2019

7. Global Profiling of the Cellular Alternative RNA Splicing Landscape during Virus-Host Interactions.

Author

Simon Boudreault, Camille Martenon-Brodeur, Marie Caron, Jean-Michel Garant, Marie-Pier Tremblay, Victoria E S Armero, Mathieu Durand, Elvy Lapointe, Philippe Thibault, Maude Tremblay-Létourneau, Jean-Pierre Perreault, Michelle S Scott, Guy Lemay, and Martin Bisaillon

Subjects

Medicine, Science

Abstract

Alternative splicing (AS) is a central mechanism of genetic regulation which modifies the sequence of RNA transcripts in higher eukaryotes. AS has been shown to increase both the variability and diversity of the cellular proteome by changing the composition of resulting proteins through differential choice of exons to be included in mature mRNAs. In the present study, alterations to the global RNA splicing landscape of cellular genes upon viral infection were investigated using mammalian reovirus as a model. Our study provides the first comprehensive portrait of global changes in the RNA splicing signatures that occur in eukaryotic cells following infection with a human virus. We identify 240 modified alternative splicing events upon infection which belong to transcripts frequently involved in the regulation of gene expression and RNA metabolism. Using mass spectrometry, we also confirm modifications to transcript-specific peptides resulting from AS in virus-infected cells. These findings provide additional insights into the complexity of virus-host interactions as these splice variants expand proteome diversity and function during viral infection.

Published

2016

8. Synthesis and Translation of Viral mRNA in Reovirus-Infected Cells: Progress and Remaining Questions

Author

Guy Lemay

Subjects

reovirus, transcription, RNA capping, translation, protein synthesis, PKR, interferon, Microbiology, QR1-502

Abstract

At the end of my doctoral studies, in 1988, I published a review article on the major steps of transcription and translation during the mammalian reovirus multiplication cycle, a topic that still fascinates me 30 years later. It is in the nature of scientific research to generate further questioning as new knowledge emerges. Our understanding of these fascinating viruses thus remains incomplete but it seemed appropriate at this moment to look back and reflect on our progress and most important questions that still puzzle us. It is also essential of being careful about concepts that seem so well established, but could still be better validated using new approaches. I hope that the few reflections presented here will stimulate discussions and maybe attract new investigators into the field of reovirus research. Many other aspects of the viral multiplication cycle would merit our attention. However, I will essentially limit my discussion to these central aspects of the viral cycle that are transcription of viral genes and their phenotypic expression through the host cell translational machinery. The objective here is not to review every aspect but to put more emphasis on important progress and challenges in the field.

Published

2018

9. Reovirus μ2 protein modulates host cell alternative splicing by reducing protein levels of U5 snRNP core components

Author

Simon Boudreault, Mathieu Durand, Carole-Anne Martineau, Jean-Pierre Perreault, Guy Lemay, and Martin Bisaillon

Subjects

Mammals, Alternative Splicing, RNA Splicing, Spliceosomes, Genetics, Animals, Reoviridae, Ribonucleoprotein, U5 Small Nuclear

Abstract

Mammalian orthoreovirus (MRV) is a double-stranded RNA virus from the Reoviridae family presenting a promising activity as an oncolytic virus. Recent studies have underlined MRV’s ability to alter cellular alternative splicing (AS) during infection, with a limited understanding of the mechanisms at play. In this study, we investigated how MRV modulates AS. Using a combination of cell biology and reverse genetics experiments, we demonstrated that the M1 gene segment, encoding the μ2 protein, is the primary determinant of MRV’s ability to alter AS, and that the amino acid at position 208 in μ2 is critical to induce these changes. Moreover, we showed that the expression of μ2 by itself is sufficient to trigger AS changes, and its ability to enter the nucleus is not required for all these changes. Moreover, we identified core components of the U5 snRNP (i.e. EFTUD2, PRPF8, and SNRNP200) as interactors of μ2 that are required for MRV modulation of AS. Finally, these U5 snRNP components are reduced at the protein level by both MRV infection and μ2 expression. Our findings identify the reduction of U5 snRNP components levels as a new mechanism by which viruses alter cellular AS.

Published

2022

10. [Reverse genetics in reovirus study: advances, difficulties and perspectives]

Author

Guy, Lemay

Abstract

In "classical" genetics, examination of a phenotype leads to the study of the gene(s) involved in its obtention. Reverse genetics is a powerful experimental approach in which, on the contrary, the genetic material is modified and used to reconstruct a complete organism in order to study the result of these modifications. This approach is especially well adapted to the study of viruses, considering their relative simplicity and small size of their genomes; the main obstacle remains to recover infectious viruses from cloned viral genomes. Over the years, this exploit has been achieved with representatives of almost all families of mammalian viruses. Until recently, the Reoviridae, viruses with segmented double-stranded RNA genome, were an exception. In this review, the progress accomplished toward the development of such an approach for the Orthoreovirus will thus be discussed. Reverse genetics could have a major impact for the optimization of novel virus strains for their use in therapy as oncolytic viruses and for the development of vaccines in the case of Rotavirus and Orbivirus. However, current works stress the limitations of the approach, the need for careful analysis of the results obtained, as well as the necessity to develop more efficient and polyvalent systems.

Published

2022

11. The μ2 and λ1 Proteins of Mammalian Reovirus Modulate Early Events Leading to Induction of the Interferon Signaling Network

Author

Kenny Ngo, Guy Lemay, and Guillaume David Després

Subjects

Infectious Diseases, Virology, reovirus, interferon, RIG-I, viral RNA, ISGs, Stat1

Abstract

It has been previously shown that amino acid polymorphisms in reovirus proteins μ2 and λ1 are associated with differing levels of interferon induction. In the present study, viruses carrying these polymorphisms in either or both proteins, were further studied. The two viral determinants exert a synergistic effect on the control of β-interferon induction at the protein and mRNA level, with a concomitant increase in RIG-I. In contrast, levels of phospho-Stat1 and interferon-stimulated genes are increased in singly substituted viruses but with no further increase when both substitutions were present. This suggests that the viral determinants are acting during initial events of viral recognition. Accordingly, difference between viruses was reduced when infection was performed with partially uncoated virions (ISVPs) and transfection of RNA recovered from early-infected cells recapitulates the differences between viruses harboring the different polymorphisms. Altogether, the data are consistent with a redundant or complementary role of μ2 and λ1, affecting either early disassembly or the nature of the viral RNA in the incoming viral particle. Proteins involved in viral RNA synthesis are thus involved in this likely critical aspect of the ability of different reovirus variants to infect various cell types, and to discriminate between parental and transformed/cancer cells.

Published

2022

12. Viral persistence of mammalian reovirus in cell culture: a model of virus-cell coevolution

Author

Guy Lemay

Subjects

Oncolytic Virotherapy, Genes, Viral, viruses, Cell Culture Techniques, Context (language use), Biology, Reoviridae, Virus Replication, Virology, Reverse genetics, Virus, Oncolytic virus, Mice, Infectious Diseases, Viral replication, Interferon, Viral evolution, Neoplasms, medicine, Animals, Humans, Virotherapy, medicine.drug

Abstract

Although mammalian reovirus exhibits only limited pathogenicity in humans, it has been, and still remains, instrumental in studies of viral replication and pathogenesis. Generally considered as cytolytic, this virus can sometimes establish long-term persistent infections in tissue culture. In fact, in this context, it constitutes one widely used model to demonstrate coevolution between virus and host cells. Initially limited to the murine L929 fibroblasts model, further studies in different cell types appeared in the last few years. Establishment of viral persistence could also become a preferred approach to isolate new viruses that are better adapted to their applications in virotherapy, for example as oncolytic agents against human or animal cancers. A better understanding of the persistence phenomenon, especially of viral genes involved, is thus essential. The development of new tools, such as reverse genetics, appears very promising to achieve these objectives. Actually, this last approach allows us to establish the biological significance of mutations found on viruses selected during viral persistence.

Published

2019

13. How Many Mammalian Reovirus Proteins are involved in the Control of the Interferon Response?

Author

Guy Lemay, Martin Bisaillon, Simon Boudreault, and Delphine Lanoie

Subjects

Microbiology (medical), viruses, lcsh:Medicine, Review, virus, Biology, reovirus, Virus, 03 medical and health sciences, Interferon, medicine, Immunology and Allergy, Mammalian reovirus, Molecular Biology, Gene, 030304 developmental biology, 0303 health sciences, Innate immune system, General Immunology and Microbiology, 030306 microbiology, lcsh:R, interferon, 3. Good health, Cell biology, Infectious Diseases, viral proteins, Viral replication, Signal transduction, medicine.drug

Abstract

As with most viruses, mammalian reovirus can be recognized and attacked by the host-cell interferon response network. Similarly, many viruses have developed resistance mechanisms to counteract the host-cell response at different points of this response. Reflecting the complexity of the interferon signaling pathways as well as the resulting antiviral response, viruses can—and often have—evolved many determinants to interfere with this innate immune response and allow viral replication. In the last few years, it has been evidenced that mammalian reovirus encodes many different determinants that are involved in regulating the induction of the interferon response or in interfering with the action of interferon-stimulated gene products. In this brief review, we present our current understanding of the different reovirus proteins known to be involved, introduce their postulated modes of action, and raise current questions that may lead to further investigations.

Published

2019

14. Viral modulation of cellular RNA alternative splicing: A new key player in virus–host interactions?

Author

Simon Boudreault, Martin Bisaillon, Guy Lemay, and Patricia Roy

Subjects

virus–host interactions, Computational biology, virus, Biology, RNA alternative splicing, Biochemistry, Virus, 03 medical and health sciences, Exon, Splicing Regulation/Alternative Splicing, Humans, RNA in Disease, Molecular Biology, Gene, 030304 developmental biology, 0303 health sciences, Host Microbial Interactions, 030302 biochemistry & molecular biology, Alternative splicing, Intron, RNA, Alternative Splicing, Advanced Review, RNA splicing, Proteome, Viruses, Advanced Reviews, RNA, Viral

Abstract

Upon viral infection, a tug of war is triggered between host cells and viruses to maintain/gain control of vital cellular functions, the result of which will ultimately dictate the fate of the host cell. Among these essential cellular functions, alternative splicing (AS) is an important RNA maturation step that allows exons, or parts of exons, and introns to be retained in mature transcripts, thereby expanding proteome diversity and function. AS is widespread in higher eukaryotes, as it is estimated that nearly all genes in humans are alternatively spliced. Recent evidence has shown that upon infection by numerous viruses, the AS landscape of host‐cells is affected. In this review, we summarize recent advances in our understanding of how virus infection impacts the AS of cellular transcripts. We also present various molecular mechanisms allowing viruses to modulate cellular AS. Finally, the functional consequences of these changes in the RNA splicing signatures during virus–host interactions are discussed. This article is categorized under:RNA in Disease and Development > RNA in DiseaseRNA Processing > Splicing Regulation/Alternative Splicing

Published

2019

15. Identification of the nuclear and nucleolar localization signals of the Feline immunodeficiency virus Rev protein

Author

Denis Archambault, Guy Lemay, and Claude Marchand

Subjects

Signal peptide, Cancer Research, Feline immunodeficiency virus, animal diseases, viruses, Green Fluorescent Proteins, Nuclear Localization Signals, Immunodeficiency Virus, Feline, Kidney, Virus Replication, Cell Line, Green fluorescent protein, 03 medical and health sciences, Virology, Animals, NLS, Amino Acid Sequence, Nuclear export signal, 030304 developmental biology, Cell Nucleus, 0303 health sciences, biology, 030306 microbiology, virus diseases, biology.organism_classification, 3. Good health, Cell biology, Gene Products, rev, Infectious Diseases, Viral replication, Lentivirus, Cats, RNA, Viral, Cell Nucleolus, Nuclear localization sequence

Abstract

Lentivirus genomes code for a regulatory protein essential for virus replication termed Rev. The Rev protein binds to partially spliced and unspliced viral RNAs and mediates their nuclear export. Therefore, Rev possesses functional domains that enable its shuttling between the cytoplasm and the nucleus. The Feline immunodeficiency virus (FIV), a lentivirus, can lead to an immunodeficiency syndrome after a long incubation period, similar to that associated with the human immunodeficiency virus type 1 (HIV-1). The FIV Rev functional domains have been predicted only by homology with those of HIV-1 Rev. In the present study, the nuclear and nucleolar localization signals (NLS and NoLS, respectively) of the FIV Rev were examined. A series of FIV Rev deletion mutants fused to the enhanced green fluorescent protein (EGFP) were used to localize the NLS in a region spanning amino acids (aa) 81–100. By using alanine substitution mutants, basic residues present between the amino acids (aa) 84–99 of the FIV Rev protein sequence were identified to form the NLS, whereas those between aa 82–95 were associated with the NoLS function. These results further enhance our understanding of how Rev exerts its role in the replication cycle of lentiviruses.

Published

2020

16. A single mutation in the mammalian orthoreovirus S1 gene is responsible for increased interferon sensitivity in a virus mutant selected in Vero cells

Author

Stéphanie Côté, Guy Lemay, Delphine Lanoie, Emmanuelle Degeorges, and Université de Montréal. Faculté de médecine. Département de microbiologie, infectiologie et immunologie

Subjects

viruses, Mutant, Orthoreovirus, Mammalian, Codon, Initiator, Genome, Viral, Biology, Reovirus, medicine.disease_cause, Virus Replication, Virus, Cell Line, 03 medical and health sciences, Mice, Interferon, Virology, Cricetinae, Chlorocebus aethiops, medicine, Animals, Gene, Vero Cells, 030304 developmental biology, 0303 health sciences, Mutation, 030302 biochemistry & molecular biology, Reverse genetics, Reverse Genetics, Viral replication, Vero cell, Capsid Proteins, Interferons, medicine.drug

Abstract

In a previous study, a mammalian orthoreovirus mutant was isolated based on its increased ability to infect interferon-defective Vero cells and was referred to as Vero-cells-adapted virus (VeroAV). This virus exhibits reduced ability to resist the antiviral effect of interferon. In the present study, the complete genome sequence of VeroAV was first determined. Reverse genetics was then used to identify a unique mutation on the S1 gene, overlapping the σ1 and σ1 s reading frame, resulting in increased sensitivity to interferon. A virus lacking σ1 s expression consecutive to mutation of its initiation codon was then shown to exhibit a further increase in sensitivity to interferon, supporting the idea that σ1 s is the viral protein responsible. This identification of a new determinant of reovirus sensitivity to interferon gives credentials to the idea that multiple reovirus genes are responsible for the level of interferon induction and susceptibility to the interferon-induced antiviral activities.

Published

2018

17. A single amino acid substitution in the mRNA capping enzyme λ2 of a mammalian orthoreovirus mutant increases interferon sensitivity

Author

Guy Lemay, Véronique Sandekian, and Université de Montréal. Faculté de médecine. Département de microbiologie, infectiologie et immunologie

Subjects

viruses, DNA Mutational Analysis, Molecular Sequence Data, Orthoreovirus, Mammalian, Mutant, virus, RNA capping, Biology, reovirus, Antiviral Agents, Genome, Article, Virus, Cell Line, Mice, reverse genetics, Plasmid, Interferon, Virology, medicine, Animals, RNA methyltransferase, Gene, ARN méthyltransférase, 2. Zero hunger, Sequence Analysis, DNA, interferon, interféron, Nucleotidyltransferases, Molecular biology, Reverse genetics, 3. Good health, Oncolytic virus, Amino Acid Substitution, réovirus, génétique inverse, structure coiffe, RNA, Viral, Interferons, medicine.drug

Abstract

In the last few years, the development of a plasmid-based reverse genetics system for mammalian reovirus has allowed the production and characterization of mutant viruses. This could be especially significant in the optimization of reovirus strains for virotherapeutic applications, either as gene vectors or oncolytic viruses. The genome of a mutant virus exhibiting increased sensitivity to interferon was completely sequenced and compared with its parental virus. Viruses corresponding to either the parental or mutant viruses were then rescued by reverse genetics and shown to exhibit the expected phenotypes. Systematic rescue of different viruses harboring either of the four parental genes in a mutant virus backbone, or reciprocally, indicated that a single amino acid substitution in one of λ2 methyltransferase domains is the major determinant of the difference in interferon sensitivity between these two viruses., Au cours des dernières années, la mise au point de la génétique inverse pour les réovirus de mammifères a permis la production et la caractérisation de virus mutants. Ceci pourrait être spécialement important pour l'optimisation de souches virales en vue d'applications thérapeutiques, comme vecteurs de gènes ou virus oncolytiques. Le génome d'un virus mutant démontrant une sensibilité accrue à l'interféron a été complètement séquencé et comparé au virus parental. Des virus correspondant au virus parental ou mutant ont ensuite été récupérés par génétique inverse et présentaient les phénotypes attendus. La récupération systématique de différents virus possédant un des quatre gènes parentaux dans un fond génétique du virus mutant, et réciproquement, a indiqué qu'une seule substitution d'acide aminé dans un des deux domaines méthyltransférase de λ2 est le déterminant majeur de la différence de sensibilité à l'interféron entre ces deux virus.

Published

2015

18. Multiple proteins differing between laboratory stocks of mammalian orthoreoviruses affect both virus sensitivity to interferon and induction of interferon production during infection

Author

Delphine Lanoie, Guy Lemay, and Université de Montréal. Faculté de médecine. Département de microbiologie, infectiologie et immunologie

Subjects

0301 basic medicine, Gene Expression Regulation, Viral, Models, Molecular, Protein Conformation, alpha-Helical, Cancer Research, Orthoreovirus, Mammalian, Interferon secretion, Biology, Reovirus, Antiviral Agents, Virus, Cell Line, 03 medical and health sciences, Mice, Viral Proteins, Plasmid, Cricetulus, Interferon, Virology, medicine, Animals, Gene, Viral Core Proteins, Interferon-alpha, RNA-Binding Proteins, Epithelial Cells, Interferon-beta, Fibroblasts, Nucleotidyltransferases, Reverse genetics, Reverse Genetics, DNA-Binding Proteins, Interferon production, 030104 developmental biology, Infectious Diseases, Host-Pathogen Interactions, Capsid Proteins, Protein Conformation, beta-Strand, Reassortant Viruses, medicine.drug

Abstract

In the course of previous works, it was observed that the virus laboratory stock (T3DS) differs in sequence from the virus encoded by the ten plasmids currently in use in many laboratories (T3DK), and derived from a different original virus stock. Seven proteins are affected by these sequence differences. In the present study, replication of T3DK was shown to be more sensitive to the antiviral effect of interferon. Infection by the T3DK virus was also shown to induce the production of higher amount of β and α-interferons compared to T3DS. Two proteins, the μ2 and λ2 proteins, were found to be responsible for increased sensitivity to interferon while both μ2 and λ1 are responsible for increased interferon secretion. Altogether this supports the idea that multiple reovirus proteins are involved in the control of induction of interferon and virus sensitivity to the interferon-induced response. While interrelated, interferon induction and sensitivity can be separated by defined gene combinations. While both μ2 and λ2 were previously suspected of a role in the control of the interferon response, other proteins are also likely involved, as first shown here for λ1. This also further stresses that due caution should be exerted when comparing different virus isolates with different genetic background.

Published

2017

19. Human T-Cell Leukemia Virus Type 3 (HTLV-3) and HTLV-4 Antisense-Transcript-Encoded Proteins Interact and Transactivate Jun Family-Dependent Transcription via Their Atypical bZIP Motif

Author

Charlotte André-Arpin, Malgorzata Borowiak, Benoit Barbeau, Émilie Larocque, Jean-Michel Mesnard, William M. Switzer, Guy Lemay, and Madeleine Duc Dodon

Subjects

Transcriptional Activation, Transcription, Genetic, Proto-Oncogene Proteins c-jun, Immunology, Biology, Deltaretrovirus, Microbiology, DNA, Antisense, Cell Line, Viral Proteins, Transactivation, Transcription (biology), Cell Line, Tumor, Virology, Chlorocebus aethiops, Gene expression, Animals, Humans, Promoter Regions, Genetic, Telomerase, Transcription factor, HEK 293 cells, Human T-lymphotropic virus 3, bZIP domain, Molecular biology, Protein Structure, Tertiary, Up-Regulation, Virus-Cell Interactions, Antisense RNA, Basic-Leucine Zipper Transcription Factors, HEK293 Cells, Viral replication, Insect Science, COS Cells, HeLa Cells

Abstract

Human T-cell leukemia virus types 3 and 4 (HTLV-3 and HTLV-4) are recently isolated retroviruses. We have previously characterized HTLV-3- and HTLV-4-encoded antisense genes, termed APH-3 and APH-4, respectively, which, in contrast to HBZ, the HTLV-1 homologue, do not contain a typical bZIP domain (M. Larocque É Halin, S. Landry, S. J. Marriott, W. M. Switzer, and B. Barbeau, J. Virol. 85: 12673–12685, 2011, doi:10.1128/JVI.05296-11). As HBZ differentially modulates the transactivation potential of various Jun family members, the effect of APH-3 and APH-4 on JunD-, c-Jun-, and JunB-mediated transcriptional activation was investigated. We first showed that APH-3 and APH-4 upregulated the transactivation potential of all tested Jun family members. Using an human telomerase catalytic subunit (hTERT) promoter construct, our results also highlighted that, unlike HBZ, which solely modulates hTERT expression via JunD, both APH-3 and APH-4 acted positively on the transactivation of the hTERT promoter mediated by tested Jun factors. Coimmunoprecipitation experiments demonstrated that these Jun proteins interacted with APH-3 and APH-4. Although no activation domain was identified for APH proteins, the activation domain of c-Jun was very important in the observed upregulation of its activation potential. We further showed that APH-3 and APH-4 required their putative bZIP-like domains and corresponding leucine residues for interaction and modulation of the transactivation potential of Jun factors. Our results demonstrate that HTLV-encoded antisense proteins behave differently, and that the bZIP-like domains of both APH-3 and APH-4 have retained their interaction potential for Jun members. These studies are important in assessing the differences between HBZ and other antisense proteins, which might further contribute to determining the role of HBZ in HTLV-1-associated diseases. IMPORTANCE HBZ, the antisense transcript-encoded protein from HTLV-1, is now well recognized as a potential factor for adult T-cell leukemia/lymphoma development. In order to better appreciate the mechanism of action of HBZ, comparison to antisense proteins from other HTLV viruses is important. Little is known in relation to the seemingly nonpathogenic HTLV-3 and HTLV-4 viruses, and studies of their antisense proteins are limited to our previously reported study (M. Larocque É Halin, S. Landry, S. J. Marriott, W. M. Switzer, and B. Barbeau, J. Virol. 85: 12673–12685, 2011, doi:10.1128/JVI.05296-11). Here, we demonstrate that Jun transcription factors are differently affected by APH-3 and APH-4 compared to HBZ. These intriguing findings suggest that these proteins act differently on viral replication but also on cellular gene expression, and that highlighting their differences of action might lead to important information allowing us to understand the link between HTLV-1 HBZ and ATL in infected individuals.

Published

2014

20. The Jembrana disease virus Rev protein: Identification of nuclear and novel lentiviral nucleolar localization and nuclear export signals

Author

Guy Lemay, Claude Marchand, and Denis Archambault

Subjects

RNA viruses, 0301 basic medicine, Cytoplasm, Confocal Microscopy, Molecular biology, viruses, Amino Acid Motifs, Nuclear Localization Signals, 030230 surgery, Pathology and Laboratory Medicine, Molecular biology assays and analysis techniques, Biochemistry, Green fluorescent protein, Database and Informatics Methods, 0302 clinical medicine, Immunodeficiency Viruses, Medicine and Health Sciences, Amino Acids, Peptide sequence, Microscopy, Alanine, Multidisciplinary, Organic Compounds, Light Microscopy, 3. Good health, Transport protein, Protein Transport, Chemistry, Gene Products, rev, Medical Microbiology, Viral Pathogens, Viruses, Physical Sciences, Medicine, Pathogens, Cellular Structures and Organelles, Basic Amino Acids, Sequence Analysis, Cell Nucleolus, Research Article, Signal peptide, Bioinformatics, Science, Recombinant Fusion Proteins, Green Fluorescent Proteins, Biology, Arginine, Microbiology, Cell Line, 03 medical and health sciences, Dogs, Sequence Motif Analysis, Retroviruses, Animals, Humans, NLS, Amino Acid Sequence, CAT assay, Nuclear export signal, Microbial Pathogens, Jembrana disease, Nuclear Export Signals, Cell Nucleus, Lentivirus, Organic Chemistry, Organisms, Chemical Compounds, Biology and Life Sciences, HIV, Proteins, Nucleolus, Cell Biology, Virology, Research and analysis methods, HEK293 Cells, Molecular biology techniques, 030104 developmental biology, Aliphatic Amino Acids, Viral replication, HIV-1, Cattle, Mutant Proteins, Confocal Laser Microscopy

Abstract

The lentiviral Rev protein, which is a regulatory protein essential for virus replication, has been first studied in the human immunodeficiency virus type 1 (HIV-1). The main function of Rev is to mediate the nuclear exportation of viral RNAs. To fulfill its function, Rev shuttles between the cytoplasm and the nucleus. The Jembrana disease virus (JDV), a lentivirus, is the etiologic agent of the Jembrana disease which was first described in Bali cattle in Indonesia in 1964. Despite the high mortality rate associated with JDV, this virus remains poorly studied. Herein the subcellular distribution of JDV Rev, the nuclear and nucleolar localization signals (NLS and NoLS, respectively) and the nuclear export signal (NES) of the protein were examined. JDV Rev fused to the enhanced green fluorescent protein (EGFP) predominantly localized to the cytoplasm and nucleolus of transfected cells, as determined by fluorescence microscopy analyses. Through transfection of a series of deletion mutants of JDV Rev, it was possible to localize the NLS/NoLS region between amino acids (aa) 74 to 105. By substituting basic residues with alanine within this sequence, we demonstrated that the JDV Rev NLS encompasses aa 76 to 86, and is exclusively composed of arginine residues, whereas a bipartite NoLS was observed for the first time in any retroviral Rev/Rev-like proteins. Finally, a NES was identified downstream of the NLS/NoLS and encompasses aa 116 to 128 of the JDV Rev protein. The JDV Rev NES was found to be of the protein kinase A inhibitor (PKI) class instead of the HIV-1 Rev class. It also corresponds to the most optimal consensus sequence of PKI NES and, as such, is novel among lentiviral Rev NES.

Published

2019

21. Characterization of HIV Type 1 Envelope Sequence Among Viral Isolates Circulating in the Northern Region of Colombia, South America

Author

Guillermo Cervantes-Acosta, Robin Hernández, Jaime Gutiérrez, Martha Peñuela, Lucy Palacio, Guy Lemay, and José-Luis Villarreal

Subjects

Genotype, Sequence analysis, Molecular Sequence Data, Immunology, HIV Infections, Sequence alignment, Colombia, HIV Envelope Protein gp120, Biology, Type (biology), Viral envelope, Phylogenetics, Virology, Cluster Analysis, Humans, Amino Acid Sequence, Peptide sequence, Phylogeny, Sequence (medicine), Genetics, Sequence Notes, Sequence Analysis, DNA, South America, Infectious Diseases, HIV-1, Sequence Alignment

Abstract

To characterize human immunodeficiency virus (HIV-1) strains circulating in the Northern region of Colombia in South America, sequences of the viral envelope C2V3C3 region were obtained from patients with different high-risk practices. Close to 60% of the sequences were predicted to belong to macrophage-tropic viruses, according to the positions of acidic amino acids and putative N-linked glycosylation sites. This is in agreement with the fact that most of the patients were recently diagnosed individuals. Phylogenic analysis then allowed assignment of all 35 samples to subtype B viruses. This same subtype was found in previous studies carried out in other Colombian regions. This study thus expands previous analyses with previously missing data from the Northern region of the country. The number and the length of the sequences examined also help to provide a clearer picture of the prevailing situation of the present HIV epidemics in this country.

Published

2012

22. Global Profiling of the Cellular Alternative RNA Splicing Landscape during Virus-Host Interactions

Author

Victoria E. S. Armero, Martin Bisaillon, Maude Tremblay-Létourneau, Mathieu Durand, Simon Boudreault, Elvy Lapointe, Camille Martenon-Brodeur, Guy Lemay, Jean-Michel Garant, Marie-Pier Tremblay, Marie Caron, Jean-Pierre Perreault, Michelle S. Scott, and Philippe Thibault

Subjects

0301 basic medicine, Proteomics, RNA splicing, Exonic splicing enhancer, lcsh:Medicine, RNA-binding protein, Biochemistry, Exon, Mice, 0302 clinical medicine, lcsh:Science, Mammalian orthoreovirus 3, Genetics, Multidisciplinary, Genome, Messenger RNA, RNA sequencing, Exons, Post-transcriptional modification, Nucleic acids, RNA editing, 030220 oncology & carcinogenesis, Host-Pathogen Interactions, Sequence Analysis, Research Article, Biology, Research and Analysis Methods, Microbiology, 03 medical and health sciences, Sequence Motif Analysis, Virology, DNA-binding proteins, Animals, Humans, Gene Regulation, Amino Acid Sequence, RNA, Messenger, Molecular Biology Techniques, Sequencing Techniques, Molecular Biology, Sequence Analysis, RNA, Alternative splicing, lcsh:R, Intron, Biology and Life Sciences, Proteins, Molecular Sequence Annotation, Fibroblasts, Regulatory Proteins, Alternative Splicing, 030104 developmental biology, Gene Ontology, RNA processing, RNA, lcsh:Q, Gene expression, Viral Transmission and Infection, Transcription Factors

Abstract

Alternative splicing (AS) is a central mechanism of genetic regulation which modifies the sequence of RNA transcripts in higher eukaryotes. AS has been shown to increase both the variability and diversity of the cellular proteome by changing the composition of resulting proteins through differential choice of exons to be included in mature mRNAs. In the present study, alterations to the global RNA splicing landscape of cellular genes upon viral infection were investigated using mammalian reovirus as a model. Our study provides the first comprehensive portrait of global changes in the RNA splicing signatures that occur in eukaryotic cells following infection with a human virus. We identify 240 modified alternative splicing events upon infection which belong to transcripts frequently involved in the regulation of gene expression and RNA metabolism. Using mass spectrometry, we also confirm modifications to transcript-specific peptides resulting from AS in virus-infected cells. These findings provide additional insights into the complexity of virus-host interactions as these splice variants expand proteome diversity and function during viral infection.

Published

2016

23. Addition of exogenous polypeptides on the mammalian reovirus outer capsid using reverse genetics

Author

Virginie Brochu-Lafontaine, Guy Lemay, and Université de Montréal. Faculté de médecine. Département de microbiologie, infectiologie et immunologie

Subjects

Recombinant Fusion Proteins, viruses, Genetic Vectors, Orthoreovirus, Mammalian, Gene Expression, Oncolytic viruses, Biology, Genome, Virus oncolytiques, Virus, Cell Line, Mice, Plasmid, Virology, Chlorocebus aethiops, Animals, Génétique inverse, chemistry.chemical_classification, Reverse genetics, Stop codon, Amino acid, chemistry, Capsid, Tag, Nucleic acid, Capsid Proteins, Epitope, Épitope, Genetic Engineering, Plasmids

Abstract

Addition of exogenous peptide sequences on viral capsids is a powerful approach to study the process of viral infection or to retarget viruses toward defined cell types. Until recently, it was not possible to manipulate the genome of mammalian reovirus and this was an obstacle to the addition of exogenous sequence tags onto the capsid of a replicating virus. This obstacle has now been overcome by the advent of the plasmid-based reverse genetics system. In the present study, reverse genetics was used to introduce different exogenous peptides, up to 40 amino acids long, at the carboxyl-terminal end of the σ1 outer capsid protein. The tagged viruses obtained were infectious, produce plaques of similar size, and could be easily propagated at hight titers. However, attempts to introduce a 750 nucleotides-long sequence failed, even when it was added after the stop codon, suggesting a possible size limitation at the nucleic acid level., L'addition aux capsides virales de séquences peptidiques exogènes est une approche puissante pour l'étude des processus d'infection virale ou pour cibler des virus vers des types cellulaires bien définis. Jusqu'à récemment, il n'était pas possible de manipuler le génome du réovirus de mammifères et ceci était un obstacle à l'addition de telles étiquettes exogènes sur la capside d'un virus pouvant se répliquer. Cet obstacle a maintenant été surmonté par la mise au point d'un système de génétique inverse à base de plasmides. Dans la présente étude, la génétique inverse a été utilisée pour introduire différents peptides exogènes, jusqu'à 40 acides aminés de longueur, à l'extrémité carboxyle de la protéine de capside externe σ1. Les virus obtenus étaient infectieux, produisent des plages de taille similaire, et peuvent être propagés facilement. Cependant, les efforts pour introduire une séquence de 750 nucléotides de longueur ont été infructueux, même lorsqu'un codon de terminaison était introduit avant celle-ci, suggérant une limite de taille au niveau des acides nucléiques.

Published

2012

24. Role of envelope processing and gp41 membrane spanning domain in the formation of human immunodeficiency virus type 1 (HIV-1) fusion–competent envelope glycoprotein complex

Author

Guy Lemay, Éric A. Cohen, and Mélanie Welman

Subjects

Cancer Research, viruses, Mutant, Hemagglutinin Glycoproteins, Influenza Virus, Biology, Gp41, Cell Line, HIV Envelope Protein gp160, Glycoprotein complex, Virology, Humans, Sequence Deletion, Recombination, Genetic, chemistry.chemical_classification, Wild type, virus diseases, Virus Internalization, Herpesvirus glycoprotein B, HIV Envelope Protein gp41, Transmembrane protein, Protein Structure, Tertiary, Infectious Diseases, Ectodomain, chemistry, HIV-1, Glycoprotein, Protein Processing, Post-Translational

Abstract

Human immunodeficiency virus type 1 (HIV-1) entry into target cells is directed by the envelope (Env) glycoproteins, which are present on the surface of HIV-1 virion or infected cells in the form of trimers consisting of gp120/gp41 complexes. The surface subunit, gp120, initiates the entry process by interacting sequentially with the CD4 receptor and a co-receptor, thereby inducing a conformational change that allows the transmembrane (TM) gp41 subunit to mediate fusion between viral and target cell membranes. Cleavage of Env into its gp120 and gp41 components is necessary for activation of its fusogenic activity. Here, the gp41 TM glycoprotein was altered by either deleting an isoleucine residue (DeltaI642) in a critical region of its ectodomain or by substituting its membrane spanning domain (MSD) by that of the influenza hemagglutinin (HA) glycoprotein (TM-HA) to examine the contribution of these regions to Env functions. Characterization of these mutant forms of gp41 revealed that they both affected the infectivity of pseudotyped virions, however, through distinct defects in Env functions. While deletion of Ile 642 drastically altered processing of Env, replacement of gp41 MSD by that of HA led to a marked fusion defect even though the TM-HA Env was efficiently processed and incorporated into viral particles. Interestingly, both DeltaI642 and TM-HA Env were found to act as trans dominant-negative mutant of viral infectivity, presumably via their ability to form hetero-oligomers with wild type Env. Together, these results support a previously proposed model whereby all three gp120-gp41 monomers must be cleaved for the Env homo-trimer to function and suggest that the gp41 MSD plays a critical role in the formation of fusion-competent Env trimers.

Published

2007

25. CD4/CXCR4 co-expression allows productive HIV-1 infection in canine kidney MDCK cells

Author

Mélanie Welman, Guy Lemay, Éric A. Cohen, Frédéric Freund, and Guillermo Cervantes-Acosta

Subjects

Receptors, CXCR4, Cancer Research, Virulence, viruses, Viral budding, HIV Infections, Biology, Kidney, Virus Replication, Virology, Herpesvirus glycoprotein B, Cell Line, Cell biology, Dogs, Infectious Diseases, Viral envelope, Viral replication, Viral entry, Cell culture, CD4 Antigens, HIV-1, Animals, Viral Accessory Proteins, Viral shedding

Abstract

The Madin-Darby canine kidney (MDCK) cell line has become the prototypic cell type for studying the mechanisms involved in viral glycoproteins transport and viral assembly in polarized cells. This cell line has been used in our laboratories for studying human immunodeficiency virus (HIV-1), despite the fact that MDCK cells cannot be infected by HIV. In transfected MDCK cells, HIV-1 glycoproteins are specifically transported to the basolateral cell surface where viral budding also mostly occurs. However, this model is of limited use when viral propagation, infection of most cells, or larger production of virions, is needed. The initial objective of this work was thus to establish an MDCK-derived cell line that could be productively infected by HIV-1, in order to pursue our studies on the polarization of viral budding. Expression of both receptor and co-receptor for T-tropic strains of the virus showed that canine cells are rendered permissive once virus binding and entry is allowed. In addition, a reduced infectivity of the viral particles released from the basolateral surface was observed. This observation most likely reflects the interference mediated by CD4 molecules that accumulate at the basolateral domain. Accordingly, this effect was largely prevented when using viruses that down-regulate cell surface CD4 by expression of both viral accessory proteins Vpu and Nef. This is a further evidence that the function of different viral proteins depends of the site of viral budding, which is itself determined by the presence of targeting signal(s) harbored by viral envelope glycoproteins.

Published

2006

26. Correlation between interferon sensitivity of reovirus isolates and ability to discriminate between normal and Ras-transformed cells

Author

Penny A. Rudd and Guy Lemay

Subjects

Viral isolate, Orthoreovirus, Mammalian, Mutant, Mutagenesis (molecular biology technique), Microbial Sensitivity Tests, Biology, Antiviral Agents, Virology, Protein kinase R, Virus, Mice, Cell Transformation, Neoplastic, Mutagenesis, Interferon, medicine, Animals, Interferons, Protein kinase A, Cells, Cultured, Intracellular, medicine.drug

Abstract

Mammalian reoviruses exhibit a propensity to replicate in transformed cells. It is currently believed that the interferon-inducible RNA-dependent protein kinase (PKR), an intracellular host-cell resistance factor that is inhibited by an activatedRas-dependent pathway in transformed cells, is responsible for this discrimination. In the present study, reovirus isolates differing in their sensitivity to interferon were obtained by chemical mutagenesis, and examined for their replicative properties in parental andRas-transformed mouse NIH-3T3 cells. It was observed that most isolates can bypass resistance mechanisms of parental cells at high m.o.i., and that there is a correlation between the ability to discriminate between transformed and parental cells, and interferon sensitivity. Most interestingly, an interferon-hypersensitive mutant virus was more dependent onRasactivation than any other viral isolate. Altogether, this suggests that optimal reovirus isolates could be selected to attack tumour cells depending on the nature of the alterations in interferon-inducible pathways found in these cells.

Published

2005

27. The tyrosine-based YXXØ targeting motif of murine leukemia virus envelope glycoprotein affects pathogenesis

Author

Julie Deschambeault, Guy Lemay, Éric A. Cohen, Carole Danis, Sonia Do Carmo, and Eric Rassart

Subjects

viruses, Viral budding, Amino Acid Motifs, Molecular Sequence Data, Cell, Mutant, Pathogenesis, Virus Replication, Endocytosis, Mice, Retrovirus, Viral Envelope Proteins, Envelope, Polarization, Virology, Murine leukemia virus, medicine, Animals, Amino Acid Sequence, Tyrosine, chemistry.chemical_classification, Targeting, biology, Virion, HIV, Cell Polarity, Basolateral, biology.organism_classification, MuLV, Leukemia Virus, Murine, medicine.anatomical_structure, chemistry, NIH 3T3 Cells, Glycoprotein

Abstract

Retroviruses, such as human and simian immunodeficiency viruses (HIV and SIV), and murine leukemia viruses (MuLV), harbor a tyrosine-based motif in the intracytoplasmic domain of their envelope glycoprotein. This motif can act as an endocytosis signal or as a targeting signal, restricting viral budding at specific cell surface membrane domains. In the present study, proviral DNA of the ecotropic Cas-Br-E strain of MuLV was modified by substitution or deletion of the critical tyrosine residue. Mutant viruses lost basolateral targeting in polarized MDCK epithelial cells while expression level of the glycoprotein at the cell surface was not affected. This suggests that the tyrosine-based motif in MuLV does not act as an endocytosis signal. Only a small delay in the appearance of disease was observed in inoculated mice. In contrast, a striking change in the pathology was observed with enlarged thymus and lymph nodes in animals inoculated with mutant viruses.

Published

2004

28. Efficiency of a programmed −1 ribosomal frameshift in the different subtypes of the human immunodeficiency virus type 1 group M

Author

Dominic Dulude, Léa Brakier-Gingras, Guy Lemay, Martin Baril, and Karine Gendron

Subjects

Gene Expression Regulation, Viral, Transcription, Genetic, Molecular Sequence Data, Mutant, Human immunodeficiency virus (HIV), Biology, Virus Replication, medicine.disease_cause, Article, Ribosomal frameshift, Frameshift mutation, Genes, Reporter, Sequence Homology, Nucleic Acid, Mole, medicine, Humans, Narrow range, Luciferases, Molecular Biology, Conserved Sequence, chemistry.chemical_classification, Genetics, Luciferase reporter, Base Sequence, Frameshifting, Ribosomal, Molecular biology, Fusion Proteins, gag-pol, Enzyme, chemistry, Protein Biosynthesis, Mutation, HIV-1, Mutagenesis, Site-Directed, Nucleic Acid Conformation, RNA, Viral

Abstract

The synthesis of the Gag-Pol polyprotein, the precursor of the enzymes of the human immunodeficiency virus type 1 (HIV-1), requires a programmed −1 ribosomal frameshift. This frameshift has been investigated so far only for subtype B of HIV-1 group M. In this subtype, the frameshift stimulatory signal was found to be a two-stem helix, in which a three-purine bulge interrupts the two stems. In this study, using a luciferase reporter system, we compare, for the first time, the frameshift efficiency of all the subtypes of group M. Mutants of subtype B, including a natural variant were also investigated. Our results with mutants of subtype B confirm that the bulge and the lower stem of the frameshift stimulatory signal contribute to the frameshift in addition to the upper stem–loop considered previously as the sole participant. Our results also show that the frameshift stimulatory signal of all of the other subtypes of group M can be folded into the same structure as in subtype B, despite sequence variations. Moreover, the frameshift efficiency of these subtypes, when assessed in cultured cells, falls within a narrow window (the maximal deviation from the mean value calculated from the experimental values of all the subtypes being ~35%), although the predicted thermodynamic stability of the frameshift stimulatory signal differs between the subtypes (from −17.2 kcal/mole to −26.2 kcal/mole). The fact that the frameshift efficiencies fall within a narrow range for all of the subtypes of HIV-1 group M stresses the potential of the frameshift event as an antiviral target.

Published

2003

29. Replacement of Murine Leukemia Virus Readthrough Mechanism by Human Immunodeficiency Virus Frameshift Allows Synthesis of Viral Proteins and Virus Replication

Author

Marie-Noëlle Brunelle, Léa Brakier-Gingras, and Guy Lemay

Subjects

Gene Expression Regulation, Viral, Recombinant Fusion Proteins, viruses, Molecular Sequence Data, Immunology, Replication, Mutagenesis (molecular biology technique), Virus Replication, Slippery sequence, Microbiology, Ribosomal frameshift, Virus, Frameshift mutation, Mice, Viral Proteins, Virology, Murine leukemia virus, Animals, Humans, Genetics, Base Sequence, biology, Frameshifting, Ribosomal, 3T3 Cells, Provirus, biology.organism_classification, Genes, gag, Genes, pol, Fusion Proteins, gag-pol, Viral replication, Protein Biosynthesis, Insect Science, HIV-1, Mutagenesis, Site-Directed, RNA, Viral, Moloney murine leukemia virus

Abstract

Retroviruses use unusual recoding strategies to synthesize the Gag-Pol polyprotein precursor of viral enzymes. In human immunodeficiency virus, ribosomes translating full-length viral RNA can shift back by 1 nucleotide at a specific site defined by the presence of both a slippery sequence and a downstream stimulatory element made of an extensive secondary structure. This so-called frameshift mechanism could become a target for the development of novel antiviral strategies. A different recoding strategy is used by other retroviruses, such as murine leukemia viruses, to synthesize the Gag-Pol precursor; in this case, a stop codon is suppressed in a readthrough process, again due to the presence of a specific structure adopted by the mRNA. Development of antiframeshift agents will greatly benefit from the availability of a simple animal and virus model. For this purpose, the murine leukemia virus readthrough region was rendered inactive by mutagenesis and the frameshift region of human immunodeficiency virus was inserted to generate a chimeric provirus. This substitution of readthrough by frameshift allows the synthesis of viral proteins, and the chimeric provirus sequence was found to generate infectious viruses. This system could be a most interesting alternative to study ribosomal frameshift in the context of a virus amenable to the use of a simple animal model.

Published

2003

30. Amino acids substitutions in σ1 and μ1 outer capsid proteins of a Vero cell-adapted mammalian orthoreovirus are required for optimal virus binding and disassembly

Author

Guy Lemay, Véronique Sandekian, and Université de Montréal. Faculté de médecine. Département de microbiologie, infectiologie et immunologie

Subjects

Cancer Research, viruses, Mutant, Orthoreovirus, Mammalian, Virus Attachment, Oncolytic viruses, Reovirus, Biology, Virus oncolytiques, Virus, 03 medical and health sciences, chemistry.chemical_compound, Interferon, Virology, Chlorocebus aethiops, medicine, Animals, Humans, Vero Cells, Génétique inverse, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Virus Assembly, 030302 biochemistry & molecular biology, Virion, Reverse genetics, N-Acetylneuraminic Acid, 3. Good health, Amino acid, Sialic acid, Oncolytic virus, Infectious Diseases, chemistry, Amino Acid Substitution, Vero cell, Réovirus, Capsid Proteins, medicine.drug, HeLa Cells

Abstract

In a recent study, the serotype 3 Dearing strain of mammalian orthoreovirus was adapted to Vero cells; cells that exhibit a limited ability to support the early steps of reovirus uncoating and are unable to produce interferon as an antiviral response upon infection. The Vero cell-adapted virus (VeroAV) exhibits amino acids substitutions in both the σ1 and μ1 outer capsid proteins but no changes in the σ3 protein. Accordingly, the virus was shown not to behave as a classical uncoating mutant. In the present study, an increased ability of the virus to bind at the Vero cell surface was observed and is likely associated with an increased ability to bind onto cell-surface sialic acid residues. In addition, the kinetics of μ1 disassembly from the virions appears to be altered. The plasmid-based reverse genetics approach confirmed the importance of σ1 amino acids substitutions in VeroAV's ability to efficiently infect Vero cells, although μ1 co-adaptation appears necessary to optimize viral infection. This approach of combining in vitro selection of reoviruses with reverse genetics to identify pertinent amino acids substitutions appears promising in the context of eventual reovirus modification to increase its potential as an oncolytic virus., Dans une étude récente, le réovirus de sérotype 3 (souche Dearing) a été adapté aux cellules Vero, cellules qui possèdent une capacité limitée à supporter les étapes précoces de décapsidation de réovirus et qui sont incapables de produire de l'interféron comme réponse antivirale lorsqu'elles sont infectées. Le virus adapté (VeroAV) possède des substitutions d'acides aminés au niveau des protéines de capside externe σ1 et μ1, mais ne présente pas de changement au niveau de la protéine σ3. Comme attendu, le virus ne se comporte donc pas comme un mutant de décapsidation classique. Dans la présente étude, une augmentation de la capacité du virus à se fixer à la surface des cellules Vero a été observée et est probablement associée à une augmentation de la fixation aux acides sialiques de la surface cellulaire. De plus, la cinétique de relâche de μ1 à partir des virions semble altérée. L'approche de génétique inverse a permis de confirmer l'importance des substitutions d'acides aminés de la protéine σ1 dans la capacité de VeroAV à infecter les cellules Vero de manière efficace, bien que la coadaptation de μ1 apparaisse nécessaire pour optimiser l'infection virale. Cette approche combinant la sélection in vitro de réovirus à la génétique inverse pour découvrir des substitutions importantes d'acides aminés apparaît prometteuse dans le contexte de la modification de réovirus afin d'accroître son potentiel en tant que virus oncolytique.

Published

2014

31. A glycosyl hydrolase activity of mammalian reovirus σ1 protein can contribute to viral infection through a mucus layer 1 1Edited by M. Yaniv

Author

Serge Sénéchal, Luc Bernier, Guy Lemay, and Martin Bisaillon

Subjects

chemistry.chemical_classification, Infectivity, Mucin, Biology, biology.organism_classification, Intestinal epithelium, Pichia pastoris, chemistry.chemical_compound, Enzyme, chemistry, Biochemistry, Structural Biology, Glycoside hydrolase, Lysozyme, Glycoprotein, Molecular Biology

Abstract

The mammalian reovirus σ1 protein is responsible for viral attachment to host cells and hemagglutination properties of the virus. In the present study, sequence similarity between σ1 and chicken-type lysozymes prompted us to investigate additional functions of the σ1 protein. Expression in Pichia pastoris yeast cells showed that σ1 can actually cleave lysozyme substrates, including complex sugars found in bacterial cell walls. Replacement by site-directed mutagenesis of acidic amino acid residues in σ1 by their respective isosteric, uncharged, amino acid residues has allowed us to identify Glu36 and Asp54 as the catalytic pair involved in σ1-mediated glycosidase activity. The enzyme appears inactive in virions but its activity is unmasked upon generation of infectious subviral particles (ISVPs) by partial proteolytic removal of the outer capsid proteins. Purified σ1 protein and ISVPs can also hydrolyze mucins, heavily glycosylated glycoproteins that are a major component of the mucus layer overlaying the intestinal epithelium. Furthermore, reovirus infection of epithelial Madin Darby canine kidney cells was inhibited tenfold in cells expressing mucin at their apical surface, while this inhibition was overcome by ISVPs. Unmasking of σ1 mucinolytic activity in the intestine, consecutive to proteolytic cleavage of virions to ISVPs, thus likely contributes to the known increase in infectivity of reovirus ISVPs compared to complete virions. This work presents the first evidence that some mammalian viruses have evolved mechanisms to facilitate their penetration through the protective barrier of the mucus layer in the intestinal tract.

Published

1999

32. [Untitled]

Author

Martin Bisaillon and Guy Lemay

Subjects

chemistry.chemical_classification, Sequence analysis, viruses, virus diseases, General Medicine, Computational biology, biochemical phenomena, metabolism, and nutrition, Biology, Molecular biology, Amino acid, Computer analysis, chemistry, Virology, Genetics, Consensus sequence, Mammalian reovirus, Molecular Biology, Cellular proteins, Sequence (medicine)

Abstract

In the present study, computer-assisted searches for sequence similarities were performed with amino acid sequences from mammalian reovirus proteins. These analysis revealed that many proteins of reovirus are partially similar to known viral or cellular proteins. Consensus sequences have been identified that are in accordance with already suspected functions of reovirus proteins. The analysis has also revealed unexpected similarities of some reovirus proteins with specific classes of proteins which sequences are present in the databases. This could suggest yet unidentified activities for some of the reovirus proteins.

Published

1999

33. Characterization of the Thermosensitive ts453 Reovirus Mutant: Increased dsRNA Binding of ς3 Protein Correlates with Interferon Resistance

Author

Guy Lemay, T Mabrouk, Josée Bergeron, and S. Garzon

Subjects

Vesicle-associated membrane protein 8, viruses, Mutant, Biology, Reoviridae, Antiviral Agents, Cell Line, HSPA4, Mice, Viral Proteins, Capsid, Mutant protein, Virology, HSPA2, Animals, RNA, Double-Stranded, Zinc finger, Temperature, RNA-Binding Proteins, Drug Resistance, Microbial, Interferon-beta, Autophagy-related protein 13, Molecular biology, Zinc, COS Cells, Mutagenesis, Site-Directed, biology.protein, Capsid Proteins, Protein G

Abstract

The mutation harbored by the reovirus ts453 thermosensitive mutant has been assigned to the S4 gene encoding the major outer capsid protein sigma 3. Previous gene sequencing has identified a nonconservative amino acid substitution located near the zinc finger of sigma 3 protein in the mutant. Coexpression in COS cells of the sigma 3 protein presenting this amino acid substitution (N16K), together with the other major capsid protein mu 1, has also revealed an altered interaction between the two proteins; this altered interaction prevents the sigma 3-dependent cleavage of mu 1 to mu 1C. This could explain the lack of outer capsid assembly observed during ts453 virus infection at nonpermissive temperature. In the present study, we pursued the characterization of this mutant sigma 3 protein. Although the N16K mutation is located close to the zinc finger region, it did not affect the ability of the protein to bind zinc. In contrast, this mutation, as well as mutations within the zinc finger motif itself, can increase the binding of the protein to double-stranded RNA (dsRNA). It also appears that the N16K mutant protein is more efficiently transported to the nucleus than the wild-type protein, an observation consistent with the postulated role of dsRNA binding in sigma 3 nuclear presence. The lack of association with mu 1, and/or the increased dsRNA-binding activity of sigma 3, could be responsible for a partial resistance of the ts453 virus to interferon treatment and this could have important consequences in the context of protein synthesis regulation during natural reovirus infection.

Published

1998

34. Characterization of the Reovirus λ1 Protein RNA 5′-Triphosphatase Activity

Author

Guy Lemay and Martin Bisaillon

Subjects

RNA-dependent RNA polymerase, Biology, Binding, Competitive, Biochemistry, GTP Phosphohydrolases, Substrate Specificity, Capsid, Transcription (biology), RNA triphosphatase, Magnesium, Molecular Biology, Manganese, RNA-Binding Proteins, RNA, RNA virus, Cell Biology, biology.organism_classification, Non-coding RNA, RNA Helicase A, Recombinant Proteins, Acid Anhydride Hydrolases, DNA-Binding Proteins, Kinetics, Capsid Proteins, Triphosphatase

Abstract

Characterization of the phosphohydrolytic activities of recombinant reovirus lambda1 protein demonstrates that, in addition to the previously reported nucleoside triphosphate phosphohydrolase and helicase activities, the protein also possesses RNA 5'-triphosphatase activity. This activity was absolutely dependent on the presence of a divalent cation, Mg2+ or Mn2+, and specifically removes the 5'-gamma-phosphate at the end of triphosphate-terminated RNAs. Kinetic competition analysis showed that nucleoside triphosphate phosphohydrolase and RNA 5'-triphosphatase reactions are carried out at a common active site. These results strongly support the idea that, in addition to its role as an RNA helicase during transcription of the viral genome, lambda1 also participates during formation of the cap structure at the 5' end of newly synthesized reovirus mRNAs. The lambda1 protein represents only the third RNA triphosphatase whose primary structure is known and the first described in a double-stranded RNA virus.

Published

1997

35. Viral and Cellular Enzymes Involved in Synthesis of mRNA Cap Structure

Author

Guy Lemay and Martin Bisaillon

Subjects

RNA Caps, chemistry.chemical_classification, Messenger RNA, Methyltransferase, Methyltransferases, Biology, Nucleotidyltransferase, Nucleotidyltransferases, Acid Anhydride Hydrolases, Enzyme, Biochemistry, chemistry, Virology, Viruses, Acid anhydride hydrolases, Animals, Humans

Published

1997

36. Two distinct oncornaviruses harbor an intracytoplasmic tyrosine-based basolateral targeting signal in their viral envelope glycoprotein

Author

Robert Lodge, David Avram Sanders, Lélia Delamarre, M C Dokhélar, Éric A. Cohen, J Alvarado, Guy Lemay, and Jean-Philippe Lalonde

Subjects

Cytoplasm, Phenylalanine, viruses, Molecular Sequence Data, Immunology, Microbiology, Jurkat cells, Cell Line, Jurkat Cells, Mice, Dogs, Retrovirus, Viral envelope, Virology, Murine leukemia virus, Serine, Animals, Humans, Point Mutation, Amino Acid Sequence, Tyrosine, Glycoproteins, Epithelial polarity, chemistry.chemical_classification, Human T-lymphotropic virus 1, biology, Gene Products, env, 3T3 Cells, biology.organism_classification, Molecular biology, chemistry, Insect Science, HIV-1, Moloney murine leukemia virus, Glycoprotein, Research Article

Abstract

It has been clearly established that the budding of the human immunodeficiency virus (HIV-1), a lentivirus, occurs specifically through the basolateral membrane in polarized epithelial cells. More recently, the signal was assigned to a tyrosine-based motif located in the intracytoplasmic domain of the envelope glycoprotein, as previously observed on various other viral and cellular basolateral proteins. In the present study, expression of human T-cell leukemia virus type 1 (HTLV-1) or Moloney murine leukemia virus envelope glycoproteins was used for trans-complementation of an envelope-negative HIV-1. This demonstrated the potential of oncornaviral retrovirus envelope glycoproteins to confer polarized basolateral budding in epithelial Madin-Darby canine kidney cells (MDCK cells). Site-directed mutagenesis confirmed the importance of a common motif encompassing at least one crucial membrane-proximal intracytoplasmic tyrosine residue. The conservation of a similar basolateral maturation signal in different retroviruses further supports its importance in the biology of this group of viruses.

Published

1997

37. Characterization of the Nucleoside Triphosphate Phosphohydrolase and Helicase Activities of the Reovirus λ1 Protein

Author

Guy Lemay, Martin Bisaillon, and Josée Bergeron

Subjects

Cations, Divalent, Reoviridae, Biochemistry, DNA-binding protein, Pichia, Pichia pastoris, law.invention, Capsid, law, Consensus Sequence, Magnesium, Amino Acid Sequence, Cloning, Molecular, Molecular Biology, Peptide sequence, Adenosine Triphosphatases, Nucleoside-triphosphatase, Manganese, biology, DNA Helicases, RNA-Binding Proteins, Helicase, Cell Biology, Nucleoside-Triphosphatase, biology.organism_classification, Molecular biology, Recombinant Proteins, Acid Anhydride Hydrolases, DNA-Binding Proteins, Kinetics, Nucleic acid, biology.protein, Recombinant DNA, Capsid Proteins, Nucleoside

Abstract

Previous studies have shown that the reovirus lambda1 core protein harbors a putative nucleotide-binding motif and exhibits an affinity for nucleic acids. In addition, a nucleoside triphosphate phosphohydrolase activity present in reovirus cores has been recently assigned to lambda1 using gene reassortment analysis. In this study, it was demonstrated that the recombinant lambda1 protein, expressed in the yeast Pichia pastoris, is able to hydrolyze nucleoside 5'-triphosphates or deoxynucleoside 5'-triphosphates. This activity was absolutely dependent on the presence of a divalent cation, Mg2+ or Mn2+. The protein can also unwind double-stranded nucleic acid molecules in the presence of a nucleoside 5'-triphosphate or deoxynucleoside 5'-triphosphate. These results provide the first biochemical evidence that the reovirus lambda1 protein is a nucleoside triphosphate phosphohydrolase/helicase and strongly support the idea that lambda1 participates in transcription of the viral genome.

Published

1997

38. The membrane-proximal intracytoplasmic tyrosine residue of HIV-1 envelope glycoprotein is critical for basolateral targeting of viral budding in MDCK cells

Author

Éric A. Cohen, Robert Lodge, Guy Lemay, and Jean-Philippe Lalonde

Subjects

Signal peptide, Viral budding, Molecular Sequence Data, Biology, Kidney, Virus Replication, medicine.disease_cause, General Biochemistry, Genetics and Molecular Biology, Cell Line, Jurkat Cells, Dogs, Viral Envelope Proteins, Viral envelope, Protein targeting, medicine, Animals, Humans, Amino Acid Sequence, Tyrosine, Molecular Biology, Central element, chemistry.chemical_classification, Membrane Glycoproteins, General Immunology and Microbiology, General Neuroscience, Cell Membrane, Virion, Cell Polarity, Molecular biology, HIV Envelope Protein gp41, chemistry, Viral replication, COS Cells, HIV-1, Mutagenesis, Site-Directed, Glycoprotein, Research Article

Abstract

Budding of retroviruses from polarized epithelial Madin-Darby canine kidney cells (MDCK) takes place specifically at the basolateral membrane surface. This sorting event is suspected to require a specific signal harbored by the viral envelope glycoprotein and it was previously shown that, as for most basolateral proteins, the intracytoplasmic domain plays a crucial role in this targeting phenomenon. It is well known that tyrosine-based motifs are a central element in basolateral targeting signals. In the present study, site-directed mutagenesis was used to generate conservative or non-conservative substitutions of each four intracytoplasmic tyrosines of the human immunodeficiency virus (HIV-1) envelope glycoprotein. This approach revealed that the membrane-proximal tyrosine is essential to ensure both the basolateral localization of envelope glycoprotein and the basolateral targeting of HIV-1 virions. Substitutions of the membrane-proximal tyrosine did not appear to affect incorporation of envelope glycoprotein into the virions, as assayed by virion infectivity and protein content, nor its capability to ensure its role in viral infection, as determined by viral multiplication kinetics. Altogether, these results indicate that the intracytoplasmic domain of the HIV-1 envelope glycoprotein harbors a unique, tyrosine-based, basolateral targeting signal. Such a tyrosine-based targeting signal may play a fundamental role in HIV transmission and pathogenesis.

Published

1997

39. Expression of a reporter gene interrupted by the Candida albicans group I intron is inhibited by base analogs

Author

Pierre Belhumeur, Guy Lemay, Serge Montplaisir, S. Mercure, and Linda Cousineau

Subjects

Antifungal Agents, RNA Splicing, Blotting, Western, Saccharomyces cerevisiae, Flucytosine, Base analog, chemistry.chemical_compound, Genes, Reporter, Gene Expression Regulation, Fungal, Candida albicans, Genetics, Group I catalytic intron, Gene, Reporter gene, biology, Intron, Blotting, Northern, beta-Galactosidase, biology.organism_classification, Molecular biology, Introns, Lac Operon, chemistry, Biochemistry, RNA, Ribosomal, RNA splicing, Mutagenesis, Site-Directed, Nucleic Acid Conformation, Fluorouracil, Cell Division, Research Article

Abstract

We previously reported the identification of an intron (CaLSU) in the 25S ribosomal RNA of some Candida albicans yeast strains. CaLSU was shown to self-splice and has the potential to adopt a secondary structure typical of group I introns. The presence of CaLSU inC. albicans strains correlates with a high degree of susceptibility to base analog antifungal agents, 5-fluorocytosine (5-FC) or 5-fluorouracil (5-FU). Cell death, resulting from addition of base analogs to growing cultures, precluded demonstration of a causal relationship between CaLSU presence and susceptibility to base analogs. In the present study, CaLSU was inserted in a non-essential lacZ reporter gene and expression was examined in Saccharomyces cerevisiae. Different mutations affecting in vitro self-splicing also had similar effects on reporter gene expression in vivo. This indicates that in vivo removal of CaLSU from the reporter gene occurs through the typical self-splicing mechanism of group I introns. Base analogs inhibited expression of the reporter gene product in a concentration-dependent manner upon their addition to the cultures. This supports a model in which disruption of intron secondary structure, consecutive to the incorporation of nucleotide analogs, is a major factor determining the susceptibility of C.albicans cells to base analogs.

Published

1997

40. Sequence analysis of murine leukemia virus envelope gene from inoculated mice

Author

Carole Danis, Eric Rassart, and Guy Lemay

Subjects

biology, Sequence analysis, viruses, biology.organism_classification, Virology, Molecular biology, Virus, Mice, chemistry.chemical_compound, Amino Acid Substitution, Viral Envelope Proteins, chemistry, Viral envelope, Mutation, Murine leukemia virus, Animals, Amino Acid Sequence, RNA extraction, Moloney murine leukemia virus, Sequence Analysis, Gene, Cells, Cultured, DNA, Gammaretrovirus

Abstract

Introduction of amino acids substitutions in murine leukemia virus genome is a powerful method to determine the relative importance of various viral factors in pathogenesis. However, introduction of such amino acids substitution could result in viruses at a selective disadvantage, and eventual selection of revertants. It is thus essential to verify if the mutation is maintained stably in replicating virus and in infected tumor cells. In the present study, viral nucleic acid sequences from diseased animals were determined using different approaches. Small blood samples were found adequate for direct RNA extraction and reverse transcriptase-PCR amplification followed by automated DNA sequencing. Alternatively, replication-competent viruses were recovered specifically by applying blood samples onto permissive cells; viral RNA is then extracted from tissue culture medium and similarly sequenced. Tissue samples were also used to amplify viral sequences from tumors DNA while small pieces of tumors tissues were applied onto permissive cells to isolate replicating viruses. The combined experimental approach was used to show sequence conservation using a mutant altered in the intracytoplasmic region of viral envelope glycoprotein. No difference was observed between viruses recovered directly from the animal and those amplified onto cultured cells.

Published

2005

41. Amino acid substitutions in σ1 and μ1 outer capsid proteins are selected during mammalian reovirus adaptation to Vero cells

Author

Roland Jabre, Guy Lemay, Véronique Sandekian, and Université de Montréal. Faculté de médecine. Département de microbiologie, infectiologie et immunologie

Subjects

Cancer Research, Cell type, viruses, Mutant, Cell, Adaptation, Biological, Mutation, Missense, Virus Attachment, Biology, Reovirus, Uncoating, Reoviridae, Virus, Protein structure, Interferon, Virology, Virus Uncoating, Chlorocebus aethiops, medicine, Animals, Serial Passage, Vero Cells, chemistry.chemical_classification, Viral Load, Amino acid, Infectious Diseases, medicine.anatomical_structure, chemistry, Persistance virale, Décapsidation, Amino Acid Substitution, Viral persistence, Vero cell, Réovirus, Capsid Proteins, medicine.drug

Abstract

Establishment of viral persistence in cell culture has previously led to the selection of mammalian reovirus mutants, although very few of those have been characterized in details. In the present study, reovirus was adapted to Vero cells that, in contrast to classically-used L929 cells, are inefficient in supporting the early steps of reovirus uncoating and are also unable to produce interferon as an antiviral response once infection occurs. The Vero cell-adapted reovirus exhibits amino acids substitutions in both the σ1 and μ1 proteins. This contrasts with uncoating mutants from persistently-infected L929 cells, and various other cell types, that generally harbor amino acids substitutions in the σ3 outer capsid protein. The Vero cell-adapted virus remained sensitive to an inhibitor of lysosomal proteases; furthermore, in the absence of selective pressure for its maintenance, t he virus has partially lost its ability to resist interferon. The positions of the amino acids substitutions on the known protein structures suggest an effect on binding of the viral σ1 protein to the cell surface and on μ1 disassembly from the outer capsid., L'établissement de la persistance virale en culture cellulaire a précédemment mené à la sélection de mutants de réovirus, bien que peu d'entre eux aient été caractérisés en détail. Dans la présence étude, le réovirus a été adapté aux cellules Vero qui, contrairement aux cellules L929 classiquement utilisées, sont peu efficaces pour les étapes précoces de décapsidation de réovirus et sont également incapables de produire de l'interféron comme réponse antivirale, lorsqu'infectées. Le réovirus adapté aux cellules Vero porte des substitutions d'acides aminés à la fois dans les protéines σ1 et μ1. Ceci contraste avec les mutants de décapsidation des cellules L929 infectées de manière persistante, aussi bien que chez divers autres types de cellules, qui présentent généralement des substitutions d'acides aminés au niveau de la protéine de capside externe σ3. Le virus adapté aux cellules Vero demeure sensible à un inhibiteur de protéases lysosomales; de plus, en absence de pression de sélection, le virus a perdu en partie sa capacité à résister à l'interféron. La position des différentes substitutions d'acides aminés sur la structure connue de la protéine suggère un effet sur la fixation de la protéine virale σ1 à la surface cellulaire et sur l'élimination de la protéine μ1 de la capside externe du virus.

Published

2013

42. Candida albicans serotype analysis by flow cytometry

Author

Serge Montplaisir, Serge Sénéchal, S. Mercure, P. Auger, and Guy Lemay

Subjects

Microbiology (medical), Antiserum, Serotype, biology, Fungi imperfecti, Flow Cytometry, biology.organism_classification, Virology, Corpus albicans, Flucytosine, Microbiology, Antigen, Candida albicans, medicine, Humans, Female, Typing, Serotyping, Research Article, medicine.drug

Abstract

Candida albicans strains can be assigned to either of two major serogroups, A or B. Antigenic surface determinants present only in serotype A strains allow such a distinction, which has epidemiologic relevance. Reports have established that the relative distributions of the two serotypes can vary depending on the geographic origin of the isolates. A prevalence of susceptibility to an antifungal agent, flucytosine, was also observed with isolates of serotype A. More recently, it was suggested that the occurrence of serotype B isolates in various clinical forms of candidiasis is increasing. However, this latest finding remains controversial since serotyping results vary widely from one laboratory to another because of the lack of standardized methodologies. Difficulty in interpretation of results, which may lead to erroneous serotype identification, is the major setback associated with current methods. For this study, we thus devised a procedure that relies on flow cytometry and that may eliminate ambiguities in serotype determination. The validation of results was achieved with two types of serotype A-specific antisera, Iatron Factor 6 antiserum and an anti-C. albicans antiserum adsorbed on serotype B yeast cells. Agreement between results obtained with these two reagents was 100% with a wide array of Candida strains. These results confirmed the potential of the flow cytometric procedure as a reliable and reproducible method to establish the serotypes of C. albicans strains. Furthermore, some applications of this procedure to the epidemiological study of this human pathogen are presented.

Published

1996

43. A novel group I intron in Candida dubliniensis is homologous to a Candida albicans intron

Author

Serge Montplaisir, S. Mercure, Hélène Boucher, and Guy Lemay

Subjects

RNA Splicing, Protein subunit, Genes, Fungal, Molecular Sequence Data, Biology, DNA, Ribosomal, Sequence Homology, Nucleic Acid, Candida albicans, Genetics, Humans, Group I catalytic intron, DNA, Fungal, Candida, Base Sequence, Nucleic acid sequence, Intron, RNA, Fungal, General Medicine, Ribosomal RNA, biology.organism_classification, Introns, Corpus albicans, Blotting, Southern, RNA, Ribosomal, Nucleic Acid Conformation, Candida dubliniensis

Abstract

In the present study, we determined the sequence of group I self-splicing introns found in the large ribosomal RNA subunit of Candida albicans, Candida stellatoidea and the recently-described species Candida dubliniensis. It was found that both the intron and ribosomal RNA nucleotide sequences are almost perfectly identical between different C. albicans strains as well as between C. albicans and C. stellatoidea strains. Comparisons of ribosomal RNA sequences suggest that local isolates of atypical C. albicans from individuals infected with human immunodeficiency virus can be assigned to the C. dubliniensis species. C. dubliniensis strains also harbor a group I intron in their ribosomal RNA, as observed in about 40% of C. albicans strains and all C. stellatoidea strains. This novel C. dubliniensis group I intron is identical to the C. albicans and C. stellatoidea intron, except for two widely divergent stem-loop regions. Despite these differences, the C. dubliniensis intron possesses self-splicing ability in an in vitro assay. Taken together, these data support the idea that C. albicans and C. stellatoidea should be joined together as variants of the same species while C. dubliniensis is a distinct but closely related microorganism. To our knowledge, the C. albicans and C. dubliniensis introns are the first example of a pair of homologous group I introns differing only by the presence of apparently facultative sequences in some stem-loops suspected to be involved in stabilization of tertiary structure.

Published

1996

44. Transient high level mammalian reovirus replication in a bat epithelial cell line occurs without cytopathic effect

Author

Patrick Prud’homme, Guy Lemay, Véronique Sandekian, Debbie Lim, and Université de Montréal. Faculté de médecine. Département de microbiologie, infectiologie et immunologie

Subjects

Cancer Research, Cell type, Cell Survival, viruses, bat, virus, Biology, reovirus, Reoviridae, Virus Replication, Virus, Cell Line, Transduction (genetics), Cytopathogenic Effect, Viral, Interferon, Transduction, Genetic, Virology, Chiroptera, medicine, Animals, Cytopathic effect, Cell growth, chauve-souris, Epithelial Cells, interferon, interféron, Infectious Diseases, réovirus, Viral replication, Cell culture, medicine.drug

Abstract

Mammalian reoviruses exhibit a large host range and infected cells are generally killed; however, most studies examined only a few cell types and host species, and are probably not representative of all possible interactions between virus and host cell. Many questions thus remain concerning the nature of cellular factors that affect viral replication and cell death. In the present work, it was observed that replication of the classical mammalian reovirus serotype 3 Dearing in a bat epithelial cell line, Tb1.Lu, does not result in cell lysis and is rapidly reduced to very low levels. Prior uncoating of virions by chymotrypsin treatment, to generate infectious subviral particles, increased the initial level of infection but without any significant effect on further viral replication or cell survival. Infected cells remain resistant to virus reinfection and secrete an antiviral factor, most likely interferon, that is protective against the unrelated encephalomyocarditis virus. Although, the transformed status of a cell is believed to promote reovirus replication and viral “oncolysis”, resistant Tb1.Lu cells exhibit a classical phenotype of transformed cells by forming colonies in semisolid soft agar medium. Further transduction of Tb.Lu cells with a constitutively-active Ras oncogene does not seem cell growth or reovirus effect on these cells. Infected Tb1.Lu cells can produce low-level of infectious virus for a long time without any apparent effect, although these cells are resistant to reinfection. The results suggest that Tb1.Lu cells can mount an unusual antiviral response. Specific properties of bat cells may thus be in part responsible for the ability of the animals to act as reservoirs for viruses in general and for novel reoviruses in particular. Their peculiar resistance to cell lysis also makes Tb1.Lu cells an attractive model to study the cellular and viral factors that determine the ability of reovirus to replicate and destroy infected cells., Les réovirus de mammifères possèdent un large spectre d'hôtes et les cellules infectées sont généralement tuées par l'infection ; cependant, la plupart des études utilisent seulement certains types de cellules provenant de quelques espèces animales. Ceci n'est sans doute pas représentatif de toutes les interactions possibles entre virus et cellule hôte. Plusieurs questions demeurent concernant la nature des facteurs cellulaires qui affectent la réplication virale et la mort cellulaire. Dans la présente étude, il a été observé que la réplication du classique réovirus de mammifères (sérotype 3 Dearing) dans une lignée de cellules épithéliales de chauve-souris, Tb1.Lu, n'entraîne pas la lyse cellulaire et est rapidement réduite à un très faible niveau. La décapsidation des virions par traitement à la chymotrypsine, afin de générer des particules dites « sous-virales infectieuses », augmente le niveau initial d'infection sans effet significatif sur la réplication virale ou la survie cellulaire. Les cellules infectées demeurent résistantes à la réinfection et sécrètent un facteur antiviral, probablement de l'interféron, qui peut protéger contre l'infection par le virus de l'encéphalomyocardite. Malgré le fait que le statut de transformation cellulaire est considéré comme pouvant promouvoir la réplication de réovirus et l'oncolyse virale, les cellules Tb1.Lu résistantes démontrent un phénotype classique de cellules transformées et forment des colonies en milieu semi-solide contenant de l'agar. La transduction de cellules Tb1.Lu avec un oncogène Ras constitutivement actif ne semble pas affecter la croissance cellulaire ni la réplication virale. Les cellules Tb1.Lu infectées peuvent produire une faible quantité de virus infectieux pour une longue période sans effet apparent, malgré le fait que ces cellules soient résistantes à la réinfection. Ces résultats suggèrent que les cellules Tb1.Lu peuvent développer une réponse antivirale inhabituelle. Les propriétés spécifiques des cellules de chauve-souris pourraient donc être en partie responsables de la capacité de ces animaux à agir comme réservoirs de virus en général et de nouveaux réovirus en particulier. Leur résistance particulière à la lyse cellulaire fait aussi de ces cellules un modèle attrayant pour étudier les facteurs cellulaires et viraux qui déterminent la capacité de réovirus à se répliquer et à détruire les cellules infectées.

Published

2012

45. [Taming our enemies to make them our allies: cancer 'virotherapy']

Author

Guy, Lemay

Subjects

Oncolytic Virotherapy, Disease Models, Animal, Biomedical Research, Organ Specificity, Virus Diseases, Neoplasms, Animals, Humans, Molecular Targeted Therapy, Host Specificity, Virus Physiological Phenomena

Published

2012

46. Further characterization and determination of the single amino acid change in the tsI138 reovirus thermosensitive mutant

Author

Guy Lemay, Martin Bisaillon, and Université de Montréal. Faculté de médecine. Département de microbiologie, infectiologie et immunologie

Subjects

Models, Molecular, Immunology, Mutant, virus, Biology, medicine.disease_cause, Reoviridae, reovirus, Applied Microbiology and Biotechnology, Microbiology, Cell Line, Mice, Protein structure, Genetics, Viral structural protein, medicine, Animals, Molecular Biology, Gene, chemistry.chemical_classification, Mutation, Virus Assembly, Temperature, RNA, General Medicine, Molecular biology, Amino acid, Protein Structure, Tertiary, Enzyme, Phenotype, chemistry, Biochemistry, Amino Acid Substitution, réovirus, RNA, Viral, Capsid Proteins

Abstract

Many temperature-sensitive mutants have been isolated in early studies of mammalian reovirus. However, the bio- logical properties and nature of the genetic alterations remain incompletely explored for most of these mutants. The mutation harbored by the tsI138 mutant was already assigned to the L3 gene encoding the l1 protein. In the present study, this mu- tant was further studied as a possible tool to establish the role of the putative l1 enzymatic activities in viral multiplication. It was observed that synthesis of viral proteins is only marginally reduced, while it was difficult to recover viral particles at the nonpermissive temperature. A single nucleotide substitution resulting in an amino acid change was found; the position of this amino acid is consistent with a probable defect in assembly of the inner capsid at the nonpermissive temperature., Plusieurs mutants thermosensibles ont été rapidement isolés dès le début de l’étude du réovirus de mammifères. Cependant, les propriétés biologiques et la nature des changements génétiques demeurent peu connues pour la plupart de ces mutants. La mutation au sein du mutant tsI138 a déjà été localisée comme étant présente sur le gène L3 codant pour la protéine l1. Dans la présente étude, ce mutant a été étudié davantage comme outil possible pour établir le rôle des poten- tielles activités enzymatiques de l1 dans la multiplication virale. Il a été observé que la synthèse des protéines virales est peu affectée alors qu’il est difficile de récupérer des particules virales à température non permissive. La substitution d’un seul nucléotide, entraînant le changement d’un acide aminé, a été retrouvée; la position de cet acide aminé est compatible avec un défaut probable d’assemblage de la capside interne à la température non permissive.

Published

2012

47. Role of glycosylation in transport and enzymic activity of neutral endopeptidase-24.11

Author

Guy Boileau, Qiong Wang, M.-H. Lafrance, Guy Lemay, Philippe Crine, and C. Vezina

Subjects

Glycosylation, Immunoblotting, Golgi Apparatus, Endoplasmic Reticulum, Transfection, Biochemistry, Cell Line, Cell membrane, chemistry.chemical_compound, medicine, Animals, Computer Simulation, Molecular Biology, chemistry.chemical_classification, biology, Endoplasmic reticulum, Cell Membrane, fungi, Mutagenesis, Biological Transport, DNA, Cell Biology, Enzyme assay, medicine.anatomical_structure, Enzyme, chemistry, Ectodomain, Cell culture, Mutation, Mutagenesis, Site-Directed, biology.protein, Electrophoresis, Polyacrylamide Gel, Neprilysin, Research Article

Abstract

Neutral endopeptidase (NEP, EC 3.4.24.11) is a major ectoenzyme of the brush-border membrane. The ectodomain of NEP contains five putative N-glycosylation sites. In order to determine the role of the addition of sugar moieties on the activity and intracellular transport of NEP, we have used site-directed mutagenesis to remove all or some of the five potential sites of sugar addition in membrane-bound and secreted forms of the enzyme. Expression of NEP glycosylation mutants in COS-1 cells showed that all five sites are used for sugar addition. Immunoblotting of NEP in COS-1 cell extracts or culture media indicated that total expression of normal membrane-bound NEP was not affected by mutations at glycosylation sites, whereas this expression level appeared to be strictly dependent on the number of glycosylation sites retained on the soluble form. The transport to the cell surface was also reduced by decreased glycosylation, but again the phenomenon appeared more drastic in the case of the soluble form than for the membrane-bound enzyme. Enzyme activity was decreased by deglycosylation. However, the presence of either of two crucial sites (sites 1 and 5; numbered from the N-terminus of the protein) was sufficient to recover close-to-normal enzymic activities. Transport to the cell surface and enzyme activity of NEP are thus both dependent on sugar residues, probably through different conformational constraints. These constraints seem to be local for enzyme activity but more global for transport to the cell surface.

Published

1994

48. The intracytoplasmic domain of gp41 mediates polarized budding of human immunodeficiency virus type 1 in MDCK cells

Author

Robert Lodge, Dana Gabuzda, H. Göttlinger, Guy Lemay, and Éric A. Cohen

Subjects

Cytoplasm, HIV Antigens, viruses, Viral budding, Immunology, Gene Products, gag, Protein Sorting Signals, Biology, Virus Replication, Gp41, gag Gene Products, Human Immunodeficiency Virus, Microbiology, Virus, Cell Line, HIV Envelope Protein gp160, Viral Proteins, Dogs, Viral envelope, Virology, Animals, Cloning, Molecular, Protein Precursors, Viral shedding, Viral matrix protein, Gene Products, env, virus diseases, Biological Transport, HIV Envelope Protein gp41, Virus Release, Viral replication, Insect Science, Mutation, HIV-1, Research Article

Abstract

Human immunodeficiency virus type 1 (HIV-1) has been shown to exhibit a specific basolateral release in polarized epithelial cells. Previous investigators have used vaccinia virus recombinants expressing HIV proteins to demonstrate that virus release is nonpolarized in the absence of viral envelope glycoproteins. In this study, we developed a transient expression system which allows the use of Madin-Darby canine kidney polarized epithelial cells directly grown on semipermeable membranes. This procedure allowed us to investigate polarized HIV viral budding following introduction of proviral DNA constructs. Expression of env gene products in trans demonstrated the ability to polarize env-negative viruses in a dose-dependent manner. The targeting signal for polarized virus release was shown to be present in the envelope gp41 transmembrane protein and absent from the gp120 portion of env. At least part of this signal is within the gp41 intracytoplasmic domain. Mutants of the p17gag matrix protein were shown to be nonpolarized only when unable to interact with the envelope glycoproteins. Together, these data are consistent with a model of polarized virus budding in which capsid proteins, lacking a targeting signal, are targeted for specific basolateral release via an interaction of p17 with the envelope glycoprotein containing the polarization signal in its intracytoplasmic domain.

Published

1994

49. The Sequence Similarity of Reovirus σ3 Protein To Picornaviral Proteases Is Unrelated to Its Role in μ1 Viral Protein Cleavage

Author

Guy Lemay and T Mabrouk

Subjects

Proteases, Viral protein, Proteolysis, Molecular Sequence Data, Reoviridae, Cleavage (embryo), medicine.disease_cause, Virus, Cell Line, Structure-Activity Relationship, Viral Proteins, Capsid, Virology, Chlorocebus aethiops, Endopeptidases, medicine, Animals, Amino Acid Sequence, COS cells, Expression vector, biology, medicine.diagnostic_test, RNA-Binding Proteins, biology.organism_classification, Biochemistry, Mutagenesis, Site-Directed, Capsid Proteins, Protein Processing, Post-Translational

Abstract

Recent data have shown that the reovirus sigma 3 protein is the only viral product required for proteolytic conversion of the viral mu 1 protein to mu 1C. In an effort to determine the importance of a sigma 3 region exhibiting sequence similarity to a functionally important region of picornaviral proteases, we analyzed proteins produced in COS cells cotransfected with expression vectors encoding mu 1 and either wild-type or mutated forms of sigma 3. This approach revealed that association with sigma 3 contributes to the stability of mu 1-related polypeptides (mu 1 + mu 1C), but conservation of the sigma 3 region related to picornaviral proteases is not required for proteolytic conversion of mu 1 to mu 1C.

Published

1994

50. HTLV-3 and HTLV-4 antisense proteins activate JunB-, c-Jun- and JunD-dependent transcription

Author

Émilie Larocque, Jean-Michel Mesnard, William M. Switzer, Benoit Barbeau, and Guy Lemay

Subjects

lcsh:Immunologic diseases. Allergy, JUNB, viruses, c-jun, bZIP domain, Transfection, Biology, Molecular biology, Transactivation, Infectious Diseases, Transcription (biology), Virology, Meeting Abstract, Gene expression, lcsh:RC581-607, Transcription factor

Abstract

Background The antisense transcript-encoded HBZ protein acts upon viral and cellular gene expression through its modulation of the activation of transcription factors such as Jun family members. A possible link between HBZ and ATL development has also been highlighted. HTLV-3 and HTLV-4 are two newly discovered human retroviruses closely related to HTLV-1; no known diseases have yet been associated to these viruses. Based on previous in silico analyses, our aim was to test for the presence of antisense transcripts in these new viruses and to functionally assess these viral proteins. Results By RT-PCR analyses, HTLV-3 and HTLV-4 were shown to produce spliced antisense transcripts termed APH (Antisense Protein of HTLV)-3 and APH-4. Confocal microscopy analyses of cells expressing Myc- or GFP-tagged APH-3 and APH-4 showed distinct localization but partial colocalization with HBZ to the nucleus and the nucleoli. Using LTR-luciferase constructs, we demonstrated that APH-3 and APH-4 inhibited Tax1 and Tax3 transactivation of respective LTRs. In transfection experiments with a collagenase promoter-driven luciferase reporter construct, we showed that APH-3 and APH-4 modulated JunB- and c-Jun-dependent transcription differently from HBZ. Deletion mutants indicated that this upregulation of the transactivation potential of Jun factors was mediated through the atypical bZIP domain of APH-3 and APH-4. Conclusion We show that HTLV-3 and HTLV-4 express new viral proteins, APH-3 and APH-4, which modulate Jundependent transcription differently from HBZ. These data underscore the importance of our study on APH-3 and APH-4 to help in better understanding the role of HBZ in the development of ATL.

Published

2011