Your search keyword '"Lukacher AE"' showing total 82 results

1. Brincidofovir inhibits polyomavirus infection in vivo .

Author

Butic AB, Katz ZE, Jin G, Fukushima K, Hazama M, Lukacher AE, and Lauver MD

Subjects

Animals, Mice, Virus Replication drug effects, Kidney virology, Kidney drug effects, Female, DNA, Viral genetics, Cells, Cultured, Disease Models, Animal, Mice, Inbred C57BL, Brain virology, Cytosine analogs & derivatives, Cytosine pharmacology, Cytosine therapeutic use, Polyomavirus Infections drug therapy, Polyomavirus Infections virology, Polyomavirus drug effects, Antiviral Agents pharmacology, Antiviral Agents therapeutic use, Organophosphonates pharmacology, Organophosphonates therapeutic use

Abstract

Polyomaviruses are species-specific DNA viruses that can cause disease in immunocompromised individuals. Despite their role as the causative agents for several diseases, there are no currently approved antivirals for treating polyomavirus infection. Brincidofovir (BCV) is an antiviral approved for the treatment of poxvirus infections and has shown activity against other double-stranded DNA viruses. In this study, we tested the efficacy of BCV against polyomavirus infection in vitro and in vivo using mouse polyomavirus (MuPyV). BCV inhibited virus production in primary mouse kidney cells and brain cortical cells. BCV treatment of cells transfected with MuPyV genomic DNA resulted in a reduction in virus levels, indicating that viral inhibition occurs post-entry. Although in vitro BCV treatment had a limited effect on viral DNA and RNA levels, drug treatment was associated with a reduction in viral protein, raising the possibility that BCV acts post-transcriptionally to inhibit MuPyV infection. In mice, BCV treatment was well tolerated, and prophylactic treatment resulted in a reduction in viral DNA levels and a potent suppression of infectious virus production in the kidney and brain. In mice with chronic polyomavirus infection, therapeutic administration of BCV decreased viremia and reduced infection in the kidney. These data demonstrate that BCV exerts antiviral activity against polyomavirus infection in vivo , supporting further investigation into the use of BCV to treat clinical polyomavirus infections., Importance: Widespread in the human population and able to persist asymptomatically for the life of an individual, polyomavirus infections cause a significant disease burden in the immunocompromised. Individuals undergoing immune suppression, such as kidney transplant patients or those treated for autoimmune diseases, are particularly at high risk for polyomavirus-associated diseases. Because no antiviral agent exists for treating polyomavirus infections, management of polyomavirus-associated diseases typically involves reducing or discontinuing immunomodulatory therapy. This can be perilous due to the risk of transplant rejection and the potential development of adverse immune reactions. Thus, there is a pressing need for the development of antivirals targeting polyomaviruses. Here, we investigate the effects of brincidofovir, an FDA-approved antiviral, on polyomavirus infection in vivo using mouse polyomavirus. We show that the drug is well-tolerated in mice, reduces infectious viral titers, and limits viral pathology, indicating the potential of brincidofovir as an anti-polyomavirus therapeutic., Competing Interests: K.F. and M.H. are employees of Symbio, which owns the license to BCV.

Published

2024

2. Polyomavirus Wakes Up and Chooses Neurovirulence.

Author

Butic AB, Spencer SA, Shaheen SK, and Lukacher AE

Subjects

Humans, Animals, Mice, Polyomavirus, Leukoencephalopathy, Progressive Multifocal, JC Virus, Polyomavirus Infections, Brain Diseases

Abstract

JC polyomavirus (JCPyV) is a human-specific polyomavirus that establishes a silent lifelong infection in multiple peripheral organs, predominantly those of the urinary tract, of immunocompetent individuals. In immunocompromised settings, however, JCPyV can infiltrate the central nervous system (CNS), where it causes several encephalopathies of high morbidity and mortality. JCPyV-induced progressive multifocal leukoencephalopathy (PML), a devastating demyelinating brain disease, was an AIDS-defining illness before antiretroviral therapy that has "reemerged" as a complication of immunomodulating and chemotherapeutic agents. No effective anti-polyomavirus therapeutics are currently available. How depressed immune status sets the stage for JCPyV resurgence in the urinary tract, how the virus evades pre-existing antiviral antibodies to become viremic, and where/how it enters the CNS are incompletely understood. Addressing these questions requires a tractable animal model of JCPyV CNS infection. Although no animal model can replicate all aspects of any human disease, mouse polyomavirus (MuPyV) in mice and JCPyV in humans share key features of peripheral and CNS infection and antiviral immunity. In this review, we discuss the evidence suggesting how JCPyV migrates from the periphery to the CNS, innate and adaptive immune responses to polyomavirus infection, and how the MuPyV-mouse model provides insights into the pathogenesis of JCPyV CNS disease.

Published

2023

3. Merkel Cell Polyomavirus Large T Antigen Induces Cellular Senescence for Host Growth Arrest and Viral Genome Persistence through Its Unique Domain.

Author

Pham AM, Ortiz LE, Lukacher AE, and Kwun HJ

Subjects

Humans, Antigens, Viral, Tumor genetics, Cellular Senescence, Genome, Viral, Polyomavirus Infections genetics, Tumor Virus Infections genetics, Tumor Virus Infections pathology, Merkel cell polyomavirus genetics, Merkel cell polyomavirus metabolism, Carcinoma, Merkel Cell genetics, Carcinoma, Merkel Cell pathology, Skin Neoplasms pathology

Abstract

Senescent cells accumulate in the host during the aging process and are associated with age-related pathogeneses, including cancer. Although persistent senescence seems to contribute to many aspects of cellular pathways and homeostasis, the role of senescence in virus-induced human cancer is not well understood. Merkel cell carcinoma (MCC) is an aggressive skin cancer induced by a life-long human infection of Merkel cell polyomavirus (MCPyV). Here, we show that MCPyV large T (LT) antigen expression in human skin fibroblasts causes a novel nucleolar stress response, followed by p21-dependent senescence and senescence-associated secretory phenotypes (SASPs), which are required for MCPyV genome maintenance. Senolytic and navitoclax treatments result in decreased senescence and MCPyV genome levels, suggesting a potential therapeutic for MCC prevention. Our results uncover the mechanism of a host stress response regulating human polyomavirus genome maintenance in viral persistency, which may lead to targeted intervention for MCC.

Published

2023

4. T cell deficiency precipitates antibody evasion and emergence of neurovirulent polyomavirus.

Author

Lauver MD, Jin G, Ayers KN, Carey SN, Specht CS, Abendroth CS, and Lukacher AE

Subjects

Animals, Mice, Antibodies, Neutralizing, Polyomavirus genetics, Immunologic Deficiency Syndromes, JC Virus genetics, Leukoencephalopathy, Progressive Multifocal

Abstract

JC polyomavirus (JCPyV) causes progressive multifocal leukoencephalopathy (PML), a life-threatening brain disease in immunocompromised patients. Inherited and acquired T cell deficiencies are associated with PML. The incidence of PML is increasing with the introduction of new immunomodulatory agents, several of which target T cells or B cells. PML patients often carry mutations in the JCPyV VP1 capsid protein, which confer resistance to neutralizing VP1 antibodies (Ab). Polyomaviruses (PyV) are tightly species-specific; the absence of tractable animal models has handicapped understanding PyV pathogenesis. Using mouse polyomavirus (MuPyV), we found that T cell deficiency during persistent infection, in the setting of monospecific VP1 Ab, was required for outgrowth of VP1 Ab-escape viral variants. CD4 T cells were primarily responsible for limiting polyomavirus infection in the kidney, a major reservoir of persistent infection by both JCPyV and MuPyV, and checking emergence of these mutant viruses. T cells also provided a second line of defense by controlling the outgrowth of VP1 mutant viruses that evaded Ab neutralization. A virus with two capsid mutations, one conferring Ab-escape yet impaired infectivity and a second compensatory mutation, yielded a highly neurovirulent variant. These findings link T cell deficiency and evolution of Ab-escape polyomavirus VP1 variants with neuropathogenicity., Competing Interests: ML, GJ, KA, SC, CS, CA, AL No competing interests declared, (© 2022, Lauver et al.)

Published

2022

5. Understanding polyomavirus CNS disease - a perspective from mouse models.

Author

Ayers KN, Carey SN, and Lukacher AE

Subjects

Animals, Disease Models, Animal, Humans, Immunomodulating Agents, Mice, Natalizumab therapeutic use, Biological Products therapeutic use, JC Virus genetics, Leukoencephalopathy, Progressive Multifocal drug therapy, Polyomavirus

Abstract

JC polyomavirus (JCPyV), a ubiquitous human pathogen, causes several devastating brain diseases in immune-compromised individuals. The most notable of these JCPyV-associated CNS diseases is the frequently fatal demyelinating brain disease progressive multifocal leukoencephalopathy (PML). PML, an AIDS-defining disease in the pre-cART epoch, has emerged as a life-threatening complication in patients receiving immunomodulatory agents for autoimmune and inflammatory disorders and treatment for certain hematological malignancies. Among the rapidly expanding list of PML-associated biologics, natalizumab (Tysabri®) has the highest incidence and is an ominous sequela for multiple sclerosis (MS) patients who otherwise benefit from dramatic reductions in relapses using this immunomodulatory agent. Drug withdrawal, the only therapeutic option for PML, is often complicated by a high-mortality cerebral inflammatory reaction. No anti-JCPyV agents are available. Lack of a tractable animal model of polyomavirus-induced central nervous system (CNS) disease is an acknowledged bottleneck to elucidating PML pathogenesis, immunological mechanisms that control JCPyV, in vivo evaluation of agents that inhibit polyomavirus replication in tissue culture, and uncovering early events that presage JCPyV-associated neuropathology. The natural virus-host mouse polyomavirus (MuPyV) model has recently been developed to explore mechanisms of polyomavirus-associated CNS disease. In this review, we will cover the benefits of using the MuPyV model to answer fundamental questions about innate and adaptive immune control of JCPyV, the impact of immunomodulation on JCPyV pathogenesis, and how this MuPyV CNS infection model will help improve criteria for identifying patients at risk for JCPyV-associated CNS diseases before the development of irreversible lesions., (© 2021 Federation of European Biochemical Societies.)

Published

2022

6. New developments implicating IL-21 in autoimmune disease.

Author

Ren HM, Lukacher AE, Rahman ZSM, and Olsen NJ

Subjects

Animals, Autoimmune Diseases blood, Cell Differentiation immunology, Disease Models, Animal, Humans, Immunologic Memory, Receptors, Interleukin-21 metabolism, Signal Transduction immunology, T Follicular Helper Cells metabolism, Autoimmune Diseases immunology, CD8-Positive T-Lymphocytes immunology, Interleukins metabolism, T Follicular Helper Cells immunology

Abstract

Elevated interleukin (IL)-21 is a common finding in the tissues and/or sera of patients with autoimmune disease. CD4 T cells are the primary producers of IL-21; often the IL-21 producing CD4 T cells will express molecules associated with follicular helper cells (T FH ). Recent work has shown that the CD4 T cell-derived IL-21 is able to promote effector functions and memory differentiation of CD8 T cells in chronic infections and cancer. Autoimmunity has similarities to chronic infections and cancer. However, CD4 T cell-derived IL-21:IL21R signaling in CD8 T cells has not been fully appreciated in the context of autoimmunity. In this review, we assess the current knowledge regarding CD4 T cell-derived IL-21 and IL21R signaling within CD8 T cells and evaluate what implications it has within several autoimmune diseases including systemic lupus erythematous, rheumatoid arthritis, juvenile idiopathic arthritis, type 1 diabetes mellitus, psoriasis, Sjögren's syndrome, vitiligo, antiphospholipid syndrome, pemphigus, and giant cell arteritis., (Copyright © 2021 Elsevier Ltd. All rights reserved.)

Published

2021

7. Balancing Inflammation and Central Nervous System Homeostasis: T Cell Receptor Signaling in Antiviral Brain T RM Formation and Function.

Author

Netherby-Winslow CS, Ayers KN, and Lukacher AE

Subjects

Animals, Brain pathology, Brain virology, CD8-Positive T-Lymphocytes pathology, Central Nervous System Viral Diseases pathology, Central Nervous System Viral Diseases virology, Humans, Immunologic Memory, Inflammation immunology, Inflammation pathology, Inflammation virology, Brain immunology, CD8-Positive T-Lymphocytes immunology, Central Nervous System Viral Diseases immunology, Lymphocyte Activation, Receptors, Antigen, T-Cell immunology, Signal Transduction immunology, Viruses immunology

Abstract

Tissue-resident memory (T RM ) CD8 T cells provide early frontline defense against regional pathogen reencounter. CD8 T RM are predominantly parked in nonlymphoid tissues and do not circulate. In addition to this anatomic difference, T RM are transcriptionally and phenotypically distinct from central-memory T cells (T CM ) and effector-memory T cells (T EM ). Moreover, T RM differ phenotypically, functionally, and transcriptionally across barrier tissues (e.g., gastrointestinal tract, respiratory tract, urogenital tract, and skin) and in non-barrier organs (e.g., brain, liver, kidney). In the brain, T RM are governed by a contextual milieu that balances T RM activation and preservation of essential post-mitotic neurons. Factors contributing to the development and maintenance of brain T RM , of which T cell receptor (TCR) signal strength and duration is a central determinant, vary depending on the infectious agent and modulation of TCR signaling by inhibitory markers that quell potentially pathogenic inflammation. This review will explore our current understanding of the context-dependent factors that drive the acquisition of brain (b)T RM phenotype and function, and discuss the contribution of T RM to promoting protective immune responses in situ while maintaining tissue homeostasis., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Netherby-Winslow, Ayers and Lukacher.)

Published

2021

8. JCPyV VP1 Mutations in Progressive MultifocalLeukoencephalopathy: Altering Tropismor Mediating Immune Evasion?

Author

Lauver MD and Lukacher AE

Subjects

Animals, Capsid immunology, Capsid Proteins immunology, Host Specificity genetics, Humans, Immune Evasion immunology, Leukoencephalopathy, Progressive Multifocal genetics, Leukoencephalopathy, Progressive Multifocal virology, Mice, Mutation, Viral Tropism genetics, Virus Replication genetics, Capsid Proteins genetics, Immune Evasion genetics, JC Virus genetics, JC Virus immunology, Leukoencephalopathy, Progressive Multifocal immunology

Abstract

Polyomaviruses are ubiquitous human pathogens that cause lifelong, asymptomatic infections in healthy individuals. Although these viruses are restrained by an intact immune system, immunocompromised individuals are at risk for developing severe diseases driven by resurgent viral replication. In particular, loss of immune control over JC polyomavirus can lead to the development of the demyelinating brain disease progressive multifocal leukoencephalopathy (PML). Viral isolates from PML patients frequently carry point mutations in the major capsid protein, VP1, which mediates virion binding to cellular glycan receptors. Because polyomaviruses are non-enveloped, VP1 is also the target of the host's neutralizing antibody response. Thus, VP1 mutations could affect tropism and/or recognition by polyomavirus-specific antibodies. How these mutations predispose susceptible individuals to PML and other JCPyV-associated CNS diseases remains to be fully elucidated. Here, we review the current understanding of polyomavirus capsid mutations and their effects on viral tropism, immune evasion, and virulence.

Published

2020

9. IL-21 in Homeostasis of Resident Memory and Exhausted CD8 T Cells during Persistent Infection.

Author

Ren HM and Lukacher AE

Subjects

Animals, B-Lymphocytes immunology, B-Lymphocytes pathology, CD8-Positive T-Lymphocytes pathology, Humans, Immunoglobulin Class Switching immunology, Infections pathology, T-Lymphocytes, Helper-Inducer immunology, T-Lymphocytes, Helper-Inducer pathology, CD8-Positive T-Lymphocytes immunology, Immunologic Memory, Infections immunology, Interleukins immunology

Abstract

CD4 T cells guide the development of CD8 T cells into memory by elaborating mitogenic and differentiation factors and by licensing professional antigen-presenting cells. CD4 T cells also act to stave off CD8 T cell dysfunction during repetitive antigen stimulation in persistent infection and cancer by mitigating generation of exhausted T cells (T EX ). CD4 T cell help is also required for establishing and maintaining tissue-resident memory T cells (T RM ), the nonrecirculating memory T cell subset parked in nonlymphoid tissues to provide frontline defense against reinvading pathogens. Interleukin (IL)-21 is the signature cytokine secreted by follicular helper CD4 T cells (T FH ) to drive B cell expansion and differentiation in germinal centers to mount high-affinity, isotype class-switched antibodies. In several infection models, IL-21 has been identified as the CD4 T help needed for formation and survival of T RM and T EX . In this review, we will explore the different memory subsets of CD8 T cells in persistent infections, the metabolic profiles associated with each, and evidence documenting the importance of CD4 T cell-derived IL-21 in regulating CD8 T RM and T EX development, homeostasis, and function.

Published

2020

10. IL-21 from high-affinity CD4 T cells drives differentiation of brain-resident CD8 T cells during persistent viral infection.

Author

Ren HM, Kolawole EM, Ren M, Jin G, Netherby-Winslow CS, Wade Q, Shwetank, Rahman ZSM, Evavold BD, and Lukacher AE

Subjects

Animals, Brain cytology, Cell Differentiation, Cytokines immunology, Interleukins genetics, Mice, Inbred C57BL, Mice, Knockout, Spleen immunology, Brain immunology, CD4-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes immunology, Interleukins immunology, Polyomavirus, Polyomavirus Infections immunology, Tumor Virus Infections immunology

Abstract

Development of tissue-resident memory (T RM ) CD8 T cells depends on CD4 T cells. In polyomavirus central nervous system infection, brain CXCR5 hi PD-1 hi CD4 T cells produce interleukin-21 (IL-21), and CD8 T cells lacking IL-21 receptors (IL21R -/- ) fail to become bT RM IL-21 + CD4 T cells exhibit elevated T cell receptor (TCR) affinity and higher TCR density. IL21R -/- brain CD8 T cells do not express CD103, depend on vascular CD8 T cells for maintenance, are antigen recall defective, and lack T RM core signature genes. CD4 T cell-deficient and IL21R -/- brain CD8 T cells show similar deficiencies in expression of genes for oxidative metabolism, and intrathecal delivery of IL-21 to CD4 T cell-depleted mice restores expression of electron transport genes in CD8 T cells to wild-type levels. Thus, high-affinity CXCR5 hi PD-1 hi CD4 T cells in the brain produce IL-21, which drives CD8 bT RM differentiation in response to a persistent viral infection., (Copyright © 2020 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works.)

Published

2020

11. Antibody escape by polyomavirus capsid mutation facilitates neurovirulence.

Author

Lauver MD, Goetschius DJ, Netherby-Winslow CS, Ayers KN, Jin G, Haas DG, Frost EL, Cho SH, Bator CM, Bywaters SM, Christensen ND, Hafenstein SL, and Lukacher AE

Subjects

Animals, Female, Leukoencephalopathy, Progressive Multifocal immunology, Male, Mice, Mice, Inbred C57BL, Polyomavirus immunology, Virulence, Antibodies, Monoclonal immunology, Capsid immunology, Mutation, Polyomavirus pathogenicity

Abstract

JCPyV polyomavirus, a member of the human virome, causes progressive multifocal leukoencephalopathy (PML), an oft-fatal demyelinating brain disease in individuals receiving immunomodulatory therapies. Mutations in the major viral capsid protein, VP1, are common in JCPyV from PML patients (JCPyV-PML) but whether they confer neurovirulence or escape from virus-neutralizing antibody (nAb) in vivo is unknown. A mouse polyomavirus (MuPyV) with a sequence-equivalent JCPyV-PML VP1 mutation replicated poorly in the kidney, a major reservoir for JCPyV persistence, but retained the CNS infectivity, cell tropism, and neuropathology of the parental virus. This mutation rendered MuPyV resistant to a monoclonal Ab (mAb), whose specificity overlapped the endogenous anti-VP1 response. Using cryo-EM and a custom sub-particle refinement approach, we resolved an MuPyV:Fab complex map to 3.2 Å resolution. The structure revealed the mechanism of mAb evasion. Our findings demonstrate convergence between nAb evasion and CNS neurovirulence in vivo by a frequent JCPyV-PML VP1 mutation., Competing Interests: ML, DG, CN, KA, GJ, DH, EF, SC, CB, SB, NC, SH, AL No competing interests declared, (© 2020, Lauver et al.)

Published

2020

12. Serine Phosphorylation of the STAT1 Transactivation Domain Promotes Autoreactive B Cell and Systemic Autoimmunity Development.

Author

Chodisetti SB, Fike AJ, Domeier PP, Schell SL, Mockus TE, Choi NM, Corradetti C, Hou B, Atkins HM, Caricchio R, Decker T, Lukacher AE, Olsen N, and Rahman ZSM

Subjects

Animals, Autoantibodies blood, Autoantigens immunology, Autoimmunity, B-Lymphocytes transplantation, Humans, Lupus Erythematosus, Systemic genetics, Mice, Mice, Inbred C57BL, Mice, Mutant Strains, Phosphorylation, Protein Domains genetics, STAT1 Transcription Factor genetics, Serine genetics, Transcriptional Activation, Transplantation Chimera, B-Lymphocytes immunology, Germinal Center immunology, Lupus Erythematosus, Systemic metabolism, STAT1 Transcription Factor metabolism, T-Lymphocytes, Helper-Inducer immunology

Abstract

Although STAT1 tyrosine-701 phosphorylation (designated STAT1-pY701) is indispensable for STAT1 function, the requirement for STAT1 serine-727 phosphorylation (designated STAT1-pS727) during systemic autoimmune and antipathogen responses remains unclear. Using autoimmune-prone B6.Sle1b mice expressing a STAT1-S727A mutant in which serine is replaced by alanine, we report in this study that STAT1-pS727 promotes autoimmune Ab-forming cell (AFC) and germinal center (GC) responses, driving autoantibody production and systemic lupus erythematosus (SLE) development. In contrast, STAT1-pS727 is not required for GC, T follicular helper cell (Tfh), and Ab responses to various foreign Ags, including pathogens. STAT1-pS727 is also not required for gut microbiota and dietary Ag-driven GC and Tfh responses in B6.Sle1b mice. By generating B cell-specific bone marrow chimeras, we demonstrate that STAT1-pS727 plays an important B cell-intrinsic role in promoting autoimmune AFC, GC, and Tfh responses, leading to SLE-associated autoantibody production. Our analysis of the TLR7-accelerated B6.Sle1b.Yaa SLE disease model expressing a STAT1-S727A mutant reveals STAT1-pS727-mediated regulation of autoimmune AFC and GC responses and lupus nephritis development. Together, we identify previously unrecognized differential regulation of systemic autoimmune and antipathogen responses by STAT1-pS727. Our data implicate STAT1-pS727 as a therapeutic target for SLE without overtly affecting STAT1-mediated protection against pathogenic infections., (Copyright © 2020 by The American Association of Immunologists, Inc.)

Published

2020

13. CD8 T Cells and STAT1 Signaling Are Essential Codeterminants in Protection from Polyomavirus Encephalopathy.

Author

Mockus TE, Netherby-Winslow CS, Atkins HM, Lauver MD, Jin G, Ren HM, and Lukacher AE

Subjects

Adaptive Immunity, Animals, Brain pathology, Brain virology, Brain Diseases pathology, Brain Diseases virology, Choroid Plexus, Disease Models, Animal, Female, Humans, Immunity, Innate, JC Virus immunology, Leukoencephalopathy, Progressive Multifocal virology, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Polyomavirus Infections mortality, Polyomavirus Infections virology, STAT1 Transcription Factor genetics, Signal Transduction, Spleen pathology, Spleen virology, Viral Load, CD8-Positive T-Lymphocytes immunology, Polyomavirus immunology, Polyomavirus Infections immunology, STAT1 Transcription Factor immunology

Abstract

JC polyomavirus (JCPyV), a human-specific virus, causes the aggressive brain-demyelinating disease progressive multifocal leukoencephalopathy (PML) in individuals with depressed immune status. The increasing incidence of PML in patients receiving immunotherapeutic and chemotherapeutic agents creates a pressing clinical need to define biomarkers to stratify PML risk and develop anti-JCPyV interventions. Mouse polyomavirus (MuPyV) CNS infection causes encephalopathology and may provide insight into JCPyV-PML pathogenesis. Type I, II, and III interferons (IFNs), which all signal via the STAT1 transcription factor, mediate innate and adaptive immune defense against a variety of viral infections. We previously reported that type I and II IFNs control MuPyV infection in non-central nervous system (CNS) organs, but their relative contributions to MuPyV control in the brain remain unknown. To this end, mice deficient in type I, II, or III IFN receptors or STAT1 were infected intracerebrally with MuPyV. We found that STAT1, but not type I, II, or III IFNs, mediated viral control during acute and persistent MuPyV encephalitis. Mice deficient in STAT1 also developed severe hydrocephalus, blood-brain barrier permeability, and increased brain infiltration by myeloid cells. CD8 T cell deficiency alone did not increase MuPyV infection and pathology in the brain. In the absence of STAT1 signaling, however, depletion of CD8 T cells resulted in lytic infection of the choroid plexus and ependymal lining, marked meningitis, and 100% mortality within 2 weeks postinfection. Collectively, these findings indicate that STAT1 signaling and CD8 T cells cocontribute to controlling MuPyV infection in the brain and CNS injury. IMPORTANCE A comprehensive understanding of JCPyV-induced PML pathogenesis is needed to define determinants that predispose patients to PML, a goal whose urgency is heightened by the lack of anti-JCPyV agents. A handicap to achieving this goal is the lack of a tractable animal model to study PML pathogenesis. Using intracerebral inoculation with MuPyV, we found that MuPyV encephalitis in wild-type mice causes an encephalopathy, which is markedly exacerbated in mice deficient in STAT1, a molecule involved in transducing signals from type I, II, and III IFN receptors. CD8 T cell deficiency compounded the severity of MuPyV neuropathology and resulted in dramatically elevated virus levels in the CNS. These findings demonstrate that STAT1 signaling and CD8 T cells concomitantly act to mitigate MuPyV-encephalopathy and control viral infection., (Copyright © 2020 American Society for Microbiology.)

Published

2020

14. To Go or Stay: The Development, Benefit, and Detriment of Tissue-Resident Memory CD8 T Cells during Central Nervous System Viral Infections.

Author

Mockus TE, Ren HM, and Lukacher AE

Subjects

Animals, Brain immunology, Central Nervous System Viral Diseases complications, Humans, CD8-Positive T-Lymphocytes immunology, Central Nervous System Viral Diseases immunology, Immunologic Memory

Abstract

CD8 T cells coordinate immune defenses against viral infections of the central nervous system (CNS). Virus-specific CD8 T cells infiltrate the CNS and differentiate into brain-resident memory CD8 T cells (CD8 bT RM ). CD8 bT RM are characterized by a lack of recirculation and expression of phenotypes and transcriptomes distinct from other CD8 T cell memory subsets. CD8 bT RM have been shown to provide durable, autonomous protection against viral reinfection and the resurgence of latent viral infections. CD8 T cells have also been implicated in the development of neural damage following viral infection, which demonstrates that the infiltration of CD8 T cells into the brain can also be pathogenic. In this review, we will explore the residency and maintenance requirements for CD8 bT RM and discuss their roles in controlling viral infections of the brain.

Published

2019

15. PD-1 Dynamically Regulates Inflammation and Development of Brain-Resident Memory CD8 T Cells During Persistent Viral Encephalitis.

Author

Shwetank, Frost EL, Mockus TE, Ren HM, Toprak M, Lauver MD, Netherby-Winslow CS, Jin G, Cosby JM, Evavold BD, and Lukacher AE

Subjects

Animals, B7-H1 Antigen genetics, B7-H1 Antigen immunology, Brain pathology, CD8-Positive T-Lymphocytes pathology, Encephalitis, Viral genetics, Encephalitis, Viral pathology, Female, Inflammation genetics, Inflammation immunology, Inflammation pathology, Mice, Mice, Knockout, Polyomavirus Infections genetics, Polyomavirus Infections pathology, Programmed Cell Death 1 Receptor genetics, Brain immunology, CD8-Positive T-Lymphocytes immunology, Encephalitis, Viral immunology, Polyomavirus immunology, Polyomavirus Infections immunology, Programmed Cell Death 1 Receptor immunology

Abstract

Programmed cell death-1 (PD-1) receptor signaling dampens the functionality of T cells faced with repetitive antigenic stimulation from chronic infections or tumors. Using intracerebral (i.c.) inoculation with mouse polyomavirus (MuPyV), we have shown that CD8 T cells establish a PD-1 hi , tissue-resident memory population in the brains (bT RM ) of mice with a low-level persistent infection. In MuPyV encephalitis, PD-L1 was expressed on infiltrating myeloid cells, microglia and astrocytes, but not on oligodendrocytes. Engagement of PD-1 on anti-MuPyV CD8 T cells limited their effector activity. NanoString gene expression analysis showed that neuroinflammation was higher in PD-L1 -/- than wild type mice at day 8 post-infection, the peak of the MuPyV-specific CD8 response. During the persistent phase of infection, however, the absence of PD-1 signaling was found to be associated with a lower inflammatory response than in wild type mice. Genetic disruption and intracerebroventricular blockade of PD-1 signaling resulted in an increase in number of MuPyV-specific CD8 bT RM and the fraction of these cells expressing CD103, the αE integrin commonly used to define tissue-resident T cells. However, PD-L1 -/- mice persistently infected with MuPyV showed impaired virus control upon i.c. re-infection with MuPyV. Collectively, these data reveal a temporal duality in PD-1-mediated regulation of MuPyV-associated neuroinflammation. PD-1 signaling limited the severity of neuroinflammation during acute infection but sustained a level of inflammation during persistent infection for maintaining control of virus re-infection.

Published

2019

16. CD4 T cells control development and maintenance of brain-resident CD8 T cells during polyomavirus infection.

Author

Mockus TE, Shwetank, Lauver MD, Ren HM, Netherby CS, Salameh T, Kawasawa YI, Yue F, Broach JR, and Lukacher AE

Subjects

Animals, Brain virology, CD4-Positive T-Lymphocytes virology, CD8-Positive T-Lymphocytes virology, Cell Differentiation, Female, Lymphocyte Depletion, Male, Mice, Mice, Inbred C57BL, Polyomavirus Infections virology, Brain immunology, CD4-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes immunology, Immunologic Memory immunology, Polyomavirus immunology, Polyomavirus Infections immunology

Abstract

Tissue-resident memory CD8 T (TRM) cells defend against microbial reinfections at mucosal barriers; determinants driving durable TRM cell responses in non-mucosal tissues, which often harbor opportunistic persistent pathogens, are unknown. JC polyomavirus (JCPyV) is a ubiquitous constituent of the human virome. With altered immunological status, JCPyV can cause the oft-fatal brain demyelinating disease progressive multifocal leukoencephalopathy (PML). JCPyV is a human-only pathogen. Using the mouse polyomavirus (MuPyV) encephalitis model, we demonstrate that CD4 T cells regulate development of functional antiviral brain-resident CD8 T cells (bTRM) and renders their maintenance refractory to systemic CD8 T cell depletion. Acquired CD4 T cell deficiency, modeled by delaying systemic CD4 T cell depletion until MuPyV-specific CD8 T cells have infiltrated the brain, impacted the stability of CD8 bTRM, impaired their effector response to reinfection, and rendered their maintenance dependent on circulating CD8 T cells. This dependence of CD8 bTRM differentiation on CD4 T cells was found to extend to encephalitis caused by vesicular stomatitis virus. Together, these findings reveal an intimate association between CD4 T cells and homeostasis of functional bTRM to CNS viral infection., Competing Interests: The authors have declared that no competing interests exist.

Published

2018

17. Combined sublethal irradiation and agonist anti-CD40 enhance donor T cell accumulation and control of autochthonous murine pancreatic tumors.

Author

Ward-Kavanagh LK, Kokolus KM, Cooper TK, Lukacher AE, and Schell TD

Subjects

Adoptive Transfer, Animals, Female, Male, Mice, Mice, Inbred C57BL, Pancreatic Neoplasms immunology, Pancreatic Neoplasms pathology, Tissue Donors, Antibodies, Monoclonal therapeutic use, CD40 Antigens immunology, CD8-Positive T-Lymphocytes immunology, Chemoradiotherapy, Lymphocyte Activation immunology, Pancreatic Neoplasms therapy, Whole-Body Irradiation

Abstract

Tumor-reactive T lymphocytes can promote the regression of established tumors. However, their efficacy is often limited by immunosuppressive mechanisms that block T cell accumulation or function. ACT provides the opportunity to ameliorate immune suppression prior to transfer of tumor-reactive T cells to improve the therapeutic benefit. We evaluated the combination of lymphodepleting whole body irradiation (WBI) and agonist anti-CD40 (αCD40) antibody on control of established autochthonous murine neuroendocrine pancreatic tumors following the transfer of naïve tumor-specific CD8 T cells. Sublethal WBI had little impact on disease outcome but did promote T cell persistence in the lymphoid organs. Host conditioning with αCD40, an approach known to enhance APC function and T cell expansion, transiently increased donor T cell accumulation in the lymphoid organs and pancreas, but failed to control tumor progression. In contrast, combined WBI and αCD40 prolonged T cell proliferation and dramatically enhanced accumulation of donor T cells in both the lymphoid organs and pancreas. This dual conditioning approach also promoted high levels of inflammation in the pancreas and tumor, induced histological regression of established tumors, and extended the lifespan of treated mice. Prolonged survival was entirely dependent upon adoptive transfer, but only partially dependent upon IFNγ production by donor T cells. Our results identify the novel combination of two clinically relevant host conditioning approaches that synergize to overcome immune suppression and drive strong tumor-specific T cell accumulation within well-established tumors.

Published

2018

18. Inhibition of Retrograde Transport Limits Polyomavirus Infection In Vivo .

Author

Maru S, Jin G, Desai D, Amin S, Shwetank, Lauver MD, and Lukacher AE

Abstract

Polyomaviruses (PyVs) silently infect most humans, but they can cause life-threatening diseases in immunocompromised individuals. The JC polyomavirus (JCPyV) induces progressive multifocal leukoencephalopathy, a severe demyelinating disease in multiple sclerosis patients receiving immunomodulatory therapy, and BK polyomavirus (BKPyV)-associated nephropathy is a major cause of kidney allograft failure. No effective anti-PyV agents are available. Several compounds have been reported to possess anti-PyV activity in vitro , but none have shown efficacy in clinical trials. Productive PyV infection involves usurping the cellular retrograde vesicular transport pathway to enable endocytosed virions to navigate to the endoplasmic reticulum where virion uncoating begins. Compounds inhibiting this pathway have been shown to reduce infection by simian virus 40 (SV40), JCPyV, and BKPyV in tissue culture. In this study, we investigated the potential of Retro-2.1, a retrograde transport inhibitor, to limit infection by mouse polyomavirus (MuPyV) in vivo . We found that Retro-2.1 significantly reduced MuPyV levels in the kidney during acute infection without affecting renal function or the MuPyV-specific CD8 T cell response. To approximate the clinical setting of PyV resurgence in immunocompromised hosts, we showed that antibody-mediated depletion of T cells in persistently infected mice elevated MuPyV levels in the kidney and that Retro-2.1 blunted this increase in virus levels. In summary, these data indicate that inhibition of retrograde vesicular transport in vivo controls infection in a natural PyV mouse model and supports development of these compounds as potential therapeutic agents for individuals at risk for human PyV-associated diseases. IMPORTANCE PyVs can cause significant morbidity and mortality in immunocompromised individuals. No clinically efficacious anti-PyV therapeutic agents are available. A recently identified inhibitor of retrograde transport, Retro-2 cycl , blocks movement of PyV virion-containing vesicles from early endosomes to the endoplasmic reticulum, an early step in the PyV life cycle. Retro-2 cycl and its derivatives have been shown to inhibit infection by human PyVs in tissue culture. Here, we demonstrate that a derivative of Retro-2 cycl , Retro-2.1, reduces infection by MuPyV in the kidneys of acutely infected mice. Mimicking the common clinical scenario of PyV resurgence, we further show that MuPyV levels increase in the kidneys of immunocompromised, persistently infected mice and that this increase is inhibited by Retro-2.1. These data provide the first evidence for control of a natural PyV infection in vivo by administration of an inhibitor of retrograde transport.

Published

2017

19. Maintenance of PD-1 on brain-resident memory CD8 T cells is antigen independent.

Author

Shwetank, Abdelsamed HA, Frost EL, Schmitz HM, Mockus TE, Youngblood BA, and Lukacher AE

Subjects

Adoptive Transfer, Animals, Brain virology, CD8-Positive T-Lymphocytes virology, Cell Differentiation, Cells, Cultured, Epigenesis, Genetic, Epitopes, T-Lymphocyte immunology, Female, Gene Expression Regulation, Immunologic Memory, Mice, Mice, Inbred C57BL, Mice, Knockout, Programmed Cell Death 1 Receptor genetics, Viral Load, Brain immunology, CD8-Positive T-Lymphocytes immunology, Polyomavirus physiology, Polyomavirus Infections immunology, Programmed Cell Death 1 Receptor metabolism

Abstract

Infection of the central nervous system (CNS) by murine polyomavirus (MuPyV), a persistent natural mouse pathogen, establishes brain-resident memory CD8 T cells (bT RM ) that uniformly and chronically express programmed cell death protein 1 (PD-1) irrespective of the expression of α E integrin CD103, a T RM cell marker. In contrast, memory antiviral CD8 T cells in the spleen are PD-1 - , despite viral loads being similar in both the brain and spleen during persistent infection. Repetitive antigen engagement is central to sustained PD-1 expression by T cells in chronic viral infections; however, recent evidence indicates that expression of inhibitory receptors, including PD-1, is part of the T RM differentiation program. Here we asked whether PD-1 expression by CD8 bT RM cells during persistent MuPyV encephalitis is antigen dependent. By transferring MuPyV-specific CD8 bT RM cells into the brains of naive mice and mice infected with cognate epitope-sufficient and -deficient MuPyVs, we demonstrate that antigen and inflammation are dispensable for PD-1 maintenance. In vitro and direct ex vivo analyses indicate that CD103 - MuPyV-specific CD8 bT RM retain functional competence. We further show that the Pdcd-1 promoter of anti-MuPyV bT RM cells is epigenetically fixed in a demethylated state in the brain. In contrast, the PD-1 promoter of splenic antiviral memory CD8 T cells undergoes remethylation after being demethylated during acute infection. These data show that PD-1 expression is an intrinsic property of brain T RM cells in a persistent CNS viral infection.

Published

2017

20. Alloimmunity But Not Viral Immunity Promotes Allograft Loss in a Mouse Model of Polyomavirus-Associated Allograft Injury.

Author

Kim SC, Wang J, Dong Y, Mathews DV, Albrecht JA, Breeden CP, Farris AB, Lukacher AE, Ford ML, Newell KA, and Adams AB

Abstract

Background: The interplay between viral infection and alloimmunity is known to influence the fate of transplanted organs. Clarifying how local virus-associated inflammation/injury and antiviral immunity can alter host alloimmune responses in transplantation remains a critical question., Methods: We used a mouse model of polyomavirus (PyV) infection and kidney transplantation to investigate the roles of direct viral pathology, the antiviral immune response, and alloimmunity in the pathogenesis of PyV-associated allograft injury. We have previously shown that an effective primary T cell response is required in PyV-associated graft injury., Results: Here we show that the transfer of primed antidonor, but not antiviral, T cells results in PyV-associated allograft injury. In further studies, we use a surrogate minor antigen model (ovalbumin) and show that only antidonor specific T cells and not antiviral specific T cells are sufficient to mediate injury. Lastly, we demonstrate that local but not systemic virus-mediated inflammation and injury within the graft itself are required., Conclusions: These data suggest that in this mouse model, the predominant mechanism of allograft injury in PyV-associated injury is due to an augmented alloimmune T cell response driven by virus-induced inflammation/injury within the graft. These studies highlight the important interplay between viral infection and alloimmunity in a model system., Competing Interests: The authors declare no conflicts of interest.

Published

2017

21. TCR stimulation strength is inversely associated with establishment of functional brain-resident memory CD8 T cells during persistent viral infection.

Author

Maru S, Jin G, Schell TD, and Lukacher AE

Subjects

Animals, Brain immunology, Epitopes, T-Lymphocyte chemistry, Epitopes, T-Lymphocyte genetics, Epitopes, T-Lymphocyte immunology, Humans, Mice, Mice, Inbred C57BL, Mice, Transgenic, Polyomavirus Infections virology, Receptors, Antigen, T-Cell genetics, Brain virology, CD8-Positive T-Lymphocytes immunology, Immunologic Memory, Polyomavirus physiology, Polyomavirus Infections immunology, Receptors, Antigen, T-Cell immunology

Abstract

Establishing functional tissue-resident memory (TRM) cells at sites of infection is a newfound objective of T cell vaccine design. To directly assess the impact of antigen stimulation strength on memory CD8 T cell formation and function during a persistent viral infection, we created a library of mouse polyomavirus (MuPyV) variants with substitutions in a subdominant CD8 T cell epitope that exhibit a broad range of efficiency in stimulating TCR transgenic CD8 T cells. By altering a subdominant epitope in a nonstructural viral protein and monitoring memory differentiation of donor monoclonal CD8 T cells in immunocompetent mice, we circumvented potentially confounding changes in viral infection levels, virus-associated inflammation, size of the immunodominant virus-specific CD8 T cell response, and shifts in TCR affinity that may accompany temporal recruitment of endogenous polyclonal cells. Using this strategy, we found that antigen stimulation strength was inversely associated with the function of memory CD8 T cells during a persistent viral infection. We further show that CD8 TRM cells recruited to the brain following systemic infection with viruses expressing epitopes with suboptimal stimulation strength respond more efficiently to challenge CNS infection with virus expressing cognate antigen. These data demonstrate that the strength of antigenic stimulation during recruitment of CD8 T cells influences the functional integrity of TRM cells in a persistent viral infection.

Published

2017

22. Reducing persistent polyomavirus infection increases functionality of virus-specific memory CD8 T cells.

Author

Qin Q, Lauver M, Maru S, Lin E, and Lukacher AE

Subjects

Animals, Base Sequence, CD8-Positive T-Lymphocytes virology, Female, Gene Expression Regulation, Viral, Humans, Immunologic Memory, Mice, Mice, Inbred C57BL, Molecular Sequence Data, Polyomavirus genetics, Polyomavirus immunology, Polyomavirus Infections virology, Viral Proteins genetics, Viral Proteins metabolism, CD8-Positive T-Lymphocytes immunology, Polyomavirus physiology, Polyomavirus Infections immunology

Abstract

Mouse polyomavirus (MuPyV) causes a smoldering persistent infection in immunocompetent mice. To lower MuPyV infection in acutely and persistently infected mice, and study the impact of a temporal reduction in viral loads on the memory CD8 T cell response, we created a recombinant MuPyV in which a loxP sequence was inserted into the A2 strain genome upstream of the early promoter and another loxP sequence was inserted in cis into the intron shared by all three T antigens. Using mice transgenic for tamoxifen-inducible Cre recombinase, we demonstrated that reduction in MuPyV load during persistent infection was associated with differentiation of virus-specific CD8 T cells having a superior recall response. Evidence presented here supports the concept that reduction in viral load during persistent infection can promote differentiation of protective virus-specific memory CD8 T cells in patients at risk for diseases caused by human polyomaviruses., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2017

23. Type I Interferons Regulate the Magnitude and Functionality of Mouse Polyomavirus-Specific CD8 T Cells in a Virus Strain-Dependent Manner.

Author

Qin Q, Shwetank, Frost EL, Maru S, and Lukacher AE

Subjects

Animals, CD8-Positive T-Lymphocytes physiology, Capsid Proteins chemistry, Capsid Proteins metabolism, Cytokines genetics, Dendritic Cells chemistry, Dendritic Cells immunology, Gene Expression Regulation, Humans, Immunization, Immunologic Memory, Interferon Type I genetics, Interferon Type I immunology, Interferon-beta genetics, Interferon-beta pharmacology, Mice, Mutation, Polyomavirus physiology, Receptors, Antigen, T-Cell immunology, Virus Replication, CD8-Positive T-Lymphocytes immunology, Capsid Proteins genetics, Interferon Type I physiology, Polyomavirus genetics, Polyomavirus immunology, Viral Tropism

Abstract

Unlabelled: Mouse polyomavirus (MPyV) is a ubiquitous persistent natural mouse pathogen. A glutamic acid (E)-to-glycine (G) difference at position 91 of the VP1 capsid protein shifts the profile of tumors induced by MPyV from an epithelial to a mesenchymal cell origin. Here we asked if this tropism difference affects the MPyV-specific CD8 T cell response, which controls MPyV infection and tumorigenesis. Infection by the laboratory MPyV strain RA (VP1-91G) or a strain A2 mutant with an E-to-G substitution at VP1 residue 91 [A2(91G)] generated a markedly smaller virus-specific CD8 T cell response than that induced by A2(VP1-91E) infection. Mutant A2(91G)-infected mice showed a higher frequency of memory precursor (CD127(hi) KLRG1(lo)) CD8 T cells and a higher recall response than those of A2-infected mice. Using T cell receptor (TCR)-transgenic CD8 T cells and immunization with peptide-pulsed dendritic cells, we found that early bystander inflammation associated with A2 infection contributed to recruitment of the larger MPyV-specific CD8 T cell response. Beta interferon (IFN-β) transcripts were induced early during A2 or A2(91G) infections. IFN-β inhibited replication of A2 and A2(91G) in vitro Using mice lacking IFN-αβ receptors (IFNAR(-/-)), we showed that type I IFNs played a role in controlling MPyV replication in vivo but differentially affected the magnitude and functionality of virus-specific CD8 T cells recruited by A2 and A2(91G) viral infections. These data indicate that type I IFNs are involved in protection against MPyV infection and that their effect on the antiviral CD8 T cell response depends on capsid-mediated tropism properties of the MPyV strain., Importance: Isolates of the human polyomavirus JC virus from patients with the frequently fatal demyelinating brain disease progressive multifocal leukoencephalopathy (PML) carry single amino acid substitutions in the domain of the VP1 capsid protein that binds the sialic acid moiety of glycoprotein/glycolipid receptors on host cells. These VP1 mutations may alter neural cell tropism or enable escape from neutralizing antibodies. Changes in host cell tropism can affect recruitment of virus-specific CD8 T cells. Using mouse polyomavirus, we demonstrate that a single amino acid difference in VP1 known to shift viral tropism profoundly affects the quantity and quality of the anti-polyomavirus CD8 T cell response and its differentiation into memory cells. These findings raise the possibility that CD8 T cell responses to infections by human polyomaviruses may be influenced by VP1 mutations involving domains that engage host cell receptors., (Copyright © 2016, American Society for Microbiology. All Rights Reserved.)

Published

2016

24. Pathogen Stimulation History Impacts Donor-Specific CD8(+) T Cell Susceptibility to Costimulation/Integrin Blockade-Based Therapy.

Author

Badell IR, Kitchens WH, Wagener ME, Lukacher AE, Larsen CP, and Ford ML

Subjects

Animals, Bacterial Infections etiology, Graft Rejection etiology, Graft Survival, Humans, Immunosuppression Therapy, Immunosuppressive Agents therapeutic use, Lymphocyte Activation immunology, Mice, Mice, Inbred C57BL, Mice, Transgenic, Risk Factors, Transplantation, Homologous, Bacteria pathogenicity, Bacterial Infections therapy, CD8-Positive T-Lymphocytes immunology, Graft Rejection therapy, Immunologic Memory immunology, Integrins antagonists & inhibitors, Skin Transplantation, Tissue Donors

Abstract

Recent studies have shown that the quantity of donor-reactive memory T cells is an important factor in determining the relative heterologous immunity barrier posed during transplantation. Here, we hypothesized that the quality of T cell memory also potently influences the response to costimulation blockade-based immunosuppression. Using a murine skin graft model of CD8(+) memory T cell-mediated costimulation blockade resistance, we elicited donor-reactive memory T cells using three distinct types of pathogen infections. Strikingly, we observed differential efficacy of a costimulation and integrin blockade regimen based on the type of pathogen used to elicit the donor-reactive memory T cell response. Intriguingly, the most immunosuppression-sensitive memory T cell populations were composed primarily of central memory cells that possessed greater recall potential, exhibited a less differentiated phenotype, and contained more multi-cytokine producers. These data, therefore, demonstrate that the memory T cell barrier is dependent on the specific type of pathogen infection via which the donor-reactive memory T cells are elicited, and suggest that the immune stimulation history of a given transplant patient may profoundly influence the relative barrier posed by heterologous immunity during transplantation., (© Copyright 2015 The American Society of Transplantation and the American Society of Transplant Surgeons.)

Published

2015

25. Cutting Edge: Resident Memory CD8 T Cells Express High-Affinity TCRs.

Author

Frost EL, Kersh AE, Evavold BD, and Lukacher AE

Subjects

Animals, CD8-Positive T-Lymphocytes pathology, Female, Mice, Organ Specificity immunology, Polyomavirus Infections pathology, Tumor Virus Infections pathology, CD8-Positive T-Lymphocytes immunology, Gene Expression Regulation immunology, Immunologic Memory, Polyomavirus immunology, Polyomavirus Infections immunology, Receptors, Antigen, T-Cell immunology, Tumor Virus Infections immunology

Abstract

Tissue-resident memory T (TRM) cells serve as vanguards of antimicrobial host defense in nonlymphoid tissues, particularly at barrier epithelia and in organs with nonrenewable cell types (e.g., brain). In this study, we asked whether an augmented ability to sense Ag complemented their role as early alarms of pathogen invasion. Using mouse polyomavirus, we show that brain-resident mouse polyomavirus-specific CD8 T cells, unlike memory cells in the spleen, progressively increase binding to MHC class I tetramers and CD8 coreceptor expression. Using the two-dimensional micropipette adhesion-frequency assay, we show that TRM cells in brain, as well as in kidney, express TCRs with up to 20-fold higher affinity than do splenic memory T cells, whereas effector cells express TCRs of similar high affinity in all organs. Together, these data demonstrate that TRM cells retain high TCR affinity, which endows them with the high Ag sensitivity needed for front-line defense against infectious agents., (Copyright © 2015 by The American Association of Immunologists, Inc.)

Published

2015

26. Distinct and synergistic roles of FcγRIIB deficiency and 129 strain-derived SLAM family proteins in the development of spontaneous germinal centers and autoimmunity.

Author

Soni C, Domeier PP, Wong EB, Shwetank, Khan TN, Elias MJ, Schell SL, Lukacher AE, Cooper TK, and Rahman ZS

Subjects

Animals, B-Lymphocytes immunology, Immune Tolerance, Mice, Mice, 129 Strain, Receptors, IgG genetics, Signaling Lymphocytic Activation Molecule Family Member 1, T-Lymphocytes, Helper-Inducer immunology, Antigens, CD metabolism, Autoimmunity physiology, Germinal Center immunology, Germinal Center metabolism, Receptors, Cell Surface metabolism, Receptors, IgG deficiency

Abstract

The inhibitory IgG Fc receptor (FcγRIIB) deficiency and 129 strain-derived signaling lymphocyte activation molecules (129-SLAMs) are proposed to contribute to the lupus phenotype in FcγRIIB-deficient mice generated using 129 ES cells and backcrossed to C57BL/6 mice (B6.129.RIIBKO). In this study, we examine the individual contributions and the cellular mechanisms by which FcγRIIB deficiency and 129-derived SLAM family genes promote dysregulated spontaneous germinal center (Spt-GC) B cell and follicular helper T cell (Tfh) responses in B6.129.RIIBKO mice. We find that B6 mice congenic for the 129-derived SLAM locus (B6.129-SLAM) and B6 mice deficient in FcγRIIB (B6.RIIBKO) have increased Spt-GC B cell responses compared to B6 controls but significantly lower than B6.129.RIIBKO mice. These data indicate that both FcγRIIB deficiency and 129-SLAMs contribute to elevated Spt-GC B cell responses in B6.129.RIIBKO mice. However, only 129-SLAMs contribute significantly to augmented Tfh responses in B6.129.RIIBKO mice, and do so by a combination of T cell-dependent effects and enhanced B cell and DC-dependent antigen presentation to T cells. Elevated Spt-GC B cell responses in mice with FcγRIIB deficiency and polymorphic 129-SLAMs were associated with elevated metabolic activity, improved GC B cell survival and increased differentiation of naïve B cells into GC B cell phenotype. Our data suggest that the interplay between 129-SLAM expression on B cells, T cells and DCs is central to the alteration of the GC tolerance checkpoint, and that deficiency of FcγRIIB on B cells is necessary to augment Spt-GC responses, pathogenic autoantibodies, and lupus disease., (Copyright © 2015 Elsevier Ltd. All rights reserved.)

Published

2015

27. The importance of mouse models to define immunovirologic determinants of progressive multifocal leukoencephalopathy.

Author

Frost EL and Lukacher AE

Abstract

Progressive multifocal leukoencephalopathy (PML) is a severely debilitating and often fatal demyelinating disease of the central nervous system (CNS) in immunosuppressed individuals caused by JC polyomavirus (JCV), a ubiquitous human pathogen. Demyelination results from lytically infected oligodendrocytes, whose clearance is impaired in the setting of depressed JCV-specific T cell-mediated CNS surveillance. Although mutations in the viral capsid and genomic rearrangements in the viral non-coding region appear to set the stage for PML in the immunosuppressed population, mechanisms of demyelination and CNS antiviral immunity are poorly understood in large part due to absence of a tractable animal model that mimics PML neuropathology in humans. Early studies using mouse polyomavirus (MPyV) in T cell-deficient mice demonstrated productive viral replication in the CNS and demyelination; however, these findings were confounded by spinal cord compression by virus-induced vertebral bone tumors. Here, we review current literature regarding animal models of PML, focusing on current trends in antiviral T cell immunity in non-lymphoid organs, including the CNS. Advances in our understanding of polyomavirus lifecycles, viral and host determinants of persistent infection, and T cell-mediated immunity to viral infections in the CNS warrant revisiting polyomavirus CNS infection in the mouse as a bona fide animal model for JCV-PML.

Published

2015

28. Peptide immunization elicits polyomavirus-specific MHC class ib-restricted CD8 T cells in MHC class ia allogeneic mice.

Author

Hofstetter AR, Evavold BD, and Lukacher AE

Subjects

Animals, Female, Genotype, H-2 Antigens genetics, Mice, Vaccines, Subunit administration & dosage, CD8-Positive T-Lymphocytes immunology, Capsid Proteins immunology, H-2 Antigens immunology, Polyomavirus immunology, Vaccines, Subunit immunology

Abstract

Unlike the polymorphic MHC class Ia molecules, MHC class Ib molecules are oligomorphic or nonpolymorphic. We recently discovered a protective CD8 T cell response to mouse polyomavirus (MPyV) in H-2(b) haplotype mice that is restricted by H2-Q9, a member of the Qa-2 MHC class Ib family. Here, we demonstrate that immunization with a peptide corresponding to a virus capsid-derived peptide presented by Q9 also elicits MHC class Ib-restricted MPyV-specific CD8 T cells in mice of H-2(s) and H-2(g7) strains. These findings support the concept that immunization with a single MHC class Ib-restricted peptide can expand CD8 T cells in MHC class Ia allogeneic hosts.

Published

2013

29. Adaptive immunity rather than viral cytopathology mediates polyomavirus-associated nephropathy in mice.

Author

Albrecht JA, Dong Y, Wang J, Breeden C, Farris AB 3rd, Lukacher AE, and Newell KA

Subjects

Animals, Immunohistochemistry, Mice, Mice, Inbred C3H, Mice, Inbred C57BL, Real-Time Polymerase Chain Reaction, Viral Load, Adaptation, Physiological, Kidney Diseases immunology, Polyomavirus Infections immunology

Abstract

Nephropathy associated with BK polyomavirus causes kidney allograft dysfunction and failure. Understanding the pathogenesis of polyomavirus-associated allograft nephropathy (PVAN) is hampered by the species specificity of Polyomaviridae family members. Using a mouse polyomavirus (MPyV) kidney transplant model, we investigated clinically relevant variables that may contribute to PVAN. We found that the timing and source (i.e. donor vs. recipient) of MPyV infection and the titer of the viral inoculum have significant effects on the extent of allograft injury, with acute infection of the recipient by high-titer MPyV inoculums producing the most profound PVAN. In contrast, altering the degree of MHC matching or increasing ischemia/reperfusion injury by prolonging the cold ischemic time of the allograft did not affect the severity of PVAN. Survival correlated positively with serum creatinine levels, but not with viral loads in the kidney allograft. Using splenectomized alymphoplasia mice, which are unable to mount primary adaptive immune responses, we further demonstrate that persistent high viral loads in the kidney are not sufficient to cause advanced PVAN. These findings suggest that the mechanism of PVAN in mice is not a direct consequence of viral cytopathology, but rather involves interplay between viral infection and the recipient antidonor immune response., (© Copyright 2012 The American Society of Transplantation and the American Society of Transplant Surgeons.)

Published

2012

30. CD8 T cells recruited early in mouse polyomavirus infection undergo exhaustion.

Author

Wilson JJ, Pack CD, Lin E, Frost EL, Albrecht JA, Hadley A, Hofstetter AR, Tevethia SS, Schell TD, and Lukacher AE

Subjects

Animals, Mice, Mice, Knockout, Polyomavirus Infections genetics, Tumor Virus Infections genetics, CD8-Positive T-Lymphocytes immunology, Immunologic Memory, Polyomavirus immunology, Polyomavirus Infections immunology, Tumor Virus Infections immunology

Abstract

Repetitive Ag encounter, coupled with dynamic changes in Ag density and inflammation, imparts phenotypic and functional heterogeneity to memory virus-specific CD8 T cells in persistently infected hosts. For herpesvirus infections, which cycle between latency and reactivation, recent studies demonstrate that virus-specific T cell memory is predominantly derived from naive precursors recruited during acute infection. Whether functional memory T cells to viruses that persist in a nonlatent, low-level infectious state (smoldering infection) originate from acute infection-recruited naive T cells is not known. Using mouse polyomavirus (MPyV) infection, we previously showed that virus-specific CD8 T cells in persistently infected mice are stably maintained and functionally competent; however, a sizeable fraction of these memory T cells are short-lived. Further, we found that naive anti-MPyV CD8 T cells are primed de novo during persistent infection and contribute to maintenance of the virus-specific CD8 T cell population and its phenotypic heterogeneity. Using a new MPyV-specific TCR-transgenic system, we now demonstrate that virus-specific CD8 T cells recruited during persistent infection possess multicytokine effector function, have strong replication potential, express a phenotype profile indicative of authentic memory capability, and are stably maintained. In contrast, CD8 T cells recruited early in MPyV infection express phenotypic and functional attributes of clonal exhaustion, including attrition from the memory pool. These findings indicate that naive virus-specific CD8 T cells recruited during persistent infection contribute to preservation of functional memory against a smoldering viral infection.

Published

2012

31. MHC class Ib-restricted CD8 T cells differ in dependence on CD4 T cell help and CD28 costimulation over the course of mouse polyomavirus infection.

Author

Hofstetter AR, Ford ML, Sullivan LC, Wilson JJ, Hadley A, Brooks AG, and Lukacher AE

Subjects

Animals, CD40 Ligand immunology, Cell Division, Clonal Selection, Antigen-Mediated, Female, Interleukin-2 pharmacology, Kidney virology, Lymphocyte Activation, Mice, Mice, Inbred C57BL, Mice, Knockout, Mice, Transgenic, Polyomavirus isolation & purification, Polyomavirus Infections virology, Salivary Glands virology, Tumor Virus Infections virology, CD28 Antigens immunology, CD4-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes immunology, Histocompatibility Antigens Class I immunology, Polyomavirus Infections immunology, Tumor Virus Infections immunology

Abstract

We recently identified a protective MHC class Ib-restricted CD8 T cell response to infection with mouse polyomavirus. These CD8 T cells recognize a peptide from aa 139-147 of the VP2 viral capsid protein bound to the nonpolymorphic H-2Q9 molecule, a member of the Qa-2 family of β(2)m-associated MHC class Ib molecules. Q9:VP2.139-specific CD8 T cells exhibit an unusual inflationary response characterized by a gradual expansion over 3 mo followed by a stable maintenance phase. We previously demonstrated that Q9:VP2.139-specific CD8 T cells are dependent on Ag for expansion, but not for long-term maintenance. In this study, we tested the hypothesis that the expansion and maintenance components of the Q9:VP2.139-specific T cell response are differentially dependent on CD4 T cell help and CD28 costimulation. Depletion of CD4(+) cells and CD28/CD40L blockade impaired expansion of Q9:VP2.139-specific CD8 T cells, and intrinsic CD28 signaling was sufficient for expansion. In contrast, CD4 T cell insufficiency, but not CD28/CD40L blockade, resulted in a decline in frequency of Q9:VP2.139-specific CD8 T cells during the maintenance phase. These results indicate that the Q9:VP2.139-specific CD8 T cell response to mouse polyomavirus infection depends on CD4 T cell help and CD28 costimulation for inflationary expansion, but only on CD4 T cell help for maintenance.

Published

2012

32. The carboxypeptidase ACE shapes the MHC class I peptide repertoire.

Author

Shen XZ, Billet S, Lin C, Okwan-Duodu D, Chen X, Lukacher AE, and Bernstein KE

Subjects

Adaptive Immunity, Animals, Antigen Presentation genetics, Autoantigens immunology, Autoantigens metabolism, Cells, Cultured, Gene Expression Regulation genetics, Gene Expression Regulation immunology, Histocompatibility Antigens Class I genetics, Mice, Mice, Inbred C57BL, Mice, Knockout, Mice, Transgenic, Peptide Fragments immunology, Peptide Fragments metabolism, Peptidyl-Dipeptidase A genetics, Peptidyl-Dipeptidase A immunology, Protein Binding immunology, T-Cell Antigen Receptor Specificity genetics, T-Lymphocytes cytology, T-Lymphocytes immunology, Transgenes genetics, Clonal Selection, Antigen-Mediated genetics, Histocompatibility Antigens Class I metabolism, Peptidyl-Dipeptidase A metabolism, Proteasome Endopeptidase Complex metabolism, T-Lymphocytes metabolism

Abstract

The surface presentation of peptides by major histocompatibility complex (MHC) class I molecules is critical to CD8(+) T cell-mediated adaptive immune responses. Aminopeptidases have been linked to the editing of peptides for MHC class I loading, but carboxy-terminal editing is thought to be due to proteasome cleavage. By analysis of wild-type mice and mice genetically deficient in or overexpressing the dipeptidase angiotensin-converting enzyme (ACE), we have now identified ACE as having a physiological role in the processing of peptides for MHC class I. ACE edited the carboxyl terminus of proteasome-produced MHC class I peptides. The lack of ACE exposed new antigens but also abrogated some self antigens. ACE had substantial effects on the surface expression of MHC class I in a haplotype-dependent manner. We propose a revised model of peptide processing for MHC class I by introducing carboxypeptidase activity into the process.

Published

2011

33. Gamma interferon controls mouse polyomavirus infection in vivo.

Author

Wilson JJ, Lin E, Pack CD, Frost EL, Hadley A, Swimm AI, Wang J, Dong Y, Breeden CP, Kalman D, Newell KA, and Lukacher AE

Subjects

Animals, Animals, Newborn, Cells, Cultured, Disease Models, Animal, Female, Interferon-gamma administration & dosage, Kidney immunology, Kidney virology, Mice, Mice, Inbred C57BL, Mice, Knockout, Rodent Diseases immunology, Rodent Diseases pathology, Rodent Diseases virology, Viral Load, Viral Proteins antagonists & inhibitors, Virus Replication drug effects, Interferon-gamma immunology, Polyomavirus immunology, Polyomavirus pathogenicity, Polyomavirus Infections immunology, Polyomavirus Infections pathology

Abstract

Human polyomaviruses are associated with substantial morbidity in immunocompromised patients, including those with HIV/AIDS, recipients of bone marrow and kidney transplants, and individuals receiving immunomodulatory agents for autoimmune and inflammatory diseases. No effective antipolyomavirus agents are currently available, and no host determinants have been identified to predict susceptibility to polyomavirus-associated diseases. Using the mouse polyomavirus (MPyV) infection model, we recently demonstrated that perforin-granzyme exocytosis, tumor necrosis factor alpha (TNF-α), and Fas did not contribute to control of infection or virus-induced tumors. Gamma interferon (IFN-γ) was recently shown to inhibit replication by human BK polyomavirus in primary cultures of renal tubular epithelial cells. In this study, we provide evidence that IFN-γ is an important component of the host defense against MPyV infection and tumorigenesis. In immortalized and primary cells, IFN-γ reduces expression of MPyV proteins and impairs viral replication. Mice deficient for the IFN-γ receptor (IFN-γR(-/-)) maintain higher viral loads during MPyV infection and are susceptible to MPyV-induced tumors; this increased viral load is not associated with a defective MPyV-specific CD8(+) T cell response. Using an acute MPyV infection kidney transplant model, we further show that IFN-γR(-/-) donor kidneys harbor higher MPyV levels than donor kidneys from wild-type mice. Finally, administration of IFN-γ to persistently infected mice significantly reduces MPyV levels in multiple organs, including the kidney, a major reservoir for persistent mouse and human polyomavirus infections. These findings demonstrate that IFN-γ is an antiviral effector molecule for MPyV infection.

Published

2011

34. Minor antigens on transfused RBCs crossprime CD8 T cells but do not induce full effector function.

Author

Desmarets M, Mylvaganam G, Waller EK, Josephson CD, Pack C, Lukacher AE, and Zimring JC

Subjects

Animals, Apoptosis, Flow Cytometry, Graft Rejection immunology, Mice, Mice, Inbred C57BL, CD8-Positive T-Lymphocytes immunology, Erythrocyte Transfusion, Erythrocytes immunology

Abstract

HLA-matched bone marrow transplantation (BMT) is a cure for nonmalignant hematological disorders; however, rejection rates are high and correlate with the number of antecedent transfusions. Recently, using murine models, we reported that minor antigens (mHAs) in transfused leukoreduced red blood cell (RBC) or platelet units induce rejection of subsequent BMT. To study RBCs as an immunogen, we utilized transgenic donors that express a model mHA selectively on RBCs (HOD mouse). Transfusion of HOD blood did not induce BMT rejection of marrow that shared mHAs with the HOD RBCs. Similarly, no endogenous anti-HOD CD8(+) T-cell response was detected with antigen-specific tetramer reagents. Adoptively transferred OT-I T cells rapidly expanded after HOD blood transfusion; however, only a semi-effector phenotype was observed (tumor necrosis factor-α and interferon-γ secretion, but essentially no Granzyme B). After initial expansion, OT-I T cells contracted rapidly to very low levels. A similar trend was observed by in vivo CTL assay, with only transient lytic activity. Together, these data indicate that RBCs may not be the component of RBC units that induces BMT rejection, and suggest that contaminating platelets or leukocytes may be responsible., (© 2011 The Authors Journal compilation © 2011 The American Society of Transplantation and the American Society of Transplant Surgeons.)

Published

2011

35. Diverse roles of non-diverse molecules: MHC class Ib molecules in host defense and control of autoimmunity.

Author

Hofstetter AR, Sullivan LC, Lukacher AE, and Brooks AG

Subjects

Adaptive Immunity, Animals, Humans, Immunity, Innate, T-Lymphocytes immunology, Autoimmunity, Histocompatibility Antigens Class I immunology

Abstract

While the prime function of classical MHC class I molecules (MHC-I) is to present peptide antigens to pathogen-specific cytotoxic T cells, non-classical MHC-I antigens perform a diverse array of functions in both innate and adaptive immunity. In this review we summarize recent evidence that non classical MHC-I molecules are not only recognized by pathogen-specific T cells but that they also serve as immunoregulatory molecules by stimulating a number of distinct non-conventional T cell subsets., (Copyright © 2010 Elsevier Ltd. All rights reserved.)

Published

2011

36. Some unmet challenges in the immunology of viral infections.

Author

Rouse BT and Lukacher AE

Subjects

HIV immunology, Hepacivirus immunology, Humans, Immunity, Innate physiology, Influenza A Virus, H1N1 Subtype immunology, Treatment Outcome, Vaccination methods, Viral Vaccines immunology, Viral Vaccines therapeutic use, Virus Diseases immunology, Virus Diseases therapy, Viruses immunology

Abstract

Viral immunology is a rapidly evolving field. Major strides have been made in our understanding of innate and adaptive immune responses to viruses, largely based on highly reductionistic animal infection models, but more recently in humans, with validation that fundamental immunological concepts do in fact translate into clinical science well. From these studies there has emerged an appreciation of the enormous complexity of the immune response to viral infections as well as the diverse array of strategies developed by viruses to deal with immune detection. In this review, we highlight some of the major challenges we face in unraveling this complexity and summarize current efforts under way to improve the efficacy of viral vaccines.

Published

2010

37. Persistence of viral infection despite similar killing efficacy of antiviral CD8(+) T cells during acute and chronic phases of infection.

Author

Ganusov VV, Lukacher AE, and Byers AM

Subjects

Acute Disease, Animals, Chronic Disease, Cytotoxins, Gene Expression Regulation, Viral physiology, Mice, Models, Biological, Polyomavirus genetics, Polyomavirus metabolism, Polyomavirus Infections immunology, Spleen cytology, Tumor Virus Infections immunology, Viral Load, CD8-Positive T-Lymphocytes physiology, Polyomavirus physiology, Polyomavirus Infections virology, Tumor Virus Infections virology

Abstract

Why some viruses establish chronic infections while others do not is poorly understood. One possibility is that the host's immune response is impaired during chronic infections and is unable to clear the virus from the host. In this report, we use a recently proposed framework to estimate the per capita killing efficacy of CD8(+) T cells, specific for the polyoma virus (PyV), which establishes a chronic infection in mice. Surprisingly, the estimated per cell killing efficacy of PyV-specific effector CD8(+) T cells during the acute phase of the infection was very similar to the efficacy of effector CD8(+) T cells specific to lymphocytic choriomeningitis virus (LCMV-Armstrong), which is cleared from the host. Our results suggest that persistence of PyV does not result from the generation of an inefficient PyV-specific CD8(+) T cell response, and that other host or viral factors are responsible for the ability of PyV to establish chronic infection., (Copyright 2010 Elsevier Inc. All rights reserved.)

Published

2010

38. Heterogeneity among viral antigen-specific CD4+ T cells and their de novo recruitment during persistent polyomavirus infection.

Author

Lin E, Kemball CC, Hadley A, Wilson JJ, Hofstetter AR, Pack CD, and Lukacher AE

Subjects

Animals, Antigens, Viral, Tumor immunology, CD4-Positive T-Lymphocytes pathology, CD4-Positive T-Lymphocytes virology, Chronic Disease, Female, Mice, Mice, Inbred C57BL, Polyomavirus growth & development, Polyomavirus immunology, Polyomavirus Infections pathology, Polyomavirus Infections virology, Antigens, Polyomavirus Transforming immunology, CD4-Positive T-Lymphocytes immunology, Capsid Proteins immunology, Cell Movement immunology, Epitopes, T-Lymphocyte immunology, Polyomavirus Infections immunology

Abstract

Virus-specific CD4(+) T cells optimize antiviral responses by providing help for antiviral humoral responses and CD8(+) T cell differentiation. Although CD4(+) T cell responses to viral infections that undergo complete clearance have been studied extensively, less is known about virus-specific CD4(+) T cell responses to viruses that persistently infect their hosts. Using a mouse polyomavirus (MPyV) infection model, we previously demonstrated that CD4(+) T cells are essential for recruiting naive MPyV-specific CD8(+) T cells in persistently infected mice. In this study, we defined two dominant MPyV-specific CD4(+) T cell populations, one directed toward an epitope derived from the nonstructural large T Ag and the other from the major viral capsid protein of MPyV. These MPyV-specific CD4(+) T cells vary in terms of their magnitude, functional profile, and phenotype during acute and persistent phases of infection. Using a minimally myeloablative-mixed bone marrow chimerism approach, we further show that naive virus-specific CD4(+) T cells, like anti-MPyV CD8(+) T cells, are primed de novo during persistent virus infection. In summary, these findings reveal quantitative and qualitative differences in the CD4(+) T cell response to a persistent virus infection and demonstrate that naive antiviral CD4(+) T cells are recruited during chronic polyomavirus infection.

Published

2010

39. Regulation of primary alloantibody response through antecedent exposure to a microbial T-cell epitope.

Author

Hudson KE, Lin E, Hendrickson JE, Lukacher AE, and Zimring JC

Subjects

Adoptive Transfer, Animals, Bacteria immunology, Enzyme-Linked Immunosorbent Assay, Epitopes, B-Lymphocyte immunology, Erythrocytes microbiology, Erythrocytes virology, Flow Cytometry, Genome, Viral genetics, Humans, Mice, Mice, Inbred C57BL, Muramidase genetics, Ovalbumin genetics, Polymerase Chain Reaction, Polyomavirus genetics, Polyomavirus immunology, Bacterial Proteins immunology, Epitopes, T-Lymphocyte immunology, Erythrocytes immunology, Isoantibodies immunology, Muramidase immunology, Ovalbumin immunology, Peptide Fragments immunology

Abstract

Humoral alloimmunization to red blood cell (RBC) antigens is a clinically significant problem that can lead to transfusion reactions and difficulty in locating future compatible blood for transfusion. However, factors regulating responder/nonresponder status are only partially understood. Herein, we identify a series of microbes with 100% identity in 8- to 9-amino acid peptides containing the variant amino acids in Kell, Kidd, and Duffy antigens. To test the hypothesis that infection with such a microbe could predispose to RBC alloimmunization, a mouse model was developed using murine polyoma virus expressing a defined CD4(+) T-cell epitope ovalbumin(323-339) ((OVA)(323-339)) and subsequent transfusion with RBCs expressing a B-cell epitope (hen egg lysozyme [HEL]) fused to (OVA)(323-339). Whereas infection alone induced no detectable anti-HEL, subsequent RBC transfusion induced 100- to 1000-fold more anti-HEL in mice that had been previously infected compared with control mice. This effect did not occur with wild-type polyoma virus or RBCs expressing HEL alone. Together, these data indicate that prior exposure to a pathogen with small peptide homology to RBC antigens can lead to an enhanced primary alloantibody response. As such priming is not detectable by current clinical tests, it is unknown to what extent this occurs in human alloimmunization.

Published

2010

40. Abl family tyrosine kinases regulate sialylated ganglioside receptors for polyomavirus.

Author

Swimm AI, Bornmann W, Jiang M, Imperiale MJ, Lukacher AE, and Kalman D

Subjects

Animals, Cells, Cultured, Humans, Mice, Mice, Knockout, Neuraminidase antagonists & inhibitors, BK Virus physiology, Oncogene Proteins v-abl metabolism, Polyomavirus physiology, Protein-Tyrosine Kinases metabolism, Receptors, Cell Surface biosynthesis, Virus Internalization

Abstract

Sialylated lipids serve as cellular receptors for polyomaviruses. Using pharmacological inhibitors and cell lines derived from knockout mice, we demonstrate that Abl family tyrosine kinases are required for replication of mouse polyomavirus and BK virus, a human polyomavirus associated with allograft failure following kidney transplantation. We show that decreasing Abl family kinase activity results in low levels of cell surface ganglioside receptors for mouse polyomavirus and that inhibition of sialidase activity promotes virion binding in the absence of Abl family kinase activity. These data provide evidence that Abl family kinases reduce ganglioside turnover in the plasma membrane by inhibiting host cell sialidase activity. Thus, Abl family kinases regulate the susceptibility of cells to polyomavirus infection by modulating gangliosides required for viral attachment.

Published

2010

41. Immunity to polyomavirus infection: the polyomavirus-mouse model.

Author

Swanson PA 2nd, Lukacher AE, and Szomolanyi-Tsuda E

Subjects

Animals, Humans, Mice, Polyomavirus immunology, Polyomavirus Infections immunology, Tumor Virus Infections immunology

Abstract

A ubiquitous clinically silent murine pathogen, polyomavirus has enjoyed long-term co-evolution with the mouse, a highly tractable and genetically and immunologically informative small animal model. Thus, polyomavirus has provided a valuable experimental construct to decipher the host immune mechanisms that come into play to control systemic low-level persistent viral infections. Impaired immunosurveillance for infected cells puts the murine host at risk both to injury resulting from excessive direct virus cytolysis and development of virus-induced tumors. In this review, we present our current understanding of the multifaceted immune response invoked by the mouse to maintain détente with this potentially deleterious persistent natural pathogen, and discuss implications of these studies for therapeutic interventions for human polyomavirus infection.

Published

2009

42. Cutting edge: shift in antigen dependence by an antiviral MHC class Ib-restricted CD8 T cell response during persistent viral infection.

Author

Swanson PA 2nd, Hofstetter AR, Wilson JJ, and Lukacher AE

Subjects

Animals, Antigen Presentation genetics, Antigen Presentation immunology, CD8-Positive T-Lymphocytes virology, Capsid Proteins immunology, Capsid Proteins metabolism, Cell Proliferation, Female, H-2 Antigens genetics, H-2 Antigens metabolism, Histocompatibility Antigens Class I immunology, Histocompatibility Antigens Class I metabolism, Mice, Mice, Inbred C57BL, Mice, Knockout, Polyomavirus Infections pathology, Polyomavirus Infections virology, Time Factors, Tumor Virus Infections pathology, Tumor Virus Infections virology, CD8-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes metabolism, H-2 Antigens immunology, Polyomavirus immunology, Polyomavirus Infections immunology, Tumor Virus Infections immunology

Abstract

The requirement for Ag in maintaining memory CD8 T cells often differs between infections that are acutely resolved and those that persist. Using the mouse polyoma virus (PyV) persistent infection model, we recently described a novel CD8 T cell response directed to a PyV peptide presented by Q9, an MHC class Ib molecule. This antiviral Q9-restricted CD8 T cell response is characterized by a 3-mo expansion phase followed by a long-term plateau phase. In this study, we demonstrate that viral Ag is required for this protracted inflation phase but is dispensable for the maintenance of this Q9-restricted CD8 T cell response. Moreover, proliferation by memory T cells, not recruitment of naive PyV-specific T cells, is primarily responsible for Q9-restricted, anti-PyV CD8 T cell inflation. These data reveal a dynamic shift in Ag dependence by an MHC class Ib-restricted memory CD8 T cell response during a persistent viral infection.

Published

2009

43. Murine Polyomavirus encodes a microRNA that cleaves early RNA transcripts but is not essential for experimental infection.

Author

Sullivan CS, Sung CK, Pack CD, Grundhoff A, Lukacher AE, Benjamin TL, and Ganem D

Subjects

Animals, Base Sequence, CD8-Positive T-Lymphocytes immunology, Cell Line, Gene Expression Regulation, Viral, Mice, Mice, Inbred C57BL, MicroRNAs genetics, Molecular Sequence Data, Mutation, NIH 3T3 Cells, Polyomavirus genetics, Polyomavirus Infections genetics, RNA, Messenger metabolism, RNA, Viral chemistry, RNA, Viral genetics, MicroRNAs metabolism, Polyomavirus physiology, Polyomavirus Infections metabolism, RNA, Viral metabolism

Abstract

MicroRNAs are small regulatory RNAs that post-transcriptionally regulate gene expression and can be encoded by viral as well as cellular genomes. The functions of most viral miRNAs are unknown and few have been studied in an in vivo context. Here we show that the murine polyomavirus (PyV) encodes a precursor microRNA that is processed into two mature microRNAs, both of which are active at directing the cleavage of the early PyV mRNAs. Furthermore, we identify a deletion mutant of polyomavirus that is defective in encoding the microRNAs. This mutant replicates normally and transforms cultured cells with efficiencies comparable to wildtype PyV. The miRNA mutant is competent to establish a transient infection of mice following parenteral inoculation, and is cleared post infection at approximately the same rate as the wildtype virus. In addition, under these laboratory conditions, we observe no differences in anti-viral CD8 T cell responses. These results indicate that PyV miRNA expression is not essential for infection of cultured cells or experimentally inoculated mice, and raise the possibility that its role in natural infection might involve aspects of acquisition or spread that are not recapitulated by experimental inoculation.

Published

2009

44. An MHC class Ib-restricted CD8 T cell response confers antiviral immunity.

Author

Swanson PA 2nd, Pack CD, Hadley A, Wang CR, Stroynowski I, Jensen PE, and Lukacher AE

Subjects

Animals, CD8 Antigens genetics, CD8-Positive T-Lymphocytes virology, Capsid Proteins genetics, Female, Histocompatibility Antigens Class I genetics, Lymphocyte Depletion, Male, Mice, Mice, Knockout, Papillomavirus Vaccines genetics, Papillomavirus Vaccines immunology, Polymorphism, Genetic immunology, Polyomavirus genetics, Polyomavirus Infections genetics, CD8 Antigens immunology, CD8-Positive T-Lymphocytes immunology, Capsid Proteins immunology, Histocompatibility Antigens Class I immunology, Polyomavirus immunology, Polyomavirus Infections immunology

Abstract

Although immunity against intracellular pathogens is primarily provided by CD8 T lymphocytes that recognize pathogen-derived peptides presented by major histocompatibility complex (MHC) class Ia molecules, MHC class Ib-restricted CD8 T cells have been implicated in antiviral immunity. Using mouse polyoma virus (PyV), we found that MHC class Ia-deficient (K(b-/-)D(b-/-)) mice efficiently control this persistently infecting mouse pathogen. CD8 T cell depletion mitigates clearance of PyV in K(b-/-)D(b-/-) mice. We identified the ligand for PyV-specific CD8 T cells in K(b-/-)D(b-/-) mice as a nonamer peptide from the VP2 capsid protein presented by Q9, a member of the beta(2) microglobulin-associated Qa-2 family. Using Q9-VP2 tetramers, we monitored delayed but progressive expansion of these antigen-specific CD8alphabeta T cells in K(b-/-)D(b-/-) mice. Importantly, we demonstrate that Q9-VP2-specific CD8 T cells more effectively clear wild-type PyV than a VP2 epitope(null) mutant PyV. Finally, we show that wild-type mice also generate Q9-restricted VP2 epitope-specific CD8 T cells to PyV infection. To our knowledge, this is the first evidence for a defined MHC class Ib-restricted antiviral CD8 T cell response that contributes to host defense. This study motivates efforts to uncover MHC class Ib-restricted CD8 T cell responses in other viral infections, and given the limited polymorphism of MHC class Ib molecules, it raises the possibility of developing peptide-based viral vaccines having broad coverage across MHC haplotypes.

Published

2008

45. Generation of antiviral major histocompatibility complex class I-restricted T cells in the absence of CD8 coreceptors.

Author

Andrews NP, Pack CD, and Lukacher AE

Subjects

Adoptive Transfer, Animals, CD3 Complex analysis, CD4 Antigens analysis, CD8-Positive T-Lymphocytes chemistry, Cytotoxicity, Immunologic, Flow Cytometry, Interferon-gamma biosynthesis, Mice, Mice, Inbred C57BL, Mice, Knockout, Polyomavirus Infections immunology, Rhabdoviridae Infections immunology, T-Lymphocyte Subsets chemistry, Time Factors, CD8-Positive T-Lymphocytes immunology, Histocompatibility Antigens Class I immunology, Polyomavirus immunology, Receptors, Antigen, T-Cell immunology, T-Lymphocyte Subsets microbiology, Vesiculovirus immunology

Abstract

The CD8 coreceptor is important for positive selection of major histocompatibility complex I (MHC-I)-restricted thymocytes and in the generation of pathogen-specific T cells. However, the requirement for CD8 in these processes may not be essential. We previously showed that mice lacking beta(2)-microglobulin are highly susceptible to tumors induced by mouse polyoma virus (PyV), but CD8-deficient mice are resistant to these tumors. In this study, we show that CD8-deficient mice also control persistent PyV infection as efficiently as wild-type mice and generate a substantial virus-specific, MHC-I-restricted, T-cell response. Infection with vesicular stomatitis virus (VSV), which is acutely cleared, also recruited antigen-specific, MHC-I-restricted T cells in CD8-deficient mice. Yet, unlike in VSV infection, the antiviral MHC-I-restricted T-cell response to PyV has a prolonged expansion phase, indicating a requirement for persistent infection in driving T-cell inflation in CD8-deficient mice. Finally, we show that the PyV-specific, MHC-I-restricted T cells in CD8-deficient mice, while maintained long term at near-wild-type levels, are short lived in vivo and have extremely narrow T-cell receptor repertoires. These findings provide a possible explanation for the resistance of CD8-deficient mice to PyV-induced tumors and have implications for the maintenance of virus-specific MHC-I-restricted T cells during persistent infection.

Published

2008

46. Expression of angiotensin-converting enzyme changes major histocompatibility complex class I peptide presentation by modifying C termini of peptide precursors.

Author

Shen XZ, Lukacher AE, Billet S, Williams IR, and Bernstein KE

Subjects

Animals, Antigen-Presenting Cells immunology, CD8-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes metabolism, Histocompatibility Antigens Class I genetics, Histocompatibility Antigens Class I immunology, Macrophages, Peritoneal cytology, Macrophages, Peritoneal immunology, Mice, Mice, Knockout, Peptidyl-Dipeptidase A genetics, Peptidyl-Dipeptidase A immunology, Antigen Presentation physiology, Antigen-Presenting Cells enzymology, Macrophages, Peritoneal enzymology, Peptidyl-Dipeptidase A biosynthesis

Abstract

We recently reported a mouse model called ACE 10/10 in which macrophages overexpress the carboxypeptidase angiotensin-converting enzyme (ACE). These mice have an enhanced inflammatory response to tumors that markedly inhibits tumor growth. Here, we show that ACE modifies the C termini of peptides for presentation by major histocompatibility complex (MHC) class I molecules. The peptide-processing activity of ACE applies to antigens from either the extracellular environment (cross-presentation) or antigens produced endogenously. Consistent with its role in MHC class I antigen processing, ACE localizes to the endoplasmic reticulum. ACE overexpression does not appear to change the overall supply of peptides available to MHC class I molecules. The immunization of wild type mice previously given ACE 10/10 macrophages enhances the efficiency of antigen-specific CD8+ T cell priming. These data reveal that ACE is a dynamic participant in fashioning the peptide repertoire for MHC class I molecules by modifying the C termini of peptide precursors. Manipulation of peptidase expression by antigen-presenting cells may ultimately prove a useful strategy to enhance the immune response.

Published

2008

47. Allogeneic differences in the dependence on CD4+ T-cell help for virus-specific CD8+ T-cell differentiation.

Author

Kemball CC, Szomolanyi-Tsuda E, and Lukacher AE

Subjects

Acute Disease, Animals, Cell Differentiation, Chronic Disease, Cytotoxicity, Immunologic, Female, Lymphocyte Depletion, Mice, Mice, Inbred C3H, Mice, Inbred Strains, Polyomavirus Infections virology, Species Specificity, Tumor Virus Infections virology, Viral Plaque Assay, CD4-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes cytology, CD8-Positive T-Lymphocytes immunology, Polyomavirus immunology, Polyomavirus Infections immunology, Tumor Virus Infections immunology

Abstract

CD4(+) T-cell help enables antiviral CD8(+) T cells to differentiate into fully competent memory cells and sustains CD8(+) T-cell-mediated immunity during persistent virus infection. We recently reported that mice of C57BL/6 and C3H strains differ in their dependence on CD28 and CD40L costimulation for long-term control of infection by polyoma virus, a persistent mouse pathogen. In this study, we asked whether mice of these inbred strains also vary in their requirement for CD4(+) T-cell help for generating and maintaining polyoma virus-specific CD8(+) T cells. CD4(+) T-cell-depleted C57BL/6 mice mounted a robust antiviral CD8(+) T-cell response during acute infection, whereas unhelped CD8(+) T-cell effectors in C3H mice were functionally impaired during acute infection and failed to expand upon antigenic challenge during persistent infection. Using (C57BL/6 x C3H)F(1) mice, we found that the dispensability for CD4(+) T-cell help for the H-2(b)-restricted polyoma virus-specific CD8(+) T-cell response during acute infection extends to the H-2(k)-restricted antiviral CD8(+) T cells. Our findings demonstrate that dependence on CD4(+) T-cell help for antiviral CD8(+) T-cell effector differentiation can vary among allogeneic strains of inbred mice.

Published

2007

48. The antiviral CD8+ T cell response is differentially dependent on CD4+ T cell help over the course of persistent infection.

Author

Kemball CC, Pack CD, Guay HM, Li ZN, Steinhauer DA, Szomolanyi-Tsuda E, and Lukacher AE

Subjects

Animals, CD4-Positive T-Lymphocytes virology, CD8-Positive T-Lymphocytes virology, Chronic Disease, Enzyme-Linked Immunosorbent Assay, Female, Flow Cytometry, Histocompatibility Antigens Class II metabolism, Mice, Mice, Inbred C57BL, Polyomavirus immunology, Antibody Formation, CD4-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes immunology, Immunologic Memory, Polyomavirus Infections immunology

Abstract

Although many studies have investigated the requirement for CD4(+) T cell help for CD8(+) T cell responses to acute viral infections that are fully resolved, less is known about the role of CD4(+) T cells in maintaining ongoing CD8(+) T cell responses to persistently infecting viruses. Using mouse polyoma virus (PyV), we asked whether CD4(+) T cell help is required to maintain antiviral CD8(+) T cell and humoral responses during acute and persistent phases of infection. Though fully intact during acute infection, the PyV-specific CD8(+) T cell response declined numerically during persistent infection in MHC class II-deficient mice, leaving a small antiviral CD8(+) T cell population that was maintained long term. These unhelped PyV-specific CD8(+) T cells were functionally unimpaired; they retained the potential for robust expansion and cytokine production in response to Ag rechallenge. In addition, although a strong antiviral IgG response was initially elicited by MHC class II-deficient mice, these Ab titers fell, and long-lived PyV-specific Ab-secreting cells were not detected in the bone marrow. Finally, using a minimally myeloablative mixed bone marrow chimerism approach, we demonstrate that recruitment and/or maintenance of new virus-specific CD8(+) T cells during persistent infection is impaired in the absence of MHC class II-restricted T cells. In summary, these studies show that CD4(+) T cells differentially affect CD8(+) T cell responses over the course of a persistent virus infection.

Published

2007

49. Early virus-associated bystander events affect the fitness of the CD8 T cell response to persistent virus infection.

Author

Andrews NP, Pack CD, Vezys V, Barber GN, and Lukacher AE

Subjects

Adoptive Transfer, Animals, Bystander Effect genetics, CD8-Positive T-Lymphocytes pathology, Cell Differentiation genetics, Cell Differentiation immunology, Cells, Cultured, Dose-Response Relationship, Immunologic, Female, Homeostasis genetics, Homeostasis immunology, Immunization Schedule, Immunophenotyping, Kinetics, Mice, Mice, Inbred C57BL, Mice, Transgenic, Polyomavirus genetics, Polyomavirus Infections pathology, Polyomavirus Infections prevention & control, Spleen cytology, Spleen immunology, Spleen transplantation, Tumor Virus Infections pathology, Tumor Virus Infections prevention & control, Bystander Effect immunology, CD8-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes virology, Polyomavirus immunology, Polyomavirus Infections immunology, Tumor Virus Infections immunology

Abstract

Chronic Ag exposure during persistent viral infection erodes virus-specific CD8 T cell numbers and effector function, with a concomitant loss of pathogen control. Less clear are the respective contributions of Ag-specific and Ag-nonspecific (bystander) events on the quantity, quality, and maintenance of antiviral CD8 T cells responding to persistent virus infection. In this study, we show that low-dose inoculation with mouse polyomavirus (PyV) elicits a delayed, but numerically equivalent, antiviral CD8 T cell response compared with high-dose inoculation. Low-dose infection generated virus-specific CD8 T cells endowed with multicytokine functionality and a superior per cell capacity to produce IFN-gamma. PyV-specific CD8 T cells primed by low-dose inoculation also expressed higher levels of IL-7Ralpha and bcl-2 and possessed enhanced Ag-independent survival. Importantly, the quantity and quality of the antiviral CD8 T cell response elicited by dendritic cell-mediated immunization were mitigated by infection with a mutant PyV lacking the dominant CD8 T cell viral epitope. These findings suggest that the fitness of the CD8 T cell response to persistent virus infection is programmed in large part by early virus-associated Ag-nonspecific factors, and imply that limiting bystander inflammation at the time of inoculation, independent of Ag load, may optimize adaptive immunity to persistent viral infection.

Published

2007

50. Protection against polyoma virus-induced tumors is perforin-independent.

Author

Byers AM, Hadley A, and Lukacher AE

Subjects

Animals, Cells, Cultured, Cytokines biosynthesis, Lymphocyte Count, Membrane Glycoproteins deficiency, Membrane Glycoproteins genetics, Mice, Mice, Inbred C3H, Mice, Inbred C57BL genetics, Perforin, Pore Forming Cytotoxic Proteins deficiency, Pore Forming Cytotoxic Proteins genetics, Species Specificity, Tumor Necrosis Factor-alpha biosynthesis, CD8-Positive T-Lymphocytes immunology, Polyomavirus immunology, Polyomavirus Infections immunology, Tumor Virus Infections immunology

Abstract

CD8 T cells are necessary for controlling tumors induced by mouse polyoma virus (PyV), but the effector mechanism(s) responsible have not been determined. We examined the PyV tumorigenicity in C57BL/6 mice mutated in Fas or carrying targeted disruptions in the perforin gene or in both TNF receptor type I and type II genes. Surprisingly, none of these mice developed tumors. Perforin/Fas double-deficient radiation bone marrow chimeric mice were also resistant to PyV-induced tumors. Anti-PyV CD8 T cells in perforin-deficient mice were found not to differ from wild type mice with respect to phenotype, capacity to produce cytokines or maintenance of memory T cells, indicating that perforin does not modulate the PyV-specific CD8 T cell response. In addition, virus was cleared and persisted to similar extents in wild type and perforin-deficient mice. In summary, perforin/granzyme exocytosis is not an essential effector pathway for protection against PyV infection or tumorigenesis.

Published

2007