Your search keyword '"Retroviridae Infections physiopathology"' showing total 112 results

1. Human reproduction is regulated by retrotransposons derived from ancient Hominidae-specific viral infections.

Author

Xiang X, Tao Y, DiRusso J, Hsu FM, Zhang J, Xue Z, Pontis J, Trono D, Liu W, and Clark AT

Subjects

Animals, Endogenous Retroviruses genetics, Enhancer Elements, Genetic, Gene Expression Regulation, Developmental, Germ Cells physiology, Germ Cells virology, Hominidae genetics, Hominidae physiology, Humans, Retroviridae Infections physiopathology, Transcription Factors genetics, Transcription Factors metabolism, Endogenous Retroviruses physiology, Hominidae virology, Reproduction, Retroelements, Retroviridae Infections virology

Abstract

Germ cells are essential to pass DNA from one generation to the next. In human reproduction, germ cell development begins with the specification of primordial germ cells (PGCs) and a failure to specify PGCs leads to human infertility. Recent studies have revealed that the transcription factor network required for PGC specification has diverged in mammals, and this has a significant impact on our understanding of human reproduction. Here, we reveal that the Hominidae-specific Transposable Elements (TEs) LTR5Hs, may serve as TEENhancers (TE Embedded eNhancers) to facilitate PGC specification. LTR5Hs TEENhancers become transcriptionally active during PGC specification both in vivo and in vitro with epigenetic reprogramming leading to increased chromatin accessibility, localized DNA demethylation, enrichment of H3K27ac, and occupation of key hPGC transcription factors. Inactivation of LTR5Hs TEENhancers with KRAB mediated CRISPRi has a significant impact on germ cell specification. In summary, our data reveals the essential role of Hominidae-specific LTR5Hs TEENhancers in human germ cell development., (© 2022. The Author(s).)

Published

2022

2. Avian leukosis virus subgroup J and reticuloendotheliosis virus coinfection induced TRIM62 regulation of the actin cytoskeleton.

Author

Li L, Zhuang P, Cheng Z, Yang J, Bi J, and Wang G

Subjects

Actin Cytoskeleton genetics, Actin Cytoskeleton metabolism, Animals, Avian Leukosis physiopathology, Avian Leukosis virology, Avian Leukosis Virus physiology, Avian Proteins metabolism, Coinfection physiopathology, Coinfection virology, Poultry Diseases virology, Reticuloendotheliosis virus physiology, Retroviridae Infections physiopathology, Retroviridae Infections virology, Tripartite Motif Proteins metabolism, Avian Proteins genetics, Coinfection veterinary, Gene Expression Regulation, Poultry Diseases physiopathology, Retroviridae Infections veterinary, Tripartite Motif Proteins genetics

Abstract

Background: Coinfection with avian leukosis virus subgroup J (ALV-J) and reticuloendotheliosis virus (REV) is common in chickens, and the molecular mechanism of the synergistic pathogenic effects of the coinfection is not clear. Exosomes have been identified as new players in the pathogenesis of retroviruses. The different functions of exosomes depend on their cargo components., Objectives: The aim of this study was to investigate the function of co-regulation differentially expressed proteins in exosomes on coinfection of ALV-J and REV., Methods: Here, viral replication in CEF cells infected with ALV-J, REV or both was detected by immunofluorescence microscopy. Then, we analyzed the exosomes isolated from supernatants of chicken embryo fibroblast (CEF) cells single infected and coinfected with ALV-J and REV by mass spectrometry. KEGG pathway enrichment analyzed the co-regulation differentially expressed proteins in exosomes. Next, we silenced and overexpressed tripartite motif containing 62 (TRIM62) to evaluate the effects of TRIM62 on viral replication and the expression levels of NCK-association proteins 1 (NCKAP1) and actin-related 2/3 complex subunit 5 (ARPC5) determined by quantitative reverse transcription polymerase chain reaction., Results: The results showed that coinfection of ALV-J and REV promoted the replication of each other. Thirty proteins, including TRIM62, NCK-association proteins 1 (NCKAP1, also known as Nap125), and Arp2/3-5, ARPC5, were identified. NCKAP1 and ARPC5 were involved in the actin cytoskeleton pathway. TRIM62 negatively regulated viral replication and that the inhibition of REV was more significant than that on ALV-J in CEF cells coinfected with TRIM62. In addition, TRIM62 decreased the expression of NCKAP1 and increased the expression of ARPC5 in coinfected CEF cells., Conclusions: Collectively, our results indicated that coinfection with ALV-J and REV competitively promoted each other's replication, the actin cytoskeleton played an important role in the coinfection mechanism, and TRIM62 regulated the actin cytoskeleton., Competing Interests: The authors declare no conflicts of interest., (© 2020 The Korean Society of Veterinary Science.)

Published

2020

3. Up-to-date knowledge about the association between multiple sclerosis and the reactivation of human endogenous retrovirus infections.

Author

Arneth B

Subjects

Humans, Endogenous Retroviruses, Multiple Sclerosis complications, Multiple Sclerosis physiopathology, Retroviridae Infections complications, Retroviridae Infections physiopathology

Abstract

Background: Although existing studies show that reactivation of the human endogenous retrovirus (HERVs) plays a leading role in multiple sclerosis (MS) progression, the practitioners are yet to establish effective approaches for managing MS without jeopardizing the patients' immune systems., Aim: To provide up-to-date knowledge on the specific roles played by the reactivation of the HERVs in the pathogenesis of MS., Materials and Methods: A systematic review of 70 peer-reviewed journals accessed via PubMed was conducted. The searches generated more than 600 sources that were evaluated based on three step in and exclusion criteria. The selected sources were critically analyzed vis-à-vis the paper's hypothesis which posits that the HERVs reactivation does not directly cause the MS, but triggers a demyelination process by promoting the pathogenic effects of the retroviruses. The paper further documents the advancements in the therapeutic applications resulting from the immunohistological analysis and pathological studies aimed at minimizing the adverse consequences of the HERVs reactivation., Results and Discussions: Only three out of the 70 reviewed sources did not find provide evidence linking the reactivation of HERV and MS progression. On the other hand, overwhelming pieces of evidence confirm that the reactivations often drive the demyelinating plaques by initiating microglial inflammation. Pathological examinations reveal that the inflammatory monocytes (Ly6ChiCCR2 + CX3CR1lo) trigger the reactivation of the malignant T cells that are responsible for the progression of MS. These findings are promoting new discoveries as far as managing MS is concerned.

Published

2018

4. Mouse Siglec-1 Mediates trans-Infection of Surface-bound Murine Leukemia Virus in a Sialic Acid N-Acyl Side Chain-dependent Manner.

Author

Erikson E, Wratil PR, Frank M, Ambiel I, Pahnke K, Pino M, Azadi P, Izquierdo-Useros N, Martinez-Picado J, Meier C, Schnaar RL, Crocker PR, Reutter W, and Keppler OT

Subjects

Animals, Binding Sites, Cell Line, Gangliosides chemistry, Gangliosides metabolism, Host-Pathogen Interactions physiology, Humans, Interferon-alpha physiology, Leukemia, Experimental physiopathology, Leukemia, Experimental virology, Lymphocytes physiology, Lymphocytes virology, Macrophages physiology, Mice, Mice, Inbred C57BL, Mice, Knockout, Models, Molecular, Moloney murine leukemia virus genetics, Moloney murine leukemia virus physiology, N-Acetylneuraminic Acid chemistry, Receptors, Virus chemistry, Receptors, Virus physiology, Retroviridae Infections physiopathology, Retroviridae Infections virology, Sialic Acid Binding Ig-like Lectin 1 genetics, Tumor Virus Infections physiopathology, Tumor Virus Infections virology, Moloney murine leukemia virus pathogenicity, Sialic Acid Binding Ig-like Lectin 1 chemistry, Sialic Acid Binding Ig-like Lectin 1 physiology

Abstract

Siglec-1 (sialoadhesin, CD169) is a surface receptor on human cells that mediates trans-enhancement of HIV-1 infection through recognition of sialic acid moieties in virus membrane gangliosides. Here, we demonstrate that mouse Siglec-1, expressed on the surface of primary macrophages in an interferon-α-responsive manner, captures murine leukemia virus (MLV) particles and mediates their transfer to proliferating lymphocytes. The MLV infection of primary B-cells was markedly more efficient than that of primary T-cells. The major structural protein of MLV particles, Gag, frequently co-localized with Siglec-1, and trans-infection, primarily of surface-bound MLV particles, efficiently occurred. To explore the role of sialic acid for MLV trans-infection at a submolecular level, we analyzed the potential of six sialic acid precursor analogs to modulate the sialylated ganglioside-dependent interaction of MLV particles with Siglec-1. Biosynthetically engineered sialic acids were detected in both the glycolipid and glycoprotein fractions of MLV producer cells. MLV released from cells carrying N-acyl-modified sialic acids displayed strikingly different capacities for Siglec-1-mediated capture and trans-infection; N-butanoyl, N-isobutanoyl, N-glycolyl, or N-pentanoyl side chain modifications resulted in up to 92 and 80% reduction of virus particle capture and trans-infection, respectively, whereas N-propanoyl or N-cyclopropylcarbamyl side chains had no effect. In agreement with these functional analyses, molecular modeling indicated reduced binding affinities for non-functional N-acyl modifications. Thus, Siglec-1 is a key receptor for macrophage/lymphocyte trans-infection of surface-bound virions, and the N-acyl side chain of sialic acid is a critical determinant for the Siglec-1/MLV interaction., (© 2015 by The American Society for Biochemistry and Molecular Biology, Inc.)

Published

2015

5. Murine leukemia virus Gag localizes to the uropod of migrating primary lymphocytes.

Author

Li F, Sewald X, Jin J, Sherer NM, and Mothes W

Subjects

Animals, B-Lymphocytes cytology, Cell Membrane virology, Cell Movement, Cell Polarity, Cells, Cultured, Friend murine leukemia virus genetics, Gene Products, gag genetics, Mice, Protein Transport, Retroviridae Infections physiopathology, Retroviridae Infections virology, Rodent Diseases physiopathology, T-Lymphocytes cytology, B-Lymphocytes virology, Friend murine leukemia virus metabolism, Gene Products, gag metabolism, Retroviridae Infections veterinary, Rodent Diseases virology, T-Lymphocytes virology

Abstract

Unlabelled: B and CD4(+) T lymphocytes are natural targets of murine leukemia virus (MLV). Migrating lymphocytes adopt a polarized morphology with a trailing edge designated the uropod. Here, we demonstrate that MLV Gag localizes to the uropod in polarized B cells and CD4(+) T cells. The uropod localization of MLV Gag was dependent on plasma membrane (PM) association and multimerization of Gag but independent of the viral glycoprotein Env. Basic residues in MA that are required for MLV Gag recruitment to virological synapses between HEK293 and XC cells were dispensable for uropod localization in migrating B cells. Ultrastructural studies indicated that both wild-type and basic-residue mutant Gag localized to the outer surface of the PM at the uropod. Late-domain mutant virus particles were seen at the uropod in form of budding-arrested intermediates. Finally, uropods mediated contact between MLV-infected B cells and uninfected T cells to form virological synapses. Our results suggest that MLV, not unlike HIV, accumulates at the uropod of primary lymphocytes to facilitate viral spreading through the formation of uropod-mediated cell-cell contacts., Importance: Viruses have evolved mechanisms to coordinate their assembly and budding with cell polarity to facilitate their spreading. In this study, we demonstrated that the viral determinants for MLV Gag to localize to the uropod in polarized B cells are distinct from the requirements to localize to virological synapses in transformed cell lines. Basic residues in MA that are required for the Gag localization to virological synapses between HEK293 and XC cells are dispensable for Gag localization to the uropod in primary B cells. Rather, plasma membrane association and capsid-driven multimerization of Gag are sufficient to drive MLV Gag to the uropod. MLV-laden uropods also mediate contacts between MLV-infected B cells and uninfected T cells to form virological synapses. Our results indicate that MLV accumulates at the uropod of primary lymphocytes to facilitate viral spreading through the formation of uropod-mediated cell-cell contacts., (Copyright © 2014, American Society for Microbiology. All Rights Reserved.)

Published

2014

6. Postinhibitory rebound neurons and networks are disrupted in retrovirus-induced spongiform neurodegeneration.

Author

Li Y, Davey RA, Sivaramakrishnan S, and Lynch WP

Subjects

Action Potentials physiology, Animals, Antigens metabolism, Calcium metabolism, Gene Products, env metabolism, Hearing Loss physiopathology, Inferior Colliculi physiopathology, Inferior Colliculi virology, Leukemia, Experimental physiopathology, Membrane Potentials physiology, Mice, Microglia physiology, Microglia virology, Neural Pathways physiopathology, Neuroglia physiology, Neuroglia virology, Neurons virology, Patch-Clamp Techniques, Proteoglycans metabolism, Retroviridae Infections virology, Tissue Culture Techniques, Tumor Virus Infections virology, Voltage-Sensitive Dye Imaging, Leukemia Virus, Murine physiology, Neurodegenerative Diseases physiopathology, Neurons physiology, Retroviridae Infections physiopathology, Tumor Virus Infections physiopathology

Abstract

Certain retroviruses induce progressive spongiform motor neuron disease with features resembling prion diseases and amyotrophic lateral sclerosis. With the neurovirulent murine leukemia virus (MLV) FrCasE, Env protein expression within glia leads to postsynaptic vacuolation, cellular effacement, and neuronal loss in the absence of neuroinflammation. To understand the physiological changes associated with MLV-induced spongiosis, and its neuronal specificity, we employed patch-clamp recordings and voltage-sensitive dye imaging in brain slices of the mouse inferior colliculus (IC), a midbrain nucleus that undergoes extensive spongiosis. IC neurons characterized by postinhibitory rebound firing (PIR) were selectively affected in FrCasE-infected mice. Coincident with Env expression in microglia and in glia characterized by NG2 proteoglycan expression (NG2 cells), rebound neurons (RNs) lost PIR, became hyperexcitable, and were reduced in number. PIR loss and hyperexcitability were reversed by raising internal calcium buffer concentrations in RNs. PIR-initiated rhythmic circuits were disrupted, and spontaneous synchronized bursting and prolonged depolarizations were widespread. Other IC neuron cell types and circuits within the same degenerative environment were unaffected. Antagonists of NMDA and/or AMPA receptors reduced burst firing in the IC but did not affect prolonged depolarizations. Antagonists of L-type calcium channels abolished both bursts and slow depolarizations. IC infection by the nonneurovirulent isogenic virus Friend 57E (Fr57E), whose Env protein is structurally similar to FrCasE, showed no RN hyperactivity or cell loss; however, PIR latency increased. These findings suggest that spongiform neurodegeneration arises from the unique excitability of RNs, their local regulation by glia, and the disruption of this relationship by glial expression of abnormal protein., (Copyright © 2014 the American Physiological Society.)

Published

2014

7. Effects of simian betaretrovirus serotype 1 (SRV1) infection on the differentiation of hematopoietic progenitor cells (CD34+) derived from bone marrow of rhesus macaques (Macaca mulatta).

Author

Montiel NA, Todd PA, Yee J, and Lerche NW

Subjects

Animals, Animals, Laboratory, Antigens, CD34 metabolism, Hematopoietic Stem Cells virology, In Vitro Techniques, Myeloid Progenitor Cells, Real-Time Polymerase Chain Reaction veterinary, Retroviridae Infections physiopathology, Reverse Transcriptase Polymerase Chain Reaction veterinary, Stromal Cells virology, Betaretrovirus, Cell Differentiation physiology, Hematopoietic Stem Cells physiology, Macaca mulatta, Monkey Diseases physiopathology, Monkey Diseases virology, Retroviridae Infections veterinary

Abstract

Peripheral blood cytopenias, particularly persistent anemia and neutropenia, are commonly associated with simian betaretrovirus infection of Asian monkeys of the genus Macaca. The pathogenetic mechanisms underlying these hematologic abnormalities are not well understood. The current study investigated the in vitro tropism of simian betaretrovirus (SRV) for both hematopoietic progenitor (CD34(+)) and stromal cells obtained from rhesus macaque bone marrow and assessed the effects of infection on hematopoietic progenitor cell differentiation in vitro. After in vitro exposure, SRV proviral DNA could be demonstrated by real-time PCR in cells and the reverse transcriptase assay in supernatants from SRV-exposed progenitor-associated stroma, but not in differentiated colonies derived from SRV-exposed progenitors. Furthermore, in vitro exposure involving cell-cell contact of uninfected CD34(+) progenitor cells with SRV-infected stromal cells resulted in a statistically significant reduction in granulocyte-macrophage colony formation in absence of detectable SRV-infection of progenitor cells. Reduction in colony formation occurred in a 'dose-dependent' fashion with increasing contact time. No effects on erythroid lineages and RBC differentiation were noted. Our results suggest that hematologic abnormalities observed during SRV disease (natural or experimental) of rhesus macaques may not result from direct effects of viral infection of progenitor cell populations, but rather be (at least in part) a consequence of SRV infection of supportive bone marrow stroma with secondary effects on differentiation of associated progenitor cells.

Published

2012

8. In situ force mapping of mammary gland transformation.

Author

Lopez JI, Kang I, You WK, McDonald DM, and Weaver VM

Subjects

Animals, Bioengineering, Biomechanical Phenomena, Biophysical Phenomena, Cell Transformation, Neoplastic, Extracellular Matrix physiology, Female, Mammary Glands, Animal physiology, Mammary Tumor Virus, Mouse, Mice, Mice, Transgenic, Microscopy, Atomic Force, Neoplasm Invasiveness physiopathology, Retroviridae Infections etiology, Retroviridae Infections physiopathology, Tensile Strength, Tumor Virus Infections etiology, Tumor Virus Infections physiopathology, Vitrification, Mammary Neoplasms, Experimental etiology, Mammary Neoplasms, Experimental physiopathology

Abstract

Tumor progression is characterized by an incremental stiffening of the tissue. The importance of tissue rigidity to cancer is appreciated, yet the contribution of specific tissue elements to tumor stiffening and their physiological significance remains unclear. We performed high-resolution atomic force microscopy indentation in live and snap-frozen fluorescently labeled mammary tissues to explore the origin of the tissue stiffening associated with mammary tumor development in PyMT mice. The tumor epithelium, the tumor-associated vasculature and the extracellular matrix all contributed to mammary gland stiffening as it transitioned from normal to invasive carcinoma. Consistent with the concept that extracellular matrix stiffness modifies cell tension, we found that isolated transformed mammary epithelial cells were intrinsically stiffer than their normal counterparts but that the malignant epithelium in situ was far stiffer than isolated breast tumor cells. Moreover, using an in situ vitrification approach, we determined that the extracellular matrix adjacent to the epithelium progressively stiffened as tissue evolved from normal through benign to an invasive state. Importantly, we also noted that there was significant mechanical heterogeneity within the transformed tissue both in the epithelium and the tumor-associated neovasculature. The vascular bed within the tumor core was substantially stiffer than the large patent vessels at the invasive front that are surrounded by the stiffest extracellular matrix. These findings clarify the contribution of individual mammary gland tissue elements to the altered biomechanical landscape of cancerous tissues and emphasize the importance of studying cancer cell evolution under conditions that preserve native interactions.

Published

2011

9. Relationships among rhinitis, fibromyalgia, and chronic fatigue.

Author

Baraniuk JN and Zheng Y

Subjects

Animals, Diagnosis, Differential, Fatigue Syndrome, Chronic etiology, Fatigue Syndrome, Chronic pathology, Fatigue Syndrome, Chronic physiopathology, Fibromyalgia, Humans, Irritable Bowel Syndrome, Leukemia Virus, Murine pathogenicity, Magnetic Resonance Imaging, Mice, Nociceptors pathology, Practice Guidelines as Topic, Retroviridae Infections complications, Retroviridae Infections pathology, Retroviridae Infections physiopathology, Rhinitis, Sensation Disorders, Fatigue Syndrome, Chronic diagnosis, Leukemia Virus, Murine immunology, Retroviridae Infections diagnosis

Abstract

New information about the pathophysiology of idiopathic nonallergic rhinopathy indicates a high prevalence in chronic fatigue syndrome (CFS). This article shows the relevance of CFS and allied disorders to allergy practice. CFS has significant overlap with systemic hyperalgesia (fibromyalgia), autonomic dysfunction (irritable bowel syndrome and migraine headaches), sensory hypersensitivity (dyspnea; congestion; rhinorrhea; and appreciation of visceral nociception in the esophagus, gastrointestinal tract, bladder, and other organs), and central nervous system maladaptations (central sensitization) recorded by functional magnetic resonance imaging (fMRI). Neurological dysfunction may account for the overlap of CFS with idiopathic nonallergic rhinopathy. Scientific advances are in fMRI, nociceptive sensor expression, and, potentially, infection with xenotropic murine leukemia-related virus provide additional insights to novel pathophysiological mechanisms of the "functional" complaints of these patients that are mistakenly interpreted as allergic syndromes. As allergists, we must accept the clinical challenges posed by these complex patients and provide proper diagnoses, assurance, and optimum care even though current treatment algorithms are lacking.

Published

2010

10. Microglial response to murine leukemia virus-induced encephalopathy is a good indicator of neuronal perturbations.

Author

Xue QS, Yang C, Hoffman PM, and Streit WJ

Subjects

Animals, Animals, Newborn, Brain physiopathology, Disease Progression, Ferritins metabolism, Neurites physiology, Neurons physiology, Rats, Rats, Inbred F344, Spinal Cord physiopathology, Time Factors, Central Nervous System Infections physiopathology, Leukemia Virus, Murine, Microglia physiology, Nerve Degeneration physiopathology, Retroviridae Infections physiopathology, Tumor Virus Infections physiopathology

Abstract

The neuronal pathology caused by neonatal infection of rats with the PVC-211 murine leukemia virus (PVC-211 MuLV) and its underlying mechanisms are not well defined even though a loss of neurons and spongiform neurodegeneration has been reported to accompany the disease. Here we sought to identify sites of neurodegeneration using microglial reactivity as an indirect marker and to characterize microglial activation during disease progression. Using a panel of microglial antibodies including Iba1, OX-42, ED1, and anti-ferritin, we have studied the response of microglial cells to neonatal CNS infection with PVC-211 at post-infection survival times 7, 14, 21, and 28 days. We found that microglial activation occurred primarily in the spinal cord and brainstem where it gradually increased in intensity over the time course of this study. Other brain areas were relatively unremarkable in their microglial reaction to viral infection within this time frame. However, the presence of activated microglial cells was not correlated directly with the presence of viral glycoprotein (gp70), which was expressed in endothelial cells throughout the CNS. Although double-labeling of microglia with Iba1 and ED1 revealed numerous actively phagocytic microglia during disease progression, not all activated microglia were ED1-positive. In addition to the intense microglial activation, we found increased ferritin expression sporadically throughout the virus-infected brain. The ferritin-positive cells were mostly microglia that exhibited dystrophic changes and likely represented a degenerating subpopulation of microglial cells. Thus, activated microglia can co-exist with degenerating microglia in the same brain region. We attempted to localize degenerating neurons or neurites using Fluoro-Jade, anti-tau, and anti-alpha synuclein staining, but none of these procedures yielded results to indicate obvious neuronal pathology. We conclude that the visualization of microglial activation is a more sensitive measure of neuronal perturbations than direct detection of neuronal pathology which may be subtle and not produce overt degenerative changes., (Copyright 2009 Elsevier B.V. All rights reserved.)

Published

2010

11. Tumour virology--history, status and future challenges.

Author

Kalland KH, Ke XS, and Øyan AM

Subjects

Animals, Avian Leukosis virology, Biological Evolution, Cell Transformation, Neoplastic, Chickens, DNA Tumor Viruses genetics, DNA Tumor Viruses pathogenicity, DNA Tumor Viruses physiology, Epigenesis, Genetic, Gene Expression Regulation, Neoplastic, Gene Expression Regulation, Viral, Genes, Viral, Humans, Mammals virology, Mice, Neoplasms etiology, Neoplasms virology, Oncogenes, Oncogenic Viruses genetics, Oncogenic Viruses pathogenicity, RNA Interference, Research, Retroviridae genetics, Retroviridae physiology, Retroviridae Infections physiopathology, Retroviridae Infections virology, Tumor Virus Infections physiopathology, Host-Pathogen Interactions physiology, Oncogenic Viruses physiology, Tumor Virus Infections virology

Abstract

Viruses enter host cells in order to complete their life cycles and have evolved to exploit host cell structures, regulatory factors and mechanisms. The virus and host cell interactions have consequences at multiple levels, spanning from evolution through disease to models and tools for scientific discovery and treatment. Virus-induced human cancers arise after a long duration of time and are monoclonal or oligoclonal in origin. Cancer is therefore a side effect rather than an essential part of viral infections in humans. Still, 15-20% of all human cancers are caused by viruses. A review of tumour virology shows its close integration in cancer research. Viral tools and experimental models have been indispensible for the progress of molecular biology. In particular, retroviruses and DNA tumour viruses have played major roles in our present understanding of the molecular biology of both viruses and the host. Recently, additional complex relationships due to virus and host co-evolution have appeared and may lead to a further understanding of the overall regulation of gene expression programmes in cancer.

Published

2009

12. Basic science summary.

Author

Stevenson M

Subjects

APOBEC-3G Deaminase, Animals, Cytidine Deaminase, Gene Products, nef, HIV Infections immunology, Humans, Lentivirus pathogenicity, Primates, Retroviridae Infections immunology, Reverse Transcription, Virus Replication genetics, HIV Infections physiopathology, Retroviridae Infections physiopathology, Virus Replication physiology

Abstract

The 16th Conference on Retroviruses and Opportunistic Infections featured a strong and balanced program that showcased exciting research into cellular restrictions that defend the cell against viral infection as well as cellular cofactors that regulate central steps in viral replication. Immunopathogenesis presentations continued to reveal some surprises such as evidence for pathogenicity in natural simian immunodeficiency virus infection. The identification of novel cellular restrictions and cellular cofactors of viral replication indicate the possibility of numerous opportunities for the development of novel therapeutic agents for the treatment of HIV and AIDS.

Published

2009

13. Retrovirus-specificity of regulatory T cells is neither present nor required in preventing retrovirus-induced bone marrow immune pathology.

Author

Antunes I, Tolaini M, Kissenpfennig A, Iwashiro M, Kuribayashi K, Malissen B, Hasenkrug K, and Kassiotis G

Subjects

Adoptive Transfer, Anemia metabolism, Anemia virology, Animals, Bone Marrow pathology, CD4-Positive T-Lymphocytes metabolism, Chronic Disease, Friend murine leukemia virus pathogenicity, Gene Knockdown Techniques, Interferon-gamma biosynthesis, Interferon-gamma immunology, Mice, Mice, Inbred C57BL, Mice, Transgenic, Receptors, Antigen, T-Cell metabolism, Retroviridae Infections pathology, Retroviridae Infections physiopathology, Retroviridae Infections virology, T-Lymphocytes, Helper-Inducer metabolism, T-Lymphocytes, Regulatory metabolism, Anemia immunology, Bone Marrow immunology, Bone Marrow physiopathology, CD4-Positive T-Lymphocytes immunology, Friend murine leukemia virus immunology, Receptors, Antigen, T-Cell immunology, Retroviridae Infections immunology, T-Lymphocytes, Helper-Inducer immunology, T-Lymphocytes, Regulatory immunology

Abstract

Chronic viral infections of the hematopoietic system are associated with bone marrow dysfunction, to which both virus-mediated and immune-mediated effects may contribute. Using unresolving noncytopathic Friend virus (FV) infection in mice, we showed that unregulated CD4(+) T cell response to FV caused IFN-gamma-mediated bone marrow pathology and anemia. Importantly, bone marrow pathology was triggered by relative insufficiency in regulatory T (Treg) cells and was prevented by added Treg cells, which suppressed the local IFN-gamma production by FV-specific CD4(+) T cells. We further showed that the T cell receptor (TCR) repertoire of transgenic Treg cells expressing the beta chain of an FV-specific TCR was virtually devoid of FV-specific clones. Moreover, anemia induction by virus-specific CD4(+) T cells was efficiently suppressed by virus-nonspecific Treg cells. Thus, sufficient numbers of polyclonal Treg cells may provide substantial protection against bone marrow pathology in chronic viral infections.

Published

2008

14. Comparative requirements for the restriction of retrovirus infection by TRIM5alpha and TRIMCyp.

Author

Diaz-Griffero F, Kar A, Lee M, Stremlau M, Poeschla E, and Sodroski J

Subjects

Animals, Antiviral Restriction Factors, Aotidae, Capsid physiology, Carrier Proteins chemistry, Carrier Proteins genetics, Cats, Cell Line, HIV-1 genetics, HIV-1 physiology, Humans, Immunodeficiency Virus, Feline genetics, Immunodeficiency Virus, Feline physiology, Protein Structure, Tertiary, Proteins chemistry, Proteins genetics, Retroviridae Infections virology, Tripartite Motif Proteins, Ubiquitin-Protein Ligases, Carrier Proteins physiology, Proteins physiology, Retroviridae Infections physiopathology

Abstract

The restriction factors, TRIM5alpha in most primates and TRIMCyp in owl monkeys, block infection of various retroviruses soon after virus entry into the host cell. Rhesus monkey TRIM5alpha (TRIM5alpha rh) inhibits human immunodeficiency virus (HIV-1) and feline immunodeficiency virus (FIV) more potently than human TRIM5alpha (TRIM5alpha hu). TRIMCyp restricts infection of HIV-1, simian immunodeficiency virus of African green monkeys (SIV agm) and FIV. Early after infection, TRIMCyp, like TRIM5alpha rh and TRIM5alpha hu, decreased the amount of particulate viral capsid in the cytosol of infected cells. The requirements for the TRIMCyp and TRIM5alpha domains in restricting different retroviruses were investigated. Potent restriction of FIV by TRIMCyp occurred in the complete absence of RING and B-box 2 domains; by contrast, efficient FIV restriction by TRIM5alpha rh required these domains. Variable region 1 of the TRIM5alpha rh B30.2 domain contributed to the potency of HIV-1, FIV and equine infectious anemia virus restriction. Thus, although differences exist in the requirements of TRIMCyp and TRIM5alpha for RING/B-box 2 domains, both restriction factors exhibit mechanistic similarities.

Published

2007

15. Bridging fundamental RNA biology, retroviral replication, and oncogenesis: Karen Beemon wins the 2007 Retrovirology Prize.

Author

Boris-Lawrie K

Subjects

Biomedical Research, Humans, Medical Laboratory Personnel, Retroviridae pathogenicity, Retroviridae Infections physiopathology, Virology, Awards and Prizes, Retroviridae physiology, Virus Replication

Abstract

The 2007 M. Jeang Retrovirology Prize has been awarded to Dr. Karen L. Beemon.

Published

2007

16. Clinical and virological characterization of persistent human infection with simian foamy viruses.

Author

Boneva RS, Switzer WM, Spira TJ, Bhullar VB, Shanmugam V, Cong ME, Lam L, Heneine W, Folks TM, and Chapman LE

Subjects

Adult, Animals, Blood virology, DNA, Viral genetics, Family Health, Female, Humans, Interviews as Topic, Male, Middle Aged, Primates, Proviruses isolation & purification, Retroviridae Infections pathology, Saliva virology, Semen virology, Simian foamy virus isolation & purification, Urine virology, Retroviridae Infections physiopathology, Retroviridae Infections virology, Simian foamy virus genetics, Zoonoses virology

Abstract

Persons occupationally exposed to nonhuman primates (NHPs) can be persistently infected with simian foamy virus (SFV). The clinical significance and person-to-person transmissibility of zoonotic SFV infection is unclear. Seven SFV-infected men responded to annual structured interviews and provided whole blood, oral, and urogenital specimens for study. Wives were tested for SFV infection. Proviral DNA was consistently detected by PCR in PBMCs of infected men and inconsistently in oral or urogenital samples. SFV was infrequently cultured from their PBMCs and throat swabs. Despite this and a long period of intimate exposure (median 20 years), wives were SFV negative. Most participants reported nonspecific symptoms and diseases common to aging. However, one of two persons with mild thrombocytopenia had clinically asymptomatic nonprogressive, monoclonal natural killer cell lymphocytosis of unclear relationship to SFV. All participants worked with NHPs before 1988 using mucocutaneous protection inconsistently; 57% described percutaneous injuries involving the infecting NHP species. SFV likely transmits to humans through both percutaneous and mucocutaneous exposures to NHP body fluids. Limited follow-up has not identified SFV-associated illness and secondary transmission among humans.

Published

2007

17. Increased proinflammatory cytokine and chemokine responses and microglial infection following inoculation with neural stem cells infected with polytropic murine retroviruses.

Author

Peterson KE, Evans LH, Wehrly K, and Chesebro B

Subjects

Animals, Astrocytes immunology, Brain immunology, Brain virology, Central Nervous System Viral Diseases pathology, Central Nervous System Viral Diseases physiopathology, Central Nervous System Viral Diseases virology, Chemokines biosynthesis, Chemokines genetics, Cytokines genetics, Disease Models, Animal, Gene Expression, Immunohistochemistry, Mice, Microglia immunology, Neurons cytology, Neurons virology, RNA, Messenger analysis, Receptors, Virus metabolism, Retroviridae physiology, Retroviridae Infections physiopathology, Retroviridae Infections virology, Stem Cell Transplantation, Viral Proteins analysis, Central Nervous System Viral Diseases immunology, Cytokines biosynthesis, Microglia virology, Retroviridae immunology, Retroviridae Infections immunology, Stem Cells virology

Abstract

Proinflammatory cytokines and chemokines are often detected in brain tissue of patients with neurological diseases such as multiple sclerosis (MS), HIV-associated dementia (HAD) and Alzheimer's disease (AD). We have utilized a mouse model of retrovirus-induced neurological disease to examine how these proinflammatory responses contribute to neuropathogenesis. In previous studies with this model, a correlation was found between neurovirulence and cytokine and chemokine expression. However, it was unclear whether the induction of these cytokines and chemokines was in response to specific virus envelope determinants or was regulated by the level of virus infection in the brain. In the current study, we demonstrated that multiple polytropic retroviruses induced cytokine and chemokine mRNA expression following increased virus levels in the brain. Increased virus levels of polytropic viruses also correlated with increased neuropathogenesis. In contrast, the ecotropic retrovirus, FB29, did not induce cytokine or chemokine mRNA expression or neurological disease, despite virus levels either similar to or higher than the polytropic retroviruses. As polytropic and ecotropic viruses utilize different receptors for entry, these receptors may play a critical role in the induction of these innate immune responses in the brain.

Published

2006

18. [Retrovirus infection and neurological disorders].

Author

Izumo S, Kubota R, and Xing HQ

Subjects

Animals, Antiretroviral Therapy, Highly Active, HTLV-I Infections, Human T-lymphotropic virus 1, Humans, Retroviridae physiology, AIDS Dementia Complex pathology, AIDS Dementia Complex therapy, Nervous System Diseases pathology, Nervous System Diseases physiopathology, Paraparesis, Tropical Spastic pathology, Paraparesis, Tropical Spastic physiopathology, Paraparesis, Tropical Spastic virology, Retroviridae Infections pathology, Retroviridae Infections physiopathology

Published

2006

19. Inclusion body disease in snakes: a review and description of three cases in boa constrictors in Belgium.

Author

Vancraeynest D, Pasmans F, Martel A, Chiers K, Meulemans G, Mast J, Zwart P, and Ducatelle R

Subjects

Animals, Arachnid Vectors virology, Belgium, Diagnosis, Differential, Microscopy, Electron, Transmission veterinary, Mites virology, Myeloid Cells pathology, Prevalence, Prognosis, Retroviridae Infections diagnosis, Retroviridae Infections pathology, Retroviridae Infections physiopathology, Snakes virology, Boidae virology, Inclusion Bodies, Viral ultrastructure, Retroviridae Infections veterinary

Abstract

Inclusion body disease, a fatal disorder in Boidae, is reviewed, and three cases in boa constrictors, the first reported cases in Belgium, are described. The snakes showed nervous signs, and numerous eosinophilic intracytoplasmic inclusions, which are considered to be characteristic of the disease, were found in the liver and pancreas. The disease is suspected to be caused by a retrovirus, but transmission electron microscopic examinations of several tissues from one of the snakes did not reveal particles with a typical retroviral morphology.

Published

2006

20. Two surface-exposed elements of the B30.2/SPRY domain as potency determinants of N-tropic murine leukemia virus restriction by human TRIM5alpha.

Author

Perron MJ, Stremlau M, and Sodroski J

Subjects

Amino Acid Sequence, Antigens, Viral drug effects, Antiviral Restriction Factors, Capsid physiology, Carrier Proteins chemistry, Carrier Proteins pharmacology, Humans, Leukemia Virus, Murine chemistry, Leukemia Virus, Murine pathogenicity, Protein Structure, Tertiary, Proteins chemistry, Proteins pharmacology, Retroviridae Infections physiopathology, Tripartite Motif Proteins, Ubiquitin-Protein Ligases, Antigens, Viral immunology, Carrier Proteins genetics, Leukemia Virus, Murine drug effects, Retroviridae Infections prevention & control

Abstract

Human TRIM5alpha (TRIM5alpha(hu)) potently restricts N-tropic (N-MLV), but not B-tropic, murine leukemia virus in a manner dependent upon residue 110 of the viral capsid. Rhesus monkey TRIM5alpha (TRIM5alpha(rh)) inhibits N-MLV only weakly. The study of human-monkey TRIM5alpha chimerae revealed that both the v1 and v3 variable regions of the B30.2/SPRY domain contain potency determinants for N-MLV restriction. These variable regions are predicted to be surface-exposed elements on one face of the B30.2 domain. Acidic residues in v3 complement basic residue 110 of the N-MLV capsid. The results support recognition of the retroviral capsid by the TRIM5alpha B30.2 domain.

Published

2006

21. Astrocytes survive chronic infection and cytopathic effects of the ts1 mutant of the retrovirus Moloney murine leukemia virus by upregulation of antioxidant defenses.

Author

Qiang W, Kuang X, Liu J, Liu N, Scofield VL, Reid AJ, Jiang Y, Stoica G, Lynn WS, and Wong PK

Subjects

Animals, Cell Line, Transformed, Cell Survival, Cell Transformation, Viral, Cells, Cultured, Cytopathogenic Effect, Viral, Leukemia, Experimental physiopathology, Mice, Moloney murine leukemia virus genetics, Moloney murine leukemia virus growth & development, Moloney murine leukemia virus metabolism, Mutation, Retroviridae Infections physiopathology, Simian virus 40 genetics, Simian virus 40 physiology, Temperature, Tumor Virus Infections physiopathology, Antioxidants metabolism, Astrocytes metabolism, Astrocytes virology, Leukemia, Experimental metabolism, Moloney murine leukemia virus physiology, Retroviridae Infections metabolism, Tumor Virus Infections metabolism, Up-Regulation

Abstract

The ts1 mutant of Moloney murine leukemia virus (MoMuLV) induces a neurodegenerative disease in mice, in which glial cells are infected by the retrovirus but neurons are not. ts1 infection of primary astrocytes, or of the immortalized astrocytic cell line C1, results in accumulation of the ts1 gPr80(env) envelope protein in the endoplasmic reticulum (ER), with ER and oxidative stress. Notably, only about half of the infected astrocytes die in these cultures, while the other half survive, continue to proliferate, and continue to produce virus. To determine how these astrocytes survive ts1 infection in culture, we established a chronically infected subline of the living cells remaining after the death of all acutely infected cells in an infected C1 cell culture (C1-ts1-S). We report here that C1-ts1-S cells proliferate more slowly, produce less virus, show reduced H2O2 levels, increase their uptake of cystine, and maintain higher levels of intracellular GSH and cysteine compared to acutely infected or uninfected C1 cells. C1-ts1-S cells also upregulate their thiol antioxidant defenses by activation of the transcription factor NF-E2-related factor 2 (Nrf2) and its target genes. Interestingly, despite maintenance of higher levels of intracellular reduced thiols, C1-ts1-S cells are more sensitive to cystine deprivation than uninfected C1 cells. We conclude that some ts1-infected astrocytes survive and adapt to virus-induced oxidative stress by successfully mobilizing their thiol redox defenses.

Published

2006

22. Impairment of blood-cerebrospinal fluid barrier properties by retrovirus-activated T lymphocytes: reduction in cerebrospinal fluid-to-blood efflux of prostaglandin E2.

Author

Khuth ST, Strazielle N, Giraudon P, Belin MF, and Ghersi-Egea JF

Subjects

Animals, Animals, Newborn, Blood-Brain Barrier virology, Cell Communication immunology, Cells, Cultured, Central Nervous System Viral Diseases immunology, Central Nervous System Viral Diseases metabolism, Central Nervous System Viral Diseases physiopathology, Cerebrospinal Fluid immunology, Cerebrospinal Fluid metabolism, Choroid Plexus virology, Coculture Techniques, Encephalitis immunology, Encephalitis metabolism, Encephalitis physiopathology, Epithelial Cells metabolism, Epithelial Cells virology, Free Radicals immunology, Free Radicals metabolism, Gene Products, tax immunology, Gene Products, tax metabolism, Inflammation Mediators immunology, Inflammation Mediators metabolism, Lymphocyte Activation immunology, Matrix Metalloproteinases immunology, Matrix Metalloproteinases metabolism, Rats, Retroviridae immunology, Retroviridae Infections metabolism, Retroviridae Infections physiopathology, T-Lymphocytes virology, Virus Shedding immunology, Blood-Brain Barrier immunology, Choroid Plexus immunology, Dinoprostone metabolism, Epithelial Cells immunology, Retroviridae Infections immunology, T-Lymphocytes immunology

Abstract

The choroid plexus epithelium forms the interface between the blood and the CSF. In conjunction with the tight junctions restricting the paracellular pathway, polarized specific transport systems in the choroidal epithelium allow a fine regulation of CSF-borne biologically active mediators. The highly vascularized stroma delimited by the choroidal epithelium can be a reservoir for retrovirus-infected or activated immune cells. In this work, new insight in the implication of the blood-CSF barrier in neuroinfectious and inflammatory diseases is provided by using a differentiated cellular model of the choroidal epithelium, exposed to infected T lymphocytes. We demonstrate that T cells activated by a retroviral infection, but not non-infected cells, reduce the transporter-mediated CSF-to-blood efflux of organic anions, in particular that of the potent pro-inflammatory prostaglandin PGE2, via the release of soluble factors. A moderate alteration of the paracellular permeability also occurs. We identified the viral protein Tax, oxygenated free radicals, matrix-metalloproteinases and pro-inflammatory cytokines as active molecules released during the exposure of the epithelium to infected T cells. Among them, tumour necrosis factor and interleukin 1 are directly involved in the mechanism underlying the decrease in some choroidal organic anion efflux. Given the strong involvement of CSF-borne PGE2 in sickness behaviour syndrome, these data suggest that the blood-CSF barrier plays an important role in the pathophysiology of neuroinflammation and neuroinfection, via changes in the transport processes controlling the CSF biodisposition of PGE2.

Published

2005

23. A role for T lymphocytes in mediating cardiac diastolic function.

Author

Yu Q, Watson RR, Marchalonis JJ, and Larson DF

Subjects

Animals, Coculture Techniques, Extracellular Matrix metabolism, Female, Fibroblasts physiology, Genetic Variation, Immune System physiopathology, Leukemia Virus, Murine genetics, Matrix Metalloproteinases genetics, Mice, Mice, Inbred C57BL, Myocardium metabolism, Peptide Fragments pharmacology, Procollagen genetics, Protein Precursors genetics, RNA, Messenger metabolism, Receptors, Antigen, T-Cell, alpha-beta chemistry, Retroviridae Infections immunology, Retroviridae Infections physiopathology, Diastole, Heart physiology, Myocardium immunology, Th1 Cells physiology, Th2 Cells physiology

Abstract

The induction of T helper (TH) lymphocytes by distinct TH ligands results in a differentiation to TH1/TH2 subsets based on their unique pattern of cytokine secretion and effector functions. We hypothesized that the relative proportion of TH1/TH2 directly relates to cardiac fibroblast (CF) function and thereby cardiac extracellular matrix (ECM) composition and cardiac diastolic function in the absence of injury or altered wall stress. We compared the effect of selective TH1 with TH2 inducers on cardiac gene expression, ECM composition, and diastolic function in C57BL/J mice. Twelve weeks after immune modulation, the left ventricular stiffness (beta) was significantly increased in the TH1 group and decreased in the TH2 group (P < 0.01). The TH2 group also demonstrated significantly increased end-diastolic and end-systolic volumes (P < 0.01). Cardiac gene expression patterns for pro-matrix metalloproteinase (MMP)-9 and -13 were increased by greater than fivefold in the TH2 group and significantly decreased in the TH1 group (P < 0.05). The total cardiac collagen and cross-linked collagen were significantly increased in the TH1 group and decreased in the TH2 group (P < 0.01). Coculturing lymphocytes harvested from the treated mice with naive primary CF demonstrated a direct control of the lymphocytes on CF pro-collagen, pro-MMP gene expression, and MMP activity. These results suggest that the TH phenotype differentially affects diastolic function through modulating CF pro-collagen and pro-MMP gene expression, MMP activity, and cardiac collagen cross-linking, resulting in altered ECM composition. Thus modulation of TH lymphocyte function could promote adaptive remodeling in heart failure and postmyocardial infarction.

Published

2005

24. Transfection techniques affecting Stat3 activity levels.

Author

Arulanandam R, Vultur A, and Raptis L

Subjects

Animals, Calcium Phosphates, Electroporation, Leukemia Virus, Murine genetics, Leukemia, Experimental physiopathology, Lipids, Liposomes, Mice, NIH 3T3 Cells, Phosphorylation, Retroviridae Infections physiopathology, STAT3 Transcription Factor, Signal Transduction physiology, Tumor Virus Infections physiopathology, DNA-Binding Proteins physiology, Trans-Activators physiology, Transfection methods

Abstract

Transfection techniques, such as calcium-phosphate or liposome-mediated gene transfer, are commonly used for the examination of the effect of a gene upon cellular phenotype and biochemical properties. We previously demonstrated that cell to cell adhesion causes a dramatic increase in Stat3 activity. Given that the opportunities for cell to cell adhesion could be altered due to the presence of the DNA-containing complexes, we examined the effect of the calcium-phosphate transfection procedure upon Stat3 activity levels. The results revealed a dramatic increase in Stat3 phosphorylation at the critical tyr705 site and Stat3 activity following calcium-phosphate transfection. This increase was noted even in the absence of DNA and was not due to the mere presence of calcium ions. In contrast, DNA introduction through electroporation or infection with a retroviral vector did not affect Stat3 activity, while cationic lipids such as lipofectamine or Fugene6 had a less pronounced effect than calcium-phosphate transfection. These results indicate that caution is required in the interpretation of results with regard to activity of Stat3 following certain commonly used transient transfection regimens.

Published

2005

25. Subtle mutational changes in the SU protein of a natural feline leukemia virus subgroup A isolate alter disease spectrum.

Author

Chandhasin C, Coan PN, and Levy LS

Subjects

Animals, Cat Diseases physiopathology, Cat Diseases virology, Cats, Cell Line, Dogs, Female, Glycoproteins metabolism, Humans, Leukemia Virus, Feline genetics, Lymphoma physiopathology, Lymphoma virology, Lymphoma, T-Cell physiopathology, Lymphoma, T-Cell virology, Molecular Sequence Data, Retroviridae Infections virology, Sequence Analysis, DNA, Thymus Gland virology, Thymus Neoplasms physiopathology, Thymus Neoplasms virology, Tumor Virus Infections virology, Viral Envelope Proteins metabolism, Glycoproteins genetics, Leukemia Virus, Feline pathogenicity, Mutation, Retroviridae Infections physiopathology, Tumor Virus Infections physiopathology, Viral Envelope Proteins genetics

Abstract

FeLV-945 is a representative isolate of the natural feline leukemia virus (FeLV) variant predominant in non-T-cell malignant, proliferative, and degenerative diseases in a geographic cohort. The FeLV-945 surface glycoprotein (SU) is closely related to natural horizontally transmissible FeLV subgroup A (FeLV-A) but was found to differ from a prototype to a larger extent than the members of FeLV-A differ among themselves. The sequence differences included point mutations restricted largely to the functional domains of SU, i.e., VRA, VRB, and PRR. Despite the sequence differences in these critical domains, measurements of receptor utilization, including host range and superinfection interference, confirmed the assignment of FeLV-945 to subgroup A. Other proviruses isolated from the cohort contained similar sequence hallmarks and were assigned to FeLV subgroup A. A provirus from cat 1046 contained a histidine-to-proline change at SU residue 6 within an SPHQ motif that was previously identified as a critical mediator of fusion events during virus entry. The 1046 pseudotype virus entered cells only in the presence of the soluble cofactor FeLIX provided in trans, but it retained an ecotropic host range even in the presence of FeLIX. The mutational changes in FeLV-945 were shown to confer significant functional differences compared to prototype FeLV-A viruses. The substitution of FeLV-945 envelope gene sequences for FeLV-A/61E sequences conferred a small but statistically significant replicative advantage in some feline cells. Moreover, substitution of the unique FeLV-945 long terminal repeat and envelope gene for those of FeLV-A/61E altered the disease spectrum entirely, from a thymic lymphoma of a T-cell origin to an as yet uncharacterized multicentric lymphoma that did not contain T cells.

Published

2005

26. [Envelope capture by retroviruses].

Author

Kim FJ, Manel N, Battini JL, and Sitbon M

Subjects

Animals, Genome, Viral, Humans, Retroelements genetics, Genes, env, Retroviridae genetics, Retroviridae Infections physiopathology, Viral Envelope Proteins genetics

Abstract

Retroelement transposition is a major source of diversity in genome evolution. Among the retrotransposable elements, the retroviruses are distinct in that their "transposition" extends from their initial host cells to neighboring cells and organisms. A determining step in the conversion of a retrotransposable element into an infectious retrovirus is the acquisition of an envelope glycoprotein, designated Env. Here, we review some examples of envelope "capture" by mammal retroviruses and provide evidence for such a mechanism by HTLV. This phenomenon may explain the notable conservation of env genes observed between phylogenetically distant retroviruses. Elucidation of these recombination processes should help to clarify retroviral phylogeny, better understand retroviral pathogenesis, and may lead to the identification of new retroelements.

Published

2004

27. Foamy viruses--a world apart.

Author

Delelis O, Lehmann-Che J, and Saïb A

Subjects

Animals, Retroviridae Infections physiopathology, Virus Replication, Retroviridae Infections virology, Spumavirus classification, Spumavirus genetics, Spumavirus pathogenicity

Abstract

Foamy viruses (FVs) or spumaviruses were described for the first time in the early 1950s in cell cultures derived from monkey kidneys. Later, FVs were isolated in several mammal species such as cats, cattle and horses. Highly prevalent in non-human primates they are not naturally present in humans, although several cases of simian-to-human transmissions have been described. Interestingly, the replication strategy of FVs differs in many aspects from that of other retroviruses, presenting features that are closely related to pararetroviruses, exemplified by the hepatitis B virus (HBV), but also characteristics that are closely related to yeast retrotransposons. These characteristics led to the creation of a distinct viral subfamily by the International Committee on Virus Taxonomy in 2002; the Spumaretrovirinae.

Published

2004

28. Possible involvement of both endoplasmic reticulum- and mitochondria-dependent pathways in MoMuLV-ts1-induced apoptosis in astrocytes.

Author

Liu N, Kuang X, Kim HT, Stoica G, Qiang W, Scofield VL, and Wong PK

Subjects

Animals, Blotting, Western, Brain Stem pathology, Brain Stem ultrastructure, Brain Stem virology, Cells, Cultured, Cytopathogenic Effect, Viral physiology, Endoplasmic Reticulum pathology, Endoplasmic Reticulum ultrastructure, Endoplasmic Reticulum Chaperone BiP, Flow Cytometry, Immunohistochemistry, Mice, Microscopy, Electron, Mitochondria pathology, Mitochondria ultrastructure, Moloney murine leukemia virus physiology, Retroviridae Infections pathology, Tumor Virus Infections pathology, Apoptosis physiology, Astrocytes virology, Endoplasmic Reticulum virology, Mitochondria virology, Retroviridae Infections physiopathology, Tumor Virus Infections physiopathology

Abstract

The Moloney murine leukemia virus (MoMuLV)-ts1 retrovirus, a naturally occurring mutant of MoMuLV-TB, causes a neuroimmunodegenerative syndrome in mice. The authors show here that ts1 triggers apoptosis in immortalized astrocytes, C1 cells, and primary cultured astrocytes, and that this apoptosis is caused by endoplasmic reticulum (ER) stress resulting from accumulation of the viral envelope preprotein gPr80(env). In ts1-infected C1 cells, an unfolded protein response was identified by activation of the ER-resident transmembrane protein kinase PERK, an event that leads to hyperphosphorylation of eIF2 alpha, up-regulation of GRP78, increased amounts of GADD153/CHOP, and cleavage of procaspase-12. Up-regulation of GRP78 and cleavage of procaspase-12 were also detected in primary cultured astrocytes infected with ts1. In ts1-infected C1 cells, ER stress was followed by mitochondrial stress, detected as mitochondrial transmembrane potential dissipation, cleavage of procaspase-9, and induction of activated caspase-3. In the brainstems of ts1-infected mice, activated caspase-3 and damaged mitochondria were identified in astrocytes within areas showing spongiform degeneration. Together the data imply that both ER stress- and mitochondrial stress-related apoptotic pathways are involved in ts1-induced astrocyte death.

Published

2004

29. MCP-1 and CCR2 contribute to non-lymphocyte-mediated brain disease induced by Fr98 polytropic retrovirus infection in mice: role for astrocytes in retroviral neuropathogenesis.

Author

Peterson KE, Errett JS, Wei T, Dimcheff DE, Ransohoff R, Kuziel WA, Evans L, and Chesebro B

Subjects

Animals, Astrocytes metabolism, Brain metabolism, Brain virology, Brain Diseases virology, Chemokine CCL7, Gene Deletion, Glial Fibrillary Acidic Protein metabolism, Mice, Mice, Inbred BALB C, Monocyte Chemoattractant Proteins metabolism, Receptors, CCR2, Receptors, Chemokine genetics, Retroviridae Infections virology, Up-Regulation, Virulence, Virus Replication, Brain Diseases physiopathology, Chemokine CCL2 metabolism, Cytokines, Lymphocytes immunology, Receptors, Chemokine metabolism, Retroviridae pathogenicity, Retroviridae Infections physiopathology

Abstract

Virus infection of the central nervous system (CNS) often results in chemokine upregulation. Although often associated with lymphocyte recruitment, increased chemokine expression is also associated with non-lymphocyte-mediated CNS disease. In these instances, the effect of chemokine upregulation on neurological disease is unclear. In vitro, several chemokines including monocyte chemotactic protein 1 (MCP-1) protect neurons from apoptosis. Therefore, in vivo, chemokine upregulation may be a protective host response to CNS damage. Alternatively, chemokines may contribute to pathogenesis by stimulating intrinsic brain cells or recruiting macrophages to the brain. To investigate these possibilities, we studied a neurovirulent retrovirus, Fr98, that induces severe non-lymphocyte-mediated neurological disease and causes the upregulation of several chemokines that bind to chemokine receptors CCR2 and CCR5. Knockout mice deficient in CCR2 had reduced susceptibility to Fr98 pathogenesis, with significantly fewer mice developing clinical disease than did wild-type controls. In contrast, no reduction in Fr98-induced disease was observed in CCR5 knockout mice. Thus, signaling through CCR2, but not CCR5, plays an important role in Fr98-mediated pathogenesis. Three ligands for CCR2 (MCP-1, MCP-3, and MCP-5) were upregulated during Fr98 infection of the brain. Antibody-blocking experiments demonstrated that MCP-1 was important for retrovirus-induced neurological disease. In situ hybridization analysis revealed that MCP-1 was expressed by glial fibrillary acidic protein-positive astrocytes. Thus, astrocytes, previously not thought to play an effector role in the disease process were found to contribute to pathogenesis through the production of MCP-1. This study also demonstrates that chemokines can mediate pathogenesis in the CNS in the absence of lymphocytic infiltrate and gives credence to the hypothesis that chemokine upregulation is a mechanism by which retroviruses such as human immunodeficiency virus induce neurological damage.

Published

2004

30. Ex vivo and in vivo biological effects of a truncated form of the receptor tyrosine kinase stk when activated by interaction with the friend spleen focus-forming virus envelope glycoprotein or by point mutation.

Author

Rulli K, Yugawa T, Hanson C, Thompson D, Ruscetti S, and Nishigaki K

Subjects

Animals, Cell Line, Erythroid Cells cytology, Erythropoietin metabolism, Genetic Vectors, Leukemia, Erythroblastic, Acute physiopathology, Leukemia, Erythroblastic, Acute virology, Mice, Mice, Inbred C57BL, Receptor Protein-Tyrosine Kinases genetics, Retroviridae Infections physiopathology, Retroviridae Infections virology, Spleen Focus-Forming Viruses metabolism, Tumor Virus Infections physiopathology, Tumor Virus Infections virology, Erythroid Cells metabolism, Point Mutation, Receptor Protein-Tyrosine Kinases metabolism, Spleen Focus-Forming Viruses pathogenicity, Viral Envelope Proteins metabolism

Abstract

The erythroleukemia-inducing Friend spleen focus-forming virus (SFFV) encodes a unique envelope protein, gp55, which interacts with the erythropoietin (Epo) receptor complex, causing proliferation and differentiation of erythroid cells in the absence of Epo. Susceptibility to SFFV-induced erythroleukemia is conferred by the Fv-2 gene, which encodes a short form of the receptor tyrosine kinase Stk/Ron (sf-Stk) only in susceptible strains of mice. We recently demonstrated that sf-Stk becomes activated by forming a strong interaction with SFFV gp55. To examine the biological consequences of activated sf-Stk on erythroid cell growth, we prepared retroviral vectors which express sf-Stk, either in conjunction with gp55 or alone in a constitutively activated mutant form, and tested them for their ability to induce Epo-independent erythroid colonies ex vivo and disease in mice. Our data indicate that both gp55-activated sf-Stk and the constitutively activated mutant of sf-Stk induce erythroid cells from Fv-2-susceptible and Fv-2-resistant (sf-Stk null) mice to form Epo-independent colonies. Mutational analysis of sf-Stk indicated that a functional kinase domain and 8 of its 12 tyrosine residues are required for the induction of Epo-independent colonies. Further studies demonstrated that coexpression of SFFV gp55 with sf-Stk significantly extends the half-life of the kinase. When injected into Fv-2-resistant mice, neither the gp55-activated sf-Stk nor the constitutively activated mutant caused erythroleukemia. Surprisingly, both Fv-2-susceptible and -resistant mice injected with the gp55-sf-Stk vector developed clinical signs not previously associated with SFFV-induced disease. We conclude that sf-Stk, activated by either point mutation or interaction with SFFV gp55, is sufficient to induce Epo-independent erythroid colonies from both Fv-2-susceptible and -resistant mice but is unable to cause erythroleukemia in Fv-2-resistant mice.

Published

2004

31. Vertical transmission of a murine retrovirus, ts1.

Author

Duggan J, Okonta H, and Chakraborty J

Subjects

Animals, Disease Models, Animal, Female, Male, Mice, Mice, Inbred BALB C, Moloney murine leukemia virus genetics, Pregnancy, Retroviridae Infections physiopathology, Retroviridae Infections virology, Spleen virology, Infectious Disease Transmission, Vertical, Moloney murine leukemia virus isolation & purification, Retroviridae Infections transmission

Abstract

Mechanism of maternal retroviral transmission remains an unsolved problem. The current investigation is a part of our ongoing research on vertical transmission of MoMuLV-TB ts1 in BALB/c mice. A total of 270 adult mice and 165 fetuses were used. Forty-four experimental mice were injected with 0.1 mL of 4.0 x 10(6) ffu/mL of ts1 virus at 72 h after birth; 24 controls were injected with DMEM. Almost half of the females went through two rounds of pregnancies. In the first round, 135 experimental and 57 control pups were produced. Forty-three experimental and 20 control pups were followed until they developed clinical symptoms. The second round of pregnancy produced a total of 46 mid-gestational and 119 full-term fetuses. PCR, and light and electron microscopy were performed to evaluate viral transmission. Overall, 99% vertical transmission occurred in pups of infected mothers. Twelve percent of mid-gestational and 39% full-term fetuses were PCR positive. We have established that, if mothers are infected with ts1 virus at 72 h after birth, then nearly 100% vertical transmission occurs, via in utero, intrapartum, or breast milk. Thirty-nine percent transmission occurred in utero alone. This is an excellent model to study the transplacental and post-gestational transmission of retroviruses, such as ts1., (Copyright Mary Ann Liebert, Inc.)

Published

2004

32. Limited infection without evidence of replication by porcine endogenous retrovirus in guinea pigs.

Author

Argaw T, Colon-Moran W, and Wilson CA

Subjects

Animals, Antibodies, Viral blood, DNA, Viral analysis, Endogenous Retroviruses drug effects, Endogenous Retroviruses immunology, Endogenous Retroviruses physiology, Hepatocytes drug effects, Polymerase Chain Reaction, Propanols pharmacology, Retroviridae Infections physiopathology, Endogenous Retroviruses pathogenicity, Guinea Pigs virology, Retroviridae Infections virology, Swine, Miniature virology, Virus Replication

Abstract

Porcine endogenous retrovirus (PERV) may potentially be transmitted through porcine xenotransplantation products administered to humans. This study examined the feasibility of using guinea pigs as a model to characterize the in vivo infectivity of PERV. To enhance the susceptibility of guinea pigs to retroviral infection or genomic integration, moderate physiological or immunological changes were induced prior to exposing the animals to PERV. Quantitative PERV-specific PCR performed on all tested samples resulted in either undetectable or very low copy numbers of proviruses, even in animals possessing PERV-specific antibody responses. The low copy number of viral DNA detected suggests that PERV infected a limited number of cells. However, PERV DNA levels did not increase over time, suggesting no virus replication occurred. These results in the guinea pig are similar to previous observations of non-human primate cells that allow PERV infection but do not support PERV replication in vitro.

Published

2004

33. Comparative pathogenesis of epsilonretroviruses.

Author

Holzschu D, Lapierre LA, and Lairmore MD

Subjects

Animals, Cell Division physiology, Cyclins physiology, Epsilonretrovirus genetics, Epsilonretrovirus metabolism, Fish Diseases physiopathology, Gene Expression Regulation, Viral, Retroviridae Infections physiopathology, Epsilonretrovirus physiology

Published

2003

34. Expression of inducible nitric oxide synthase and elevation of tyrosine nitration of a 32-kilodalton cellular protein in brain capillary endothelial cells from rats infected with a neuropathogenic murine leukemia virus.

Author

Jinno-Oue A, Wilt SG, Hanson C, Dugger NV, Hoffman PM, Masuda M, and Ruscetti SK

Subjects

3T3 Cells, Animals, Brain enzymology, Brain metabolism, Brain virology, Capillaries virology, Cells, Cultured, Endothelium, Vascular cytology, Endothelium, Vascular enzymology, Endothelium, Vascular metabolism, Mice, Nervous System pathology, Nervous System virology, Nitric Oxide Synthase Type II, Rats, Rats, Inbred F344, Retroviridae Infections physiopathology, Retroviridae Infections virology, Tumor Virus Infections physiopathology, Tumor Virus Infections virology, Brain blood supply, Endothelium, Vascular virology, Leukemia Virus, Murine pathogenicity, Nitric Oxide Synthase biosynthesis, Proteins metabolism, Tyrosine analogs & derivatives, Tyrosine metabolism

Abstract

PVC-211 murine leukemia virus (MuLV) is a neuropathogenic variant of Friend MuLV (F-MuLV) which causes a rapidly progressive spongiform neurodegenerative disease in rodents. The primary target of PVC-211 MuLV infection in the brain is the brain capillary endothelial cell (BCEC), which is resistant to F-MuLV infection. Previous studies have shown that changes in the envelope gene of PVC-211 MuLV confer BCEC tropism to the virus. However, little is known about how infection of BCECs by PVC-211 MuLV induces neurological disease. Previous results suggest that nitric oxide (NO), which has been implicated as a potential neurotoxin, is involved in PVC-211 MuLV-induced neurodegeneration. In this study, we show that expression of inducible nitric oxide synthase (iNOS), which produces NO from L-arginine, is induced in BCECs from PVC-211 MuLV-infected rats. Furthermore, elevated levels of a 32-kDa cellular protein modified by 3-nitrotyrosine, which is a hallmark of NO production, were observed in virus-infected BCECs. BCECs from rats infected with BCEC-tropic but nonneuropathogenic PVF-e5 MuLV, which is a chimeric virus between PVC-211 MuLV and F-MuLV, fail to induce either iNOS expression or elevation of tyrosine nitration of a 32-kDa protein. These results suggest that expression of iNOS and nitration of tyrosine residues of a 32-kDa protein in PVC-211 MuLV-infected BCECs may play an important role in neurological disease induction.

Published

2003

35. Simian retrovirus infections: potential confounding variables in primate toxicology studies.

Author

Lerche NW and Osborn KG

Subjects

Animals, Confounding Factors, Epidemiologic, Models, Animal, Retroviridae Infections pathology, Retroviridae Infections virology, Retroviruses, Simian isolation & purification, Toxicology, Tumor Virus Infections pathology, Tumor Virus Infections virology, Primates microbiology, Retroviridae Infections epidemiology, Retroviridae Infections physiopathology, Tumor Virus Infections epidemiology, Tumor Virus Infections physiopathology

Abstract

Various species of nonhuman primates are natural hosts for 6 exogenous retroviruses, including gibbon-ape leukemia virus (GaLV), simian sarcoma virus, simian T-lymphotropic virus (STLV), simian immunodeficiency virus (SIV), simian type D retrovirus (SRV), and simian foamy virus (SFV). These viruses establish persistent infections with a broad spectrum of pathogenic potential, ranging from highly pathogenic to nonpathogenic, depending on various host, virus, and environmental factors. Latent or subclinical infections are common, and various procedures associated with experimental protocols may lead to virus reactivation and disease. Adverse effects on toxicologic research by undetected retroviral infections can occur in several ways, including loss of experimental subjects (and statistical power) due to increased morbidity and mortality. In addition, results may be confounded by virus-induced clinical abnormalities, histologic lesions, alteration of physiologic parameters and responses, and interference with in vitro assays and/or destruction of primary cell cultures. Key clinical and epidemiological features of several important retroviruses are reviewed, with emphasis on viruses infecting species of macaques most commonly used as research subjects in primate toxicology studies. Examples of actual and potential confounding of toxicologic studies by retroviruses are discussed, including altered cytokine profiles in healthy STLV carriers, and clinical and pathological abnormalities induced by SRV infection. Adequate prestudy viral screening is critical to exclude retrovirus-infected primates from toxicologic research protocols and prevent potential confounding of research results.

Published

2003

36. [Retrovirus, mycotoxins, immunosuppression and neurodegeneration].

Author

León-Sarmiento FE and Carpintero de Jimeno M

Subjects

HIV Infections physiopathology, Humans, Leukemia, T-Cell virology, Mycosis Fungoides virology, Neurodegenerative Diseases virology, Paraparesis, Tropical Spastic virology, Sjogren's Syndrome virology, Retroviridae Infections physiopathology

Abstract

Aims: To analyse the pros and cons of the etiopathogenic aspects of the different clinical entities that, over the years, have been found to be associated with the so called human retroviruses in order to propose possible etiological alternatives., Method: Since research on retroviruses began there has been a tendency to blame these elements for a number of clinical entities, the most important of which include Aids, tropical spastic paraparesis (TSP), fungoid mycosis, Sjogren's syndrome and T cell leukaemia. Yet many patients and scientific publications point out the existence of a large number of clinical and laboratory inconsistencies, which suggests that the so called cofactors associated with all these entities are far more likely to be the real generators of these public health problems. Among these, we pay special attention to environmental toxins, of which a prototypical example is the group of neuromycotoxins. There are several ways these can enter the organism of an individual exposed to them (through food, breathing and intravenously) or, worse still, they can be generated endogenously in immunosuppressed individuals., Conclusion: The possibility of some cofactors being the real causes behind a large number of entities considered to be Aids, TSP, Sjogren s syndrome, fungoid mycosis or T cell leukaemia, among others, regardless of their retroviral serological state, is becoming more and more likely and scientifically plausible. All these facts should be researched in much greater depth to determine their real dimensions, which would therefore enable us to face the future with better means of prevention, diagnosis and treatment at our disposal.

Published

2002

37. Effects of LP-BM5 murine leukemia virus infection on errors and response time in a two-choice serial reaction time task in C57BL/6 mice.

Author

Lee B, Tumu P, and Paul IA

Subjects

Animals, Behavior, Animal, Conditioning, Operant, Male, Mice, Mice, Inbred C57BL, Murine Acquired Immunodeficiency Syndrome physiopathology, Organ Size, Photic Stimulation, Reference Values, Attention, Choice Behavior physiology, Leukemia Virus, Murine pathogenicity, Reaction Time, Retroviridae Infections physiopathology, Tumor Virus Infections physiopathology

Abstract

Human immunodeficiency virus type 1 (HIV-1) infection is often accompanied by cognitive, motor, and behavioral dysfunction. Cognitive function diminishes in indices of attention, psychomotor speed, and learning and memory. These are collectively termed acquired immunodeficiency syndrome dementia complex (ADC or neuroAIDS). Inoculation with the LP-BM5 murine leukemia virus (MuLV) causes profound immunosuppression (murine acquired immunodeficiency syndrome, or MAIDS) in C57BL/6 mice. Previous studies show that the LP-BM5 MuLV impairs learning and memory without gross motor impairment. Since learning and memory performance deficits can be related to attention deficits, we assessed the effect of LP-BM5 MuLV infection on sustained attention performance using a two-choice serial reaction time task. This task required the animals to detect a visual stimulus presented randomly on the right or the left unit and respond by a nose-poke in the illuminated hole within a 5 s period for water reward. The LP-BM5 MuLV infected group, like the control group, improved sustained attention performance until 7 weeks of virus infection in all measures including choice accuracy, response omission, and correct response time. However, during the late stage of infection, LP-BM5 MuLV infected mice showed selective sustained attention performance deficits. From 8 weeks after LP-BM5 MuLV infection, the virus infected mice started to lose their improved sustained attention performance in response omission and began to make correct responses more slowly than the control mice when the duration of stimulus light was 5 s. Moreover, at 13 and 14 weeks after LP-BM5 MuLV infection, the virus infected group made correct choices significantly less accurately than the control group when duration of stimulus light was shortest (1 s). These data show that LP-BM5 MuLV infection causes not only the previously reported learning and memory deficits but also produces sustained attention performance deficits in mice., (Copyright 2002 Elsevier Science B.V.)

Published

2002

38. Effects of chronic methamphetamine exposure on heart function in uninfected and retrovirus-infected mice.

Author

Yu Q, Montes S, Larson DF, and Watson RR

Subjects

Animals, Blood Pressure drug effects, Blood Pressure physiology, Cardiac Catheterization, Cardiac Output drug effects, Cardiac Output physiology, Female, Heart Function Tests, Hemodynamics drug effects, Hemodynamics physiology, Mice, Mice, Inbred C57BL, Stroke Volume drug effects, Stroke Volume physiology, Central Nervous System Stimulants pharmacology, Heart drug effects, Heart physiopathology, Leukemia Virus, Murine, Leukemia, Experimental physiopathology, Methamphetamine pharmacology, Retroviridae Infections physiopathology, Tumor Virus Infections physiopathology

Abstract

Methamphetamine (MA) increases catecholamine levels, which have detrimental effects on heart function through vasoconstriction, myocardial hypertrophy, and fibrosis. Murine retrovirus infection induces dilated cardiomyopathy (DCM). The present study investigated the cardiovascular effects of chronic MA treatment on uninfected and retrovirus-infected mice. C57BL/6 mice were studied after 12 weeks treatment. The four study groups were (group I) uninfected, MA placebo; (group II) infected, MA placebo; (group III) uninfected, MA treatment; and (group IV) infected and MA treatment. MA injections were given i.p. once a day for 5 days/week with a increasing dose from 15 mg/kg to 40 mg/kg. Left ventricular mechanics were measured in situ a using Millar conductance catheter system for pressure-volume loop analysis. Cardiac pathology was determined with histological analysis. In the uninfected mice, the load independent contractile parameters, pre-load recruitable stroke work (PRSW) and dP/dt(max) vs. Ved, significantly decreased by 32% and 35% in MA treated mice when compared to the saline injected mice. In retrovirus-infected mice, although there were no significant difference in Ees, PRSW, and dP/dt(max) vs. Ved due to MA treatment, they were increased 45%, 15% and 42% respectively when compared to saline treated mice. No further lowered heart function during murine AIDS may be due to the counteraction of the retroviral DCM and the MA induced myocardial fibrosis and hypertrophy (thickening of the ventricular walls). This is supported by increases in the End-diastolic volume (Ved, 38%) and End-systolic volume (Ves, 84%) in the retrovirus-infected saline injected mice, the decreases of 33% and 17% in the uninfected MA-treated mice, but no significant changes in the retrovirus-infected MA treated mice when compared to uninfected saline injected mice. These data suggest that MA induced myocardial cellular changes compensate for retrovirus induced DCM.

Published

2002

39. Temporal effects of gamma interferon deficiency on the course of Friend retrovirus infection in mice.

Author

Stromnes IM, Dittmer U, Schumacher TN, Schepers K, Messer RJ, Evans LH, Peterson KE, Race B, and Hasenkrug KJ

Subjects

Animals, Antibodies, Viral blood, Antiviral Agents therapeutic use, CD8-Positive T-Lymphocytes immunology, DNA, Viral blood, Flow Cytometry, Friend murine leukemia virus genetics, Friend murine leukemia virus isolation & purification, Interferon-gamma genetics, Interferon-gamma physiology, Interferon-gamma therapeutic use, Leukemia, Erythroblastic, Acute drug therapy, Leukemia, Erythroblastic, Acute virology, Leukemia, Experimental immunology, Leukemia, Experimental virology, Mice, Mice, Inbred C57BL, Mice, Knockout, Neutralization Tests, Polymerase Chain Reaction, RNA, Viral blood, Recombinant Proteins, Retroviridae Infections immunology, Retroviridae Infections virology, Spleen virology, Tumor Virus Infections immunology, Tumor Virus Infections virology, Friend murine leukemia virus pathogenicity, Interferon-gamma deficiency, Leukemia, Experimental physiopathology, Retroviridae Infections physiopathology, Tumor Virus Infections physiopathology

Abstract

The current studies demonstrate complex and seemingly contradictory effects by gamma interferon (IFN-gamma) on Friend virus (FV) infection. Both temporal and tissue-specific effects were observed. During the first week of infection, IFN-gamma-deficiency caused increased levels of FV infection in multiple tissues. Surprisingly, however, by 2 weeks postinfection, IFN-gamma-deficient mice had significantly lower levels of infection in both the spleen and bone marrow compared to wild-type mice. The rapid reduction of virus in the IFN-gamma-deficient mice correlated with a more rapid virus-neutralizing antibody response than was observed in the wild-type mice. Furthermore, the virus-neutralizing antibody response in wild-type mice could be accelerated by ablation of their IFN-gamma response. Although the IFN-gamma-deficient mice developed an accelerated virus-neutralizing antibody response, they did not class-switch to immunoglobulin G class immunoglobulins nor could they maintain long-term virus-neutralizing antibody titers. Eventually, all of the IFN-gamma-deficient mice failed to keep persistent virus in check and developed fatal FV-induced erythroleukemia.

Published

2002

40. Disruption of hematopoiesis and thymopoiesis in the early premalignant stages of infection with SL3-3 murine leukemia virus.

Author

Rulli K, Lenz J, and Levy LS

Subjects

3T3 Cells, Animals, Hematopoietic Stem Cells pathology, Hematopoietic Stem Cells virology, Leukemia, Experimental pathology, Leukemia, Experimental physiopathology, Leukemia, Experimental virology, Mice, Polymerase Chain Reaction, Preleukemia virology, Retroviridae Infections pathology, Retroviridae Infections physiopathology, Retroviridae Infections virology, Thymus Gland cytology, Thymus Gland virology, Tumor Virus Infections pathology, Tumor Virus Infections physiopathology, Tumor Virus Infections virology, Virus Replication, Hematopoiesis, Leukemia Virus, Murine, Preleukemia pathology, Preleukemia physiopathology, Thymus Gland pathology

Abstract

A time course analysis of SL3-3 murine leukemia virus (SL3) infection in thymus and bone marrow of NIH/Swiss mice was performed to assess changes that occur during the early stages of progression to lymphoma. Virus was detectable in thymocytes, bone marrow, and spleen as early as 1 to 2 weeks postinoculation (p.i.). In bone marrow, virus infection was detected predominantly in immature myeloid or granulocytic cells. Flow cytometry revealed significant reductions of the Ter-119(+) and Mac-1(+) populations, and significant expansions of the Gr-1(+) and CD34(+) populations, between 2 and 4 weeks p.i. Analysis of colony-forming potential confirmed these findings. In the thymus, SL3 replication was associated with significant disruption in thymocyte subpopulation distribution between 4 and 7 weeks p.i. A significant thymic regression was observed just prior to the clonal outgrowth of tumor cells. Proviral long terminal repeats (LTRs) with increasing numbers of enhancer repeats were observed to accumulate exclusively in the thymus during the first 8 weeks p.i. Observations were compared to the early stages of infection with a virtually nonpathogenic SL3 mutant, termed SL3DeltaMyb5, which was shown by real-time PCR to be replication competent. Comparison of SL3 with SL3DeltaMyb5 implicated certain premalignant changes in tumorigenesis, including (i) increased proportions of Gr-1(+) and CD34(+) bone marrow progenitors, (ii) a significant increase in the proportion of CD4(-) CD8(-) thymocytes, (iii) thymic regression prior to tumor outgrowth, and (iv) accumulation of LTR enhancer variants. A model in which disrupted bone marrow hematopoiesis and thymopoiesis contribute to the development of lymphoma in the SL3-infected animal is discussed.

Published

2002

41. Retroviral diseases of the nervous system: pathogenic host response or viral gene-mediated neurovirulence?

Author

Power C

Subjects

Animals, Humans, Life Cycle Stages, Phylogeny, Retroviridae classification, Virulence genetics, Nervous System Diseases virology, Retroviridae genetics, Retroviridae pathogenicity, Retroviridae Infections physiopathology, Retroviridae Infections virology

Abstract

Retroviruses represent an important group of RNA viruses that cause a spectrum of nervous system diseases. Furthermore, newly recognized retroviral infections of the nervous system and some retroviral vectors or proteins used for gene delivery raise potential safety concerns. This article highlights different retroviruses and their causative mechanisms of nervous system disease, or neurovirulence. Specific sequences within retroviral genes might determine the development of neurovirulence. Conversely, neurovirulent retroviruses also activate host immune responses, resulting in a neuropathogenic cascade that is mediated by pro-inflammatory and neurotoxic molecules, ultimately culminating in neuronal death. Thus, retroviral infections of the nervous system illustrate a molecular interplay between distinct infectious agents and pathogenic host responses, which results in neurovirulence.

Published

2001

42. c-MYC induces mammary tumorigenesis by means of a preferred pathway involving spontaneous Kras2 mutations.

Author

D'Cruz CM, Gunther EJ, Boxer RB, Hartman JL, Sintasath L, Moody SE, Cox JD, Ha SI, Belka GK, Golant A, Cardiff RD, and Chodosh LA

Subjects

Animals, Female, Genes, ras, Humans, Intracellular Signaling Peptides and Proteins, Mammary Tumor Virus, Mouse genetics, Mammary Tumor Virus, Mouse physiology, Mice, Mice, Transgenic, Mutagenesis, Ornithine Decarboxylase genetics, Proteins genetics, Proto-Oncogene Proteins p21(ras), RNA, Messenger metabolism, ras Proteins, GADD45 Proteins, Adenocarcinoma physiopathology, Gene Expression Regulation, Neoplastic, Mammary Neoplasms, Experimental physiopathology, Proto-Oncogene Proteins genetics, Proto-Oncogene Proteins c-myc genetics, Retroviridae Infections physiopathology, Tumor Virus Infections physiopathology

Abstract

Although the process of mammary tumorigenesis requires multiple genetic events, it is unclear to what extent carcinogenesis proceeds through preferred secondary pathways following a specific initiating oncogenic event. Similarly, the extent to which established mammary tumors remain dependent on individual mutations for maintenance of the transformed state is unknown. Here we use the tetracycline regulatory system to conditionally express the human c-MYC oncogene in the mammary epithelium of transgenic mice. MYC encodes a transcription factor implicated in multiple human cancers. In particular, amplification and overexpression of c-MYC in human breast cancers is associated with poor prognosis, although the genetic mechanisms by which c-MYC promotes tumor progression are poorly understood. We show that deregulated c-MYC expression in this inducible system results in the formation of invasive mammary adenocarcinomas, many of which fully regress following c-MYC deinduction. Approximately half of these tumors harbor spontaneous activating point mutations in the ras family of proto-oncogenes with a strong preference for Kras2 compared with Hras1. Nearly all tumors lacking activating ras mutations fully regressed following c-MYC deinduction, whereas tumors bearing ras mutations did not, suggesting that secondary mutations in ras contribute to tumor progression. These findings demonstrate that c-MYC-induced mammary tumorigenesis proceeds through a preferred secondary oncogenic pathway involving Kras2.

Published

2001

43. Friend erythroleukemia revisited.

Author

Ney PA and D'Andrea AD

Subjects

Animals, Friend murine leukemia virus chemistry, Friend murine leukemia virus enzymology, Leukemia, Erythroblastic, Acute enzymology, Leukemia, Erythroblastic, Acute metabolism, Leukemia, Erythroblastic, Acute physiopathology, Mice, Multigene Family, Protein-Tyrosine Kinases physiology, Proto-Oncogene Proteins c-met genetics, Proto-Oncogene Proteins c-met physiology, Receptors, Erythropoietin metabolism, Receptors, Erythropoietin physiology, Retroviridae Infections enzymology, Retroviridae Infections metabolism, Retroviridae Infections physiopathology, Signal Transduction, Tumor Virus Infections enzymology, Tumor Virus Infections metabolism, Tumor Virus Infections physiopathology, Viral Envelope Proteins metabolism, Viral Envelope Proteins physiology, Friend murine leukemia virus physiology, Leukemia, Erythroblastic, Acute virology

Published

2000

44. Soluble complement receptor 1 (CD35) delivered by retrovirally infected syngeneic cells or by naked DNA injection prevents the progression of collagen-induced arthritis.

Author

Dreja H, Annenkov A, and Chernajovsky Y

Subjects

Animals, Arthritis drug therapy, Arthritis immunology, Arthritis, Rheumatoid chemically induced, Autoimmune Diseases drug therapy, Collagen, Complement Pathway, Alternative drug effects, DNA administration & dosage, Disease Progression, Injections, Injections, Intramuscular, Male, Mice, Receptors, Complement genetics, Arthritis, Rheumatoid therapy, Fibroblasts virology, Genetic Therapy methods, Receptors, Complement therapeutic use, Retroviridae Infections physiopathology

Abstract

Objective: The complement system is important in the development of autoimmune inflammation, including rheumatoid arthritis (RA) and collagen-induced arthritis (CIA). Complement receptor 1 (CR1) is involved in regulation of complement activity. Studies on models of autoimmunity have demonstrated that soluble CR1 (sCR1) is a potent therapeutic agent. The present study was thus undertaken to investigate the feasibility of antiinflammatory gene therapy to prevent CIA by delivery of genes encoding truncated sCR1 (tsCR1) and dimeric tsCR1-Ig., Methods: Syngeneic fibroblasts or arthritogenic splenocytes, engineered to express tsCR1 using retrovirus-mediated gene transfer, were injected into DBA/1 recipients that had been immunized with bovine type II collagen (CII). In separate experiments, naked DNA containing tsCR1 and tsCR1-Ig genes was injected intramuscularly into the immunized animals. The clinical development of arthritis was monitored, anti-CII levels measured, and antigenic T cell response studied. Affinity-purified tsCR1-Ig was assayed for its inhibitory effect on the alternative complement pathway in mouse serum., Results: Treatment of CII-immunized mice with the tsCR1-expressing cells inhibited development of CIA, reduced anti-CII antibody levels, and inhibited T cell response to CII in vitro. Intramuscular injections of DNA encoding the CR1 genes prevented the progression of disease. Furthermore, compared with full-length sCR1, purified tsCR1-Ig was more active in inhibiting the murine alternative complement pathway., Conclusion: Our findings demonstrated that tsCR1 and tsCR1-Ig, when delivered via gene therapy, had a beneficial effect on autoimmune inflammation. These results indicate that targeting the complement system in RA patients may be of clinical importance.

Published

2000

45. Suppression of neurocognitive damage in LP-BM5-infected mice with a targeted deletion of the TNF-alpha gene.

Author

Iida R, Saito K, Yamada K, Basile AS, Sekikawa K, Takemura M, Fujii H, Wada H, Seishima M, and Nabeshima T

Subjects

Animals, CD4-CD8 Ratio, Maze Learning, Mice, Mice, Inbred C57BL, Mice, Knockout, Nervous System Diseases genetics, Retroviridae Infections immunology, Gene Deletion, Leukemia Virus, Murine physiology, Nervous System Diseases prevention & control, Retroviridae Infections physiopathology, Tumor Necrosis Factor-alpha genetics

Abstract

Brain levels of TNF-alpha increase in many inflammatory conditions, including HIV-1 infection, and may contribute to neurodegenerative processes. The paucity of agents that can selectively and potently block TNF-alpha processing or its receptors has led us to investigate the role of TNF-alpha in chronic neurodegeneration associated with retroviral infection using mice with targeted deletions of the TNF-alpha gene. Infection of wild-type C57BL/6 mice with the LP-BM5 murine leukemia retrovirus mixture leads to the development of a severe immunodeficiency as well as cognitive deficits and neuronal damage. TNF-alpha-(-/-) mice infected with LP-BM5 developed a systemic immunopathology indistinguishable in severity from that observed in contemporaneously infected wild-type mice. In contrast, the performance of infected TNF-alpha-(-/-) mice in the Y-maze and Morris water maze was not different from that of uninfected TNF-alpha-(-/-) mice. The extent of glial activation in the striatum, as indicated by the increase in density of peripheral benzodiazepine receptors, was equivalent in both groups of LP-BM5-infected mice. However, the decrease in striatal MAP-2 expression, a marker of neurodegeneration observed in infected wild-type mice, was not found in infected TNF-alpha-(-/-) mice. While the loss of TNF-alpha appeared to have no effect on the course or severity of the central or peripheral immunopathology resulting from LP-BM5 infection, the behavioral and biochemical manifestations were substantially curtailed in the TNF-alpha-(-/-) mice. These findings directly support a role for TNF-alpha in the neurodegenerative processes associated with viral infections such as HIV-1.

Published

2000

46. Strategies of antiretroviral therapy in adults.

Author

Itani S and Bartlett JA

Subjects

Adult, Antiviral Agents adverse effects, HIV Infections drug therapy, HIV Infections prevention & control, Humans, Protease Inhibitors therapeutic use, Retroviridae Infections physiopathology, Urinary Tract Infections physiopathology, Antiviral Agents therapeutic use, Retroviridae Infections drug therapy, Urinary Tract Infections drug therapy, Urinary Tract Infections virology

Abstract

Recent progress in antiretroviral treatment has led to dramatic improvements in HIV-related morbidity and mortality. These improvements have been fostered by advances in our understanding of HIV-related pathogenesis, the use of plasma HIV RNA levels to monitor patients, and the availability of 13 licensed antiretroviral drugs. Numerous drug combinations, especially those containing three or more agents, can suppress plasma HIV RNA levels below the lower limit of detection in the majority of treated patients. Urologists should be familiar with the limitations of this therapeutic response: patient adherence, drug resistance, a residual burden of chronically infected cells which are refractory to treatment, an unknown impact on HIV in genital secretions, and potential transmissibility through sexual contact.

Published

1999

47. A friendly signal.

Author

Schwartzberg PL

Subjects

Animals, Humans, Leukemia, Erythroblastic, Acute virology, Receptor Protein-Tyrosine Kinases physiology, Receptors, Cell Surface physiology, Friend murine leukemia virus, Retroviridae Infections physiopathology, Signal Transduction, Tumor Virus Infections physiopathology

Published

1999

48. Increased blood-brain barrier permeability in LP-BM5 infected mice is mediated by neuroexcitatory mechanisms.

Author

Kustova Y, Grinberg A, and Basile AS

Subjects

Animals, Blood Proteins metabolism, Coloring Agents, Dizocilpine Maleate pharmacology, Evans Blue, Excitatory Amino Acid Antagonists pharmacology, Glutamic Acid physiology, Immunohistochemistry, Male, Mice, Mice, Inbred C57BL, Prosencephalon drug effects, Prosencephalon metabolism, Receptors, N-Methyl-D-Aspartate antagonists & inhibitors, Blood-Brain Barrier physiology, Brain Diseases physiopathology, Leukemia, Experimental physiopathology, Retroviridae Infections physiopathology

Abstract

Serum protein levels in LP-BM5 infected mouse brains were investigated to gain insight into the contribution of blood-brain barrier (BBB) patency to the pathogenesis of retroviral encephalopathy. Evans blue uptake by the forebrain and cerebellum was significantly increased between 8-12 weeks post inoculation. Immunohistochemistry revealed foci of albumin, transferrin, alpha(2)-macroglobulin and IgG transudation around blood vessels particularly in the cerebral cortex and cerebellar vermis. These leaks were often associated with astrocytosis and apoptotic cells. Unlike the other serum proteins, IgG immunoreactivity extended from the circumventricular organs and disseminated throughout the brain parenchyma, accumulating on the plasma membranes of hippocampal and cortical neurons. Consistent with the chronic elevation of free glutamate levels in LP-BM5 infected mice, the increase in Evans blue uptake into the forebrain was completely reversed following dizocilpine administration. Thus, the chronic increase in free glutamate levels in LP-BM5 infected mouse brain contributes to BBB disruption. Furthermore, the CNS accumulation of serum proteins, particularly IgG, observed in these mice may increase osmotic load, impair neuronal function, and cause white matter pallor. Administration of NMDA receptor antagonists may prove useful in managing BBB permeability in those neuropathologies, such as HIV-associated dementia/cognitive/motor complex, having a glutamatergic component.

Published

1999

49. Experimental infection of calves with bovine leukemia virus (BLV): an applicable model of a retroviral infection.

Author

Ungar-Waron H, Paz R, Brenner J, Yakobson B, Partosh N, and Trainin Z

Subjects

Animals, CD4 Antigens analysis, CD5 Antigens analysis, CD8 Antigens analysis, Cattle, Lymphocytes chemistry, Lymphocytes immunology, Male, Disease Models, Animal, Enzootic Bovine Leukosis physiopathology, Leukemia Virus, Bovine, Retroviridae Infections physiopathology

Abstract

An experimental model of chronic infection with bovine leukemia virus (BLV) was established in young calves within a relatively short time. In the sera of all infected calves, precipitating antibodies were detected within 5 weeks after infection but upon disease progression pattern of cellular profiles varied. Three calves exhibited transient lymphocytosis 3-5 weeks after infection, two became persistent lymphocytotic (PL+) by that time and one stayed non-lymphocytotic (PL-) for 11 weeks and became PL+ after 4.5 months. Eventually all infected calves became PL+ by the end of the experiment, 6-12 months after infection. Increase of total counts of peripheral blood mononuclear cells (PBMC) related to polyclonal expansion of B-cells. The latter was assessed in all infected calves where the expansion of CD5-bearing cells (B+ CD5+) correlated with increase or decrease of total PBMC counts. Other cell populations such as CD4 and CD8 were also affected. Percentages decreased by 5 weeks after experimental infection to about half their original values though actual cell numbers stayed relatively stable. The experimental model we established compared well with field cases of naturally BLV-infected cattle and thus permitted the investigation of the disease at early stages of infection.

Published

1999

50. [Molecular dialogue between human retroviruses and host cells].

Author

Devaux CA

Subjects

CD4 Antigens physiology, HIV pathogenicity, HIV physiology, Humans, Receptors, CXCR4 physiology, Receptors, HIV physiology, Retroviridae pathogenicity, Retroviridae Infections virology, Virus Replication, Receptors, Virus physiology, Retroviridae physiology, Retroviridae Infections physiopathology

Abstract

Several exogenous retroviruses are etiologic agents of severe human diseases. Retrovirus replication depends on a plethora of highly specific interactions with the host cell resulting in the subversion of multiple cellular signal transduction pathways. Understanding the molecular cross-talk that regulates the relationship between the virus and the host cell is currently the objective of many researchers and should contribute to gain insight into puzzling features of the physiopathology of retrovirus infections. A large body of recent data indicates that retroviruses utilize a variety of unrelated cell surface receptors to initiate infection and modulate the homeostasis of the target cell following receptors binding. As an example, I discuss here the tremendous capacity of HIV-1 envelope glycoproteins to modulate kinases activation and nuclear translocation of transcription factors following binding to surface receptors CD4 and CXCR4. Viral envelope glycoproteins interaction with CD4 controls cell activation and proliferation required for virus production whereas interaction with CXCR4 favors apoptosis thereby decreasing the host immune response.

Published

1999