Your search keyword '"Jason A. Iskarpatyoti"' showing total 6 results

1. Age-dependent susceptibility to reovirus encephalitis in mice is influenced by maturation of the type-I interferon response

Author

Judy J. Brown, Allen G Wu, Jennifer E. Stencel-Baerenwald, Andrea J. Pruijssers, Danica M. Sutherland, Jason A. Iskarpatyoti, and Terence S. Dermody

Subjects

Gene Expression Regulation, Viral, 0301 basic medicine, viruses, Orthoreovirus, Mammalian, Apoptosis, Receptor, Interferon alpha-beta, Adaptive Immunity, Biology, Virus Replication, Article, Cell Line, Microbiology, Mice, 03 medical and health sciences, 0302 clinical medicine, Immune system, Interferon, Immunity, medicine, Animals, Encephalitis, Viral, Mice, Knockout, Inoculation, Viral encephalitis, Age Factors, Brain, Viral Load, medicine.disease, Immunity, Innate, Reoviridae Infections, 3. Good health, DNA-Binding Proteins, Mice, Inbred C57BL, 030104 developmental biology, Viral replication, Interferon Type I, Pediatrics, Perinatology and Child Health, Viral load, Spleen, 030217 neurology & neurosurgery, Encephalitis, medicine.drug

Abstract

BackgroundInfants and young children are particularly susceptible to viral encephalitis; however, the mechanisms are unknown. We determined the age-dependent contribution of innate and adaptive immune functions to reovirus-induced encephalitis in mice.MethodsNewborn wild-type mice, 2-20 days of age, were inoculated with reovirus or diluent and monitored for mortality, weight gain, and viral load. Four- and fifteen-day-old IFNAR-/- and RAG2-/- mice were inoculated with reovirus and similarly monitored.ResultsWeight gain was impaired in mice inoculated with reovirus at 8 days of age or less. Clinical signs of encephalitis were detected in mice inoculated at 10 days of age or less. Mortality decreased when mice were inoculated after 6 days of age. Survival was ≤15% in wild type (WT), RAG2-/-, and IFNAR-/- mice inoculated at 4 days of age. All WT mice, 92% of RAG2-/- mice, and only 48% of IFNAR-/- mice survived following inoculation at 15 days of age.ConclusionsSusceptibility of mice to reovirus-induced disease decreases between 6 and 8 days of age. Enhanced reovirus virulence in IFNAR-/- mice relative to WT and RAG2-/- mice inoculated at 15 days of age suggests that maturation of the type-I interferon response contributes to age-related mortality following reovirus infection.

Published

2018

2. Reovirus infection triggers inflammatory responses to dietary antigens and development of celiac disease

Author

Mine R. Ikizler, Fengling Hu, Matthew A. Zurenski, Bana Jabri, Karl W. Boehme, Hans Christian Reinecker, Chaitan Khosla, Brad A. Palanski, Sangman M. Kim, Romain Bouziat, Jason A. Iskarpatyoti, Valentina Discepolo, Ian Lawrence, Jordan D. Ernest, Léa M.M. Costes, Valérie Abadie, Mukund Varma, Janneke N. Samsom, Terence S. Dermody, Solomiia Khomandiak, Ramnik J. Xavier, Carol E. Semrad, Marlies Meisel, Andrea J. Pruijssers, Jennifer E. Stencel-Baerenwald, Nicole McAllister, Sonia S. Kupfer, Reinhard Hinterleitner, Toufic Mayassi, Pavithra Aravamudhan, Stefano Guandalini, Luis B. Barreiro, Judy J. Brown, Aylwin Ng, Bouziat, R., Hinterleitner, R., Brown, J. J., Stencel-Baerenwald, J. E., Ikizler, M., Mayassi, T., Meisel, M., Kim, S. M., Discepolo, V., Pruijssers, A. J., Ernest, J. D., Iskarpatyoti, J. A., Costes, L. M. M., Lawrence, I., Palanski, B. A., Varma, M., Zurenski, M. A., Khomandiak, S., Mcallister, N., Aravamudhan, P., Boehme, K. W., Hu, F., Samsom, J. N., Reinecker, H. -C., Kupfer, S. S., Guandalini, S., Semrad, C. E., Abadie, V., Khosla, C., Barreiro, L. B., Xavier, R. J., Ng, A., Dermody, T. S., Jabri, B., and Pediatrics

Subjects

0301 basic medicine, viruses, Autoimmunity, Receptor, Interferon alpha-beta, Disease, Mice, 0302 clinical medicine, Interferon, Reoviridae Infection, Pathogen, Multidisciplinary, Effector, Intestine, Intestines, medicine.anatomical_structure, Antigen, Interferon Type I, 030211 gastroenterology & hepatology, Genetic Engineering, Human, medicine.drug, Glutens, Regulatory T cell, Mice, Transgenic, Biology, Reoviridae, Article, Virus, 03 medical and health sciences, Immunity, Immune Tolerance, medicine, Animals, Humans, Antigens, Autoantibodies, Inflammation, Transglutaminases, Animal, Th1 Cells, biochemical phenomena, metabolism, and nutrition, Virology, Diet, Reoviridae Infections, Mice, Inbred C57BL, Celiac Disease, Disease Models, Animal, 030104 developmental biology, IRF1, Immunology, Gluten, Interferon Regulatory Factor-1

Abstract

Viral infections have been proposed to elicit pathological processes leading to the initiation of T helper 1 (TH1) immunity against dietary gluten and celiac disease (CeD). To test this hypothesis and gain insights into mechanisms underlying virus-induced loss of tolerance to dietary antigens, we developed a viral infection model that makes use of two reovirus strains that infect the intestine but differ in their immunopathological outcomes. Reovirus is an avirulent pathogen that elicits protective immunity, but we discovered that it can nonetheless disrupt intestinal immune homeostasis at inductive and effector sites of oral tolerance by suppressing peripheral regulatory T cell (pTreg) conversion and promoting TH1 immunity to dietary antigen. Initiation of TH1 immunity to dietary antigen was dependent on interferon regulatory factor 1 and dissociated from suppression of pTreg conversion, which was mediated by type-1 interferon. Last, our study in humans supports a role for infection with reovirus, a seemingly innocuous virus, in triggering the development of CeD.

Published

2017

3. Antiviral immunity via RIG-I-mediated recognition of RNA bearing 5′-diphosphates

Author

Tsutomu Fujimura, Christine Schuberth, Andrea J. Pruijssers, Jan Rehwinkel, Caetano Reis e Sousa, Delphine Goubau, Jason A. Iskarpatyoti, Martin Schlee, Gunther Hartmann, Thomas Zillinger, Terence S. Dermody, Annemarthe G. van der Veen, Safia Deddouche, Janos Ludwig, Marion Goldeck, Winfried Barchet, Cancer Research UK, European Research Council, Fondation Bettencourt Schueller, Department of Health and Human Services (US), Vanderbilt University, Fundación Ramón Areces, German Research Foundation, and German Center for Infection Research

Subjects

Male, viruses, Genome, Viral, Biology, Reoviridae, RIG-I-like receptor, Article, Virus, DEAD-box RNA Helicases, Mice, Sense (molecular biology), Animals, Base Pairing, Gene, Multidisciplinary, Innate immune system, Base Sequence, RIG-I, virus diseases, RNA, MDA5, biochemical phenomena, metabolism, and nutrition, Virology, Immunity, Innate, 3. Good health, Diphosphates, DEAD Box Protein 58, RNA, Viral, Female

Abstract

Mammalian cells possess mechanisms to detect and defend themselves from invading viruses. In the cytosol, the RIG-I-like receptors (RLRs), RIG-I (retinoic acid-inducible gene I; encoded by DDX58) and MDA5 (melanoma differentiation-associated gene 5; encoded by IFIH1) sense atypical RNAs associated with virus infection. Detection triggers a signalling cascade via the adaptor MAVS that culminates in the production of type I interferons (IFN-¿ and ß; hereafter IFN), which are key antiviral cytokines. RIG-I and MDA5 are activated by distinct viral RNA structures and much evidence indicates that RIG-I responds to RNAs bearing a triphosphate (ppp) moiety in conjunction with a blunt-ended, base-paired region at the 5'-end (reviewed in refs 1, 2, 3). Here we show that RIG-I also mediates antiviral responses to RNAs bearing 5'-diphosphates (5'pp). Genomes from mammalian reoviruses with 5'pp termini, 5'pp-RNA isolated from yeast L-A virus, and base-paired 5'pp-RNAs made by in vitro transcription or chemical synthesis, all bind to RIG-I and serve as RIG-I agonists. Furthermore, a RIG-I-dependent response to 5'pp-RNA is essential for controlling reovirus infection in cultured cells and in mice. Thus, the minimal determinant for RIG-I recognition is a base-paired RNA with 5'pp. Such RNAs are found in some viruses but not in uninfected cells, indicating that recognition of 5'pp-RNA, like that of 5'ppp-RNA, acts as a powerful means of self/non-self discrimination by the innate immune system., C.R.S., D.G., S.D. and A.G.V.V. are funded by Cancer Research UK, a prize from Fondation Bettencourt-Schueller, and a grant from the European Research Council (ERC Advanced Researcher Grant AdG-2010-268670). A.J.P. and T.S.D. are supported by Public Health Service award R37 AI038296 and the Elizabeth B. Lamb Center for Pediatric Research. T.F. is supported by the Fundación Ramón Areces. G.H., M.S. and W.B. are supported by the Deutsche Forschungsgemeinschaft (http://www.dfg.de; SFB670 to M.S., W.B. and G.H., DFG SCHL1930/1-1 to M.S., SFB704 to G.H. and W.B., SFB832 and KFO177 to G.H.). G.H. and M.S. are supported by the DFG Excellence Cluster ImmunoSensation. G.H. is supported by the German Center of Infectious Disease (DZIF).

Published

2014

4. Proteomic Analysis of Mitochondrial-Associated ER Membranes (MAM) during RNA Virus Infection Reveals Dynamic Changes in Protein and Organelle Trafficking

Author

Courtney Wilkins, Stacy M. Horner, Samantha Badil, Michael Gale, and Jason A. Iskarpatyoti

Subjects

Proteome, viruses, Science, Hepacivirus, Proteomics, Endoplasmic Reticulum, Virus Replication, Sendai virus, Cell Line, 03 medical and health sciences, 0302 clinical medicine, Immune system, Tandem Mass Spectrometry, Microsomes, Humans, Chromatography, High Pressure Liquid, 030304 developmental biology, 0303 health sciences, Principal Component Analysis, Multidisciplinary, Innate immune system, biology, Signal transducing adaptor protein, RNA, Correction, RNA virus, biology.organism_classification, Virology, 3. Good health, Cell biology, Mitochondria, Viral replication, Medicine, 030217 neurology & neurosurgery, Metabolic Networks and Pathways, Research Article

Abstract

RIG-I pathway signaling of innate immunity against RNA virus infection is organized between the ER and mitochondria on a subdomain of the ER called the mitochondrial-associated ER membrane (MAM). The RIG-I adaptor protein MAVS transmits downstream signaling of antiviral immunity, with signaling complexes assembling on the MAM in association with mitochondria and peroxisomes. To identify components that regulate MAVS signalosome assembly on the MAM, we characterized the proteome of MAM, ER, and cytosol from cells infected with either chronic (hepatitis C) or acute (Sendai) RNA virus infections, as well as mock-infected cells. Comparative analysis of protein trafficking dynamics during both chronic and acute viral infection reveals differential protein profiles in the MAM during RIG-I pathway activation. We identified proteins and biochemical pathways recruited into and out of the MAM in both chronic and acute RNA viral infections, representing proteins that drive immunity and/or regulate viral replication. In addition, by using this comparative proteomics approach, we identified 3 new MAVS-interacting proteins, RAB1B, VTN, and LONP1, and defined LONP1 as a positive regulator of the RIG-I pathway. Our proteomic analysis also reveals a dynamic cross-talk between subcellular compartments during both acute and chronic RNA virus infection, and demonstrates the importance of the MAM as a central platform that coordinates innate immune signaling to initiate immunity against RNA virus infection.

Published

2015

5. A plasmid-based reverse genetics system for mammalian orthoreoviruses driven by a plasmid-encoded T7 RNA polymerase

Author

Takahiro Kawagishi, Mine R. Ikizler, Takeshi Kobayashi, Terence S. Dermody, Satoshi Komoto, Jason A. Iskarpatyoti, and Koki Taniguchi

Subjects

viruses, Orthoreovirus, Mammalian, RNA-dependent RNA polymerase, DNA-Directed RNA Polymerases, Biology, Transfection, Virology, Reverse genetics, Virus, Reverse Genetics, Article, Viral vector, Cell Line, Viral Proteins, Plasmid, Viral replication, Complementary DNA, medicine, T7 RNA polymerase, Animals, Humans, medicine.drug

Abstract

Mammalian orthoreoviruses (reoviruses) have served as highly useful models for studies of virus replication and pathogenesis. The development of a plasmid-based reverse genetics system represented a major breakthrough in reovirus research. The current reverse genetics systems for reoviruses rely on the expression of T7 RNA polymerase within cells transfected with reovirus gene-segment cDNA plasmids. In these systems, the T7 RNA polymerase is provided by using a recombinant vaccinia virus expressing T7 RNA polymerase or a cell line constitutively expressing T7 RNA polymerase. Here, we describe an alternative plasmid-based rescue system driven by a plasmid-encoded T7 RNA polymerase, which could increase the flexibility of such reverse genetics systems. Although this approach requires transfection of an additional plasmid, virus recovery was achieved when A549, BHK-21, or L929 cells were co-transfected with a reovirus 10-plasmid set together with a plasmid encoding T7 RNA polymerase. Theoretically, this system offers the possibility to generate reoviruses in any cell line, including those amenable to propagation of viral vectors for clinical use. Thus, this approach will increase the flexibility of reverse genetics for basic studies of reovirus biology and foster development of reoviruses for clinical applications.

Published

2013

6. A rapid, automated approach for quantitation of rotavirus and reovirus infectivity

Author

John Guan, Jason A. Iskarpatyoti, Nikhat Contractor, Mine R. Ikizler, E. Ashley Morse, Terence S. Dermody, J. Denise Wetzel, and Janet Z. Willis

Subjects

Infectivity, Antiserum, Rotavirus, medicine.diagnostic_test, biology, medicine.drug_class, viruses, Fluorescent Antibody Technique, Monoclonal antibody, Immunofluorescence, medicine.disease_cause, Reoviridae, Primary and secondary antibodies, Virology, Molecular biology, Virus, Cell Line, Automation, Polyclonal antibodies, medicine, biology.protein, Image Processing, Computer-Assisted, Humans

Abstract

Current microscopy-based approaches for immunofluorescence detection of viral infectivity are time consuming and labor intensive and can yield variable results subject to observer bias. To circumvent these problems, we developed a rapid and automated infrared immunofluorescence imager-based infectivity assay for both rotavirus and reovirus that can be used to quantify viral infectivity and infectivity inhibition. For rotavirus, monolayers of MA104 cells were infected with simian strain SA-11 or SA-11 preincubated with rotavirus-specific human IgA. For reovirus, monolayers of either HeLa S3 cells or L929 cells were infected with strains type 1 Lang (T1L), type 3 Dearing (T3D), or either virus preincubated with a serotype-specific neutralizing monoclonal antibody (mAb). Infected cells were fixed and incubated with virus-specific polyclonal antiserum, followed by an infrared fluorescence-conjugated secondary antibody. Well-to-well variation in cell number was normalized using fluorescent reagents that stain fixed cells. Virus-infected cells were detected by scanning plates using an infrared imager, and results were obtained as a percent response of fluorescence intensity relative to a virus-specific standard. An expected dose-dependent inhibition of both SA-11 infectivity with rotavirus-specific human IgA and reovirus infectivity with T1L-specific mAb 5C6 and T3D-specific mAb 9BG5 was observed, confirming the utility of this assay for quantification of viral infectivity and infectivity blockade. The imager-based viral infectivity assay fully automates data collection and provides an important advance in technology for applications such as screening for novel modulators of viral infectivity. This basic platform can be adapted for use with multiple viruses and cell types.

Published

2011