Your search keyword '"Pichlmair A"' showing total 15 results

1. Protein Kinase R Contributes to Immunity against Specific Viruses by Regulating Interferon mRNA Integrity.

Author

Schulz, Oliver, Pichlmair, Andreas, Rehwinkel, Jan, Rogers, Neil C., Scheuner, Donalyn, Kato, Hiroki, Takeuchi, Osamu, Akira, Shizuo, Kaufman, Randal J., and Reis e Sousa, Caetano

Subjects

PROTEIN kinases, CELLULAR immunity, MESSENGER RNA, INTERFERONS, GENETIC regulation, RNA viruses, MOLECULAR recognition, LABORATORY mice

Abstract

Summary: Cytosolic viral RNA recognition by the helicases RIG-I and MDA5 is considered the major pathway for IFN-α/β induction in response to RNA viruses. However, other cytoplasmic RNA sensors, including the double-stranded RNA-binding protein kinase R (PKR), have been implicated in IFN-α/β production, although their relative contribution and mechanism have been unclear. Using cells expressing nonfunctional PKR or reduced levels of kinase, we show that PKR is required for production of IFN-α/β proteins in response to a subset of RNA viruses including encephalomyocarditis, Theiler''s murine encephalomyelitis, and Semliki Forest virus, but not influenza or Sendai virus. Surprisingly, although IFN-α/β mRNA induction is largely normal in PKR-deficient cells, much of that mRNA lacks the poly(A) tail, indicating that its integrity is compromised. Our results suggest that PKR plays a nonredundant role in IFN-α/β production in response to some but not all viruses, in part by regulating IFN-α/β mRNA stability. [Copyright &y& Elsevier]

Published

2010

2. Innate Recognition of Viruses

Author

Pichlmair, Andreas and Reis e Sousa, Caetano

Subjects

*NATURAL immunity, *VIRAL disease prevention, *VIRUS diseases, *IMMUNOREGULATION

Abstract

Virus infection elicits potent responses in all cells intended to contain virus spread before intervention by the adaptive immune system. Central to this process is the virus-elicited production of type I interferons (IFNs) and other cytokines. The sensors involved in coupling recognition of viruses to the induction of the type I IFN genes have only recently been uncovered and include endosomal and cytosolic receptors for RNA and DNA. Here, we review their properties and discuss how their ability to recognize the unusual presence of atypical nucleic acids in particular subcellular compartments is used by the body to detect virus presence. [Copyright &y& Elsevier]

Published

2007

3. Gambling with Flu: “All in” to Maximize Reward.

Author

Stukalov, Alexey and Pichlmair, Andreas

Abstract

In this issue of Cell Host & Microbe , Tripathi et al. (2015) report an in-depth meta-analysis of eight influenza virus siRNA screens combined with viral-host protein interactome data. The integration of the different omics datasets highlights candidate genes and pathways for further investigation and potential therapeutic targeting in the future. [ABSTRACT FROM AUTHOR]

Published

2015

4. Cell-free production of personalized therapeutic phages targeting multidrug-resistant bacteria.

Author

Emslander, Quirin, Vogele, Kilian, Braun, Peter, Stender, Jana, Willy, Christian, Joppich, Markus, Hammerl, Jens A., Abele, Miriam, Meng, Chen, Pichlmair, Andreas, Ludwig, Christina, Bugert, Joachim J., Simmel, Friedrich C., and Westmeyer, Gil G.

Subjects

*BACTERIOPHAGES, *PROTEOMICS, *YERSINIA pestis, *BACTERIA, *GRAM-positive bacteria, *KLEBSIELLA pneumoniae, *MULTIDRUG resistance in bacteria

Abstract

Bacteriophages are potent therapeutics against biohazardous bacteria, which rapidly develop multidrug resistance. However, routine administration of phage therapy is hampered by a lack of rapid production, safe bioengineering, and detailed characterization of phages. Thus, we demonstrate a comprehensive cell-free platform for personalized production, transient engineering, and proteomic characterization of a broad spectrum of phages. Using mass spectrometry, we validated hypothetical and non-structural proteins and could also monitor the protein expression during phage assembly. Notably, a few microliters of a one-pot reaction produced effective doses of phages against enteroaggregative Escherichia coli (EAEC), Yersinia pestis , and Klebsiella pneumoniae. By co-expressing suitable host factors, we could extend the range of cell-free production to phages targeting gram-positive bacteria. We further introduce a non-genomic phage engineering method, which adds functionalities for only one replication cycle. In summary, we expect this cell-free methodology to foster reverse and forward phage engineering and customized production of clinical-grade bacteriophages. [Display omitted] • Personalized and cell-free production of phages against multidrug-resistant bacteria • Extending cell-free production to phages targeting gram-positive bacteria • Transient, non-genomic engineering of bacteriophages • Time-resolved proteomics during phage assembly and validation of phage proteins Emslander, Vogele et al. demonstrate the personalized production of therapeutic bacteriophages in a cell-free system. This approach is faster and safer than the conventional method based on cultivating host bacteria. Cell-free production also allows for time-resolved proteome analysis during phage assembly and biosafe, non-genomic engineering of single-use phages targeting multidrug-resistant bacteria. [ABSTRACT FROM AUTHOR]

Published

2022

5. Phosphorylation-Dependent Feedback Inhibition of RIG-I by DAPK1 Identified by Kinome-wide siRNA Screening.

Author

Willemsen, Joschka, Wicht, Oliver, Wolanski, Julia C., Baur, Nina, Bastian, Sandra, Haas, Darya A., Matula, Petr, Knapp, Bettina, Meyniel-Schicklin, Laurène, Wang, Chen, Bartenschlager, Ralf, Lohmann, Volker, Rohr, Karl, Erfle, Holger, Kaderali, Lars, Marcotrigiano, Joseph, Pichlmair, Andreas, and Binder, Marco

Subjects

*PHOSPHORYLATION, *SMALL interfering RNA, *PROTEIN kinases, *PHYSIOLOGICAL control systems, *TYPE I interferons

Abstract

Summary Cell-autonomous induction of type I interferon must be stringently regulated. Rapid induction is key to control virus infection, whereas proper limitation of signaling is essential to prevent immunopathology and autoimmune disease. Using unbiased kinome-wide RNAi screening followed by thorough validation, we identified 22 factors that regulate RIG-I/IRF3 signaling activity. We describe a negative-feedback mechanism targeting RIG-I activity, which is mediated by death associated protein kinase 1 (DAPK1). RIG-I signaling triggers DAPK1 kinase activation, and active DAPK1 potently inhibits RIG-I stimulated IRF3 activity and interferon-beta production. DAPK1 phosphorylates RIG-I in vitro at previously reported as well as other sites that limit 5′ppp-dsRNA sensing and virtually abrogate RIG-I activation. [ABSTRACT FROM AUTHOR]

Published

2017

6. Early host defense against virus infections.

Author

Paludan SR, Pradeu T, Pichlmair A, Wray KB, Mikkelsen JG, Olagnier D, and Mogensen TH

Subjects

Humans, Animals, Inflammation immunology, Inflammation pathology, Host-Pathogen Interactions immunology, Virus Replication, Viruses immunology, Viruses pathogenicity, Virus Diseases immunology, Immunity, Innate

Abstract

Early host defense eliminates many viruses before infections are established while clearing others so they remain subclinical or cause only mild disease. The field of immunology has been shaped by broad concepts, including the pattern recognition theory that currently dominates innate immunology. Focusing on early host responses to virus infections, we analyze the literature to build a working hypothesis for the principles that govern the early line of cellular antiviral defense. Aiming to ultimately arrive at a criteria-based theory with strong explanatory power, we propose that both controlling infection and limiting inflammation are key drivers for the early cellular antiviral response. This response, which we suggest is exerted by a set of "microbe- and inflammation-restricting mechanisms," directly restrict viral replication while also counteracting inflammation. Exploring the mechanisms and physiological importance of the early layer of cellular antiviral defense may open further lines of research in immunology., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2024 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2024

7. Dengue virus and Zika virus alter endoplasmic reticulum-mitochondria contact sites to regulate respiration and apoptosis.

Author

Freppel W, Barragan Torres VA, Uyar O, Anton A, Nouhi Z, Broquière M, Mazeaud C, Sow AA, Léveillé A, Gilbert C, Tremblay N, Owen JE, Bemis CL, Laulhé X, Lamarre A, Neufeldt CJ, Rodrigue-Gervais IG, Pichlmair A, Girard D, Scaturro P, Hulea L, and Chatel-Chaix L

Abstract

During infection, dengue virus (DENV) and Zika virus (ZIKV), two (ortho)flaviviruses of public health concern worldwide, induce alterations of mitochondria morphology to favor viral replication, suggesting a viral co-opting of mitochondria functions. Here, we performed an extensive transmission electron microscopy-based quantitative analysis to demonstrate that both DENV and ZIKV alter endoplasmic reticulum-mitochondria contact sites (ERMC). This correlated at the molecular level with an impairment of ERMC tethering protein complexes located at the surface of both organelles. Furthermore, virus infection modulated the mitochondrial oxygen consumption rate. Consistently, metabolomic and mitoproteomic analyses revealed a decrease in the abundance of several metabolites of the Krebs cycle and changes in the stoichiometry of the electron transport chain. Most importantly, ERMC destabilization by protein knockdown increased virus replication while dampening ZIKV-induced apoptosis. Overall, our results support the notion that flaviviruses hijack ERMCs to generate a cytoplasmic environment beneficial for sustained and efficient replication., Competing Interests: The authors declare that they have no conflicts of interest., (© 2024 The Author(s).)

Published

2024

8. Protein turnover regulation is critical for influenza A virus infection.

Author

Huang Y, Urban C, Hubel P, Stukalov A, and Pichlmair A

Subjects

Humans, Isotope Labeling, Host-Pathogen Interactions, A549 Cells, Madin Darby Canine Kidney Cells, HEK293 Cells, Influenza A virus, Influenza, Human metabolism, Influenza, Human virology, Virus Replication

Abstract

The abundance of a protein is defined by its continuous synthesis and degradation, a process known as protein turnover. Here, we systematically profiled the turnover of proteins in influenza A virus (IAV)-infected cells using a pulse-chase stable isotope labeling by amino acids in cell culture (SILAC)-based approach combined with downstream statistical modeling. We identified 1,798 virus-affected proteins with turnover changes (tVAPs) out of 7,739 detected proteins (data available at pulsechase.innatelab.org). In particular, the affected proteins were involved in RNA transcription, splicing and nuclear transport, protein translation and stability, and energy metabolism. Many tVAPs appeared to be known IAV-interacting proteins that regulate virus propagation, such as KPNA6, PPP6C, and POLR2A. Notably, our analysis identified additional IAV host and restriction factors, such as the splicing factor GPKOW, that exhibit significant turnover rate changes while their total abundance is minimally affected. Overall, we show that protein turnover is a critical factor both for virus replication and antiviral defense., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2024 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2024

9. SND1 binds SARS-CoV-2 negative-sense RNA and promotes viral RNA synthesis through NSP9.

Author

Schmidt N, Ganskih S, Wei Y, Gabel A, Zielinski S, Keshishian H, Lareau CA, Zimmermann L, Makroczyova J, Pearce C, Krey K, Hennig T, Stegmaier S, Moyon L, Horlacher M, Werner S, Aydin J, Olguin-Nava M, Potabattula R, Kibe A, Dölken L, Smyth RP, Caliskan N, Marsico A, Krempl C, Bodem J, Pichlmair A, Carr SA, Chlanda P, Erhard F, and Munschauer M

Subjects

Humans, Endonucleases metabolism, SARS-CoV-2 genetics, Virus Replication, COVID-19 metabolism, RNA, Viral metabolism

Abstract

Regulation of viral RNA biogenesis is fundamental to productive SARS-CoV-2 infection. To characterize host RNA-binding proteins (RBPs) involved in this process, we biochemically identified proteins bound to genomic and subgenomic SARS-CoV-2 RNAs. We find that the host protein SND1 binds the 5' end of negative-sense viral RNA and is required for SARS-CoV-2 RNA synthesis. SND1-depleted cells form smaller replication organelles and display diminished virus growth kinetics. We discover that NSP9, a viral RBP and direct SND1 interaction partner, is covalently linked to the 5' ends of positive- and negative-sense RNAs produced during infection. These linkages occur at replication-transcription initiation sites, consistent with NSP9 priming viral RNA synthesis. Mechanistically, SND1 remodels NSP9 occupancy and alters the covalent linkage of NSP9 to initiating nucleotides in viral RNA. Our findings implicate NSP9 in the initiation of SARS-CoV-2 RNA synthesis and unravel an unsuspected role of a cellular protein in orchestrating viral RNA production., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2023 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2023

10. SARS-CoV-2 CD8 + T cell killing assays using replicating viruses and transgenic antigens.

Author

Mateyka LM, Grass V, Pichlmair A, Busch DH, and D'Ippolito E

Subjects

Animals, CD8-Positive T-Lymphocytes, Antigen Presentation, Animals, Genetically Modified, Cell Death, SARS-CoV-2, COVID-19

Abstract

The quality of an antigen-specific CD8 + T cell repertoire is crucial for the clearance of intracellular pathogens, in particular for viral infections. Here, we describe killing assays to determine the function of CD8 + T cells engineered with SARS-CoV-2-specific T cell receptors in a near-physiological system for antigen presentation. We detail the use of target cells either infected with replicating SARS-CoV-2 virus or engineered with SARS-CoV-2 open reading frames. For complete details on the use and execution of this protocol, please refer to Moosmann et al. (2022) and Wagner et al. (2022)., Competing Interests: Declaration of interests D.H.B. is co-founder of STAGE Cell Therapeutics GmbH (now Juno Therapeutics, a Bristol-Myers Squibb Company) and T cell Factory B.V. (now Kite, a Gilead Company). D.H.B. has a consulting contract with and receives sponsored research support from Juno Therapeutics. D.H.B. is member of the Scientific Board of Immatics. All other authors declare no competing interests., (Copyright © 2022 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2022

11. Recruitment of highly cytotoxic CD8 + T cell receptors in mild SARS-CoV-2 infection.

Author

Wagner KI, Mateyka LM, Jarosch S, Grass V, Weber S, Schober K, Hammel M, Burrell T, Kalali B, Poppert H, Beyer H, Schambeck S, Holdenrieder S, Strötges-Achatz A, Haselmann V, Neumaier M, Erber J, Priller A, Yazici S, Roggendorf H, Odendahl M, Tonn T, Dick A, Witter K, Mijočević H, Protzer U, Knolle PA, Pichlmair A, Crowell CS, Gerhard M, D'Ippolito E, and Busch DH

Subjects

Adult, Cells, Cultured, Cross Reactions immunology, Epitopes, T-Lymphocyte immunology, Female, Humans, Immunodominant Epitopes immunology, Leukocytes, Mononuclear immunology, Leukocytes, Mononuclear virology, Male, Spike Glycoprotein, Coronavirus immunology, T-Lymphocytes, Cytotoxic immunology, CD8-Positive T-Lymphocytes immunology, COVID-19 immunology, Receptors, Antigen, T-Cell immunology, SARS-CoV-2 immunology

Abstract

T cell immunity is crucial for control of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection and has been studied widely on a quantitative level. However, the quality of responses, in particular of CD8 + T cells, has only been investigated marginally so far. Here, we isolate T cell receptor (TCR) repertoires specific for immunodominant SARS-CoV-2 epitopes restricted to common human Leukocyte antigen (HLA) class I molecules in convalescent individuals. SARS-CoV-2-specific CD8 + T cells are detected up to 12 months after infection. TCR repertoires are diverse, with heterogeneous functional avidity and cytotoxicity toward virus-infected cells, as demonstrated for TCR-engineered T cells. High TCR functionality correlates with gene signatures that, remarkably, could be retrieved for each epitope:HLA combination analyzed. Overall, our data demonstrate that polyclonal and highly functional CD8 + TCRs-classic features of protective immunity-are recruited upon mild SARS-CoV-2 infection, providing tools to assess the quality of and potentially restore functional CD8 + T cell immunity., Competing Interests: Declaration of interests D.H.B. is co-founder of STAGE Cell Therapeutics GmbH (now Juno Therapeutics/Celgene) and T cell Factory B.V. (now Kite/Gilead). D.H.B. has a consulting contract with and receives sponsored research support from Juno Therapeutics, a Bristol Myers Squibb Company., (Copyright © 2021 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2022

12. Nuclear-localized human respiratory syncytial virus NS1 protein modulates host gene transcription.

Author

Pei J, Beri NR, Zou AJ, Hubel P, Dorando HK, Bergant V, Andrews RD, Pan J, Andrews JM, Sheehan KCF, Pichlmair A, Amarasinghe GK, Brody SL, Payton JE, and Leung DW

Subjects

A549 Cells, Animals, Binding Sites, Cell Nucleus virology, Chromatin genetics, Chromatin virology, Dendritic Cells virology, Epithelial Cells virology, Female, HEK293 Cells, Host-Pathogen Interactions, Humans, Lung virology, Mediator Complex genetics, Mediator Complex metabolism, Mice, Inbred BALB C, Promoter Regions, Genetic, Respiratory Syncytial Virus Infections genetics, Respiratory Syncytial Virus Infections virology, Respiratory Syncytial Virus, Human genetics, Respiratory Syncytial Virus, Human pathogenicity, Viral Nonstructural Proteins genetics, Mice, Cell Nucleus metabolism, Chromatin metabolism, Dendritic Cells metabolism, Epithelial Cells metabolism, Lung metabolism, Respiratory Syncytial Virus Infections metabolism, Respiratory Syncytial Virus, Human metabolism, Transcription, Genetic, Viral Nonstructural Proteins metabolism

Abstract

Human respiratory syncytial virus (RSV) is a common cause of lower respiratory tract infections in the pediatric, elderly, and immunocompromised individuals. RSV non-structural protein NS1 is a known cytosolic immune antagonist, but how NS1 modulates host responses remains poorly defined. Here, we observe NS1 partitioning into the nucleus of RSV-infected cells, including the human airway epithelium. Nuclear NS1 coimmunoprecipitates with Mediator complex and is chromatin associated. Chromatin-immunoprecipitation demonstrates enrichment of NS1 that overlaps Mediator and transcription factor binding within the promoters and enhancers of differentially expressed genes during RSV infection. Mutation of the NS1 C-terminal helix reduces NS1 impact on host gene expression. These data suggest that nuclear NS1 alters host responses to RSV infection by binding at regulatory elements of immune response genes and modulating host gene transcription. Our study identifies another layer of regulation by virally encoded proteins that shapes host response and impacts immunity to RSV., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2021 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2021

13. A Comprehensive Analysis of the Dynamic Response to Aphidicolin-Mediated Replication Stress Uncovers Targets for ATM and ATMIN.

Author

Mazouzi A, Stukalov A, Müller AC, Chen D, Wiedner M, Prochazkova J, Chiang SC, Schuster M, Breitwieser FP, Pichlmair A, El-Khamisy SF, Bock C, Kralovics R, Colinge J, Bennett KL, and Loizou JI

Abstract

The cellular response to replication stress requires the DNA-damage-responsive kinase ATM and its cofactor ATMIN; however, the roles of this signaling pathway following replication stress are unclear. To identify the functions of ATM and ATMIN in response to replication stress, we utilized both transcriptomics and quantitative mass-spectrometry-based phosphoproteomics. We found that replication stress induced by aphidicolin triggered widespread changes in both gene expression and protein phosphorylation patterns. These changes gave rise to distinct early and late replication stress responses. Furthermore, our analysis revealed previously unknown targets of ATM and ATMIN downstream of replication stress. We demonstrate ATMIN-dependent phosphorylation of H2AX and of CRMP2, a protein previously implicated in Alzheimer's disease but not in the DNA damage response. Overall, our dataset provides a comprehensive resource for discovering the cellular responses to replication stress and, potentially, associated pathologies., (Copyright © 2016 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2016

14. The Lipid-Modifying Enzyme SMPDL3B Negatively Regulates Innate Immunity.

Author

Heinz LX, Baumann CL, Köberlin MS, Snijder B, Gawish R, Shui G, Sharif O, Aspalter IM, Müller AC, Kandasamy RK, Breitwieser FP, Pichlmair A, Bruckner M, Rebsamen M, Blüml S, Karonitsch T, Fauster A, Colinge J, Bennett KL, Knapp S, Wenk MR, and Superti-Furga G

Subjects

Animals, Cyclic Nucleotide Phosphodiesterases, Type 3 immunology, Disease Models, Animal, Humans, Inflammation immunology, Inflammation pathology, Lipids immunology, Macrophages immunology, Mice, Peritonitis immunology, Peritonitis pathology, Toll-Like Receptors genetics, Toll-Like Receptors immunology, Cyclic Nucleotide Phosphodiesterases, Type 3 genetics, Immunity, Innate genetics, Inflammation genetics, Peritonitis genetics

Abstract

Lipid metabolism and receptor-mediated signaling are highly intertwined processes that cooperate to fulfill cellular functions and safeguard cellular homeostasis. Activation of Toll-like receptors (TLRs) leads to a complex cellular response, orchestrating a diverse range of inflammatory events that need to be tightly controlled. Here, we identified the GPI-anchored Sphingomyelin Phosphodiesterase, Acid-Like 3B (SMPDL3B) in a mass spectrometry screening campaign for membrane proteins co-purifying with TLRs. Deficiency of Smpdl3b in macrophages enhanced responsiveness to TLR stimulation and profoundly changed the cellular lipid composition and membrane fluidity. Increased cellular responses could be reverted by re-introducing affected ceramides, functionally linking membrane lipid composition and innate immune signaling. Finally, Smpdl3b-deficient mice displayed an intensified inflammatory response in TLR-dependent peritonitis models, establishing its negative regulatory role in vivo. Taken together, our results identify the membrane-modulating enzyme SMPDL3B as a negative regulator of TLR signaling that functions at the interface of membrane biology and innate immunity., (Copyright © 2015 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2015

15. RIG-I detects viral genomic RNA during negative-strand RNA virus infection.

Author

Rehwinkel J, Tan CP, Goubau D, Schulz O, Pichlmair A, Bier K, Robb N, Vreede F, Barclay W, Fodor E, and Reis e Sousa C

Subjects

Animals, Cell Line, DEAD Box Protein 58, Dogs, Humans, Interferons immunology, Mice, RNA Viruses physiology, Receptors, Cell Surface, Receptors, Immunologic, Virus Replication, DEAD-box RNA Helicases immunology, Membrane Proteins immunology, Nerve Tissue Proteins immunology, RNA Virus Infections immunology, RNA, Viral immunology

Abstract

RIG-I is a key mediator of antiviral immunity, able to couple detection of infection by RNA viruses to the induction of interferons. Natural RIG-I stimulatory RNAs have variously been proposed to correspond to virus genomes, virus replication intermediates, viral transcripts, or self-RNA cleaved by RNase L. However, the relative contribution of each of these RNA species to RIG-I activation and interferon induction in virus-infected cells is not known. Here, we use three approaches to identify physiological RIG-I agonists in cells infected with influenza A virus or Sendai virus. We show that RIG-I agonists are exclusively generated by the process of virus replication and correspond to full-length virus genomes. Therefore, nongenomic viral transcripts, short replication intermediates, and cleaved self-RNA do not contribute substantially to interferon induction in cells infected with these negative strand RNA viruses. Rather, single-stranded RNA viral genomes bearing 5'-triphosphates constitute the natural RIG-I agonists that trigger cell-intrinsic innate immune responses during infection., (2010 Elsevier Inc. All rights reserved.)

Published

2010