Mechanisms of Central Nervous System Viral Persistence: the Critical Role of Antibody and B Cells

Ramakrishna, Chandran; Stohlman, Stephen A.; Atkinson, Roscoe; Shlomchik, Mark J.; Bergmann, Cornelia C.

doi:10.4049/jimmunol.168.3.1204

Cited by 111 publications

(182 citation statements)

References 51 publications

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“…MHV can enter the CNS via the olfactory nerve system (40) and spreads transneuronally, leading to infection of distinct parts of the brain and the spinal cord. CTLs control viral replication within the CNS but cannot completely eliminate the virus (21), whereas neutralizing Abs are essential to prevent viral recrudescence (24). Thus, MHV is well adapted to use the CNS as an immunoprivileged site to escape complete clearance from the system.…”

Section: Discussionmentioning

confidence: 99%

“…This natural mouse pathogen is one of the most extensively studied coronaviruses (20). A strong CTL response mediates clearance of the virus between days 6 and 8 postinfection (21,22), and neutralizing Abs appear to be required to prevent re-emergence of persistent CNS infection (23,24). Nonetheless, before effective adaptive immune responses are elicited, type I IFN-mediated innate immune responses are essential for the survival of the host in the early phase of infection.…”

mentioning

confidence: 99%

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Type I IFN-Mediated Protection of Macrophages and Dendritic Cells Secures Control of Murine Coronavirus Infection

Cervantes-Barragán

Kalinke

Züst

et al. 2009

The Journal of Immunology

118

135

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The swift production of type I IFNs is one of the fundamental aspects of innate immune responses against viruses. Plasmacytoid dendritic cell-derived type I IFNs are of prime importance for the initial control of highly cytopathic viruses such as the mouse hepatitis virus (MHV). The aim of this study was to determine the major target cell populations of this first wave of type I IFNs. Generation of bone marrow-chimeric mice expressing the type I IFN receptor (IFNAR) on either hemopoietic or non-bone marrow-derived cells revealed that the early control of MHV depended mainly on IFNAR expression on hemopoietic cells. To establish which cell population responds most efficiently to type I IFNs, mice conditionally deficient for the IFNAR on different leukocyte subsets were infected with MHV. This genetic analysis revealed that IFNAR expression on LysM+ macrophages and CD11c+ dendritic cells was most important for the early containment of MHV within secondary lymphoid organs and to prevent lethal liver disease. This study identifies type I IFN-mediated cross-talk between plasmacytoid dendritic cells on one side and macrophages and conventional dendritic cells on the other, as an essential cellular pathway for the control of fatal cytopathic virus infection.

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Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

Type I IFN-Mediated Protection of Macrophages and Dendritic Cells Secures Control of Murine Coronavirus Infection

Cervantes-Barragán

Kalinke

Züst

et al. 2009

The Journal of Immunology

118

135

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“…In some experiments, CD8 TCR Tg mice (a gift from Dr. L. Sherman, The Scripps Research Institute) specific for peptide 518 -526 of PR8 HA and OVA 323-339-specific (DO11.10) TCR Tg mice were used as controls. WT TCR Tg, IFN-␥ Ϫ/Ϫ TCR Tg, BALB/c/Thy1.1, and B cell-deficient mice homozygous for a disruption at the J H locus (J H D) (20), backcrossed to BALB/c mice were all maintained at Trudeau Institute. BALB/c By and BALB/c nu/nu mice were purchased from The Jackson Laboratory.…”

Section: Micementioning

confidence: 99%

CD4 T Cell-Mediated Protection from Lethal Influenza: Perforin and Antibody-Mediated Mechanisms Give a One-Two Punch

Brown

Dilzer

Meents

et al. 2006

The Journal of Immunology

260

300

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The mechanisms whereby CD4 T cells contribute to the protective response against lethal influenza infection remain poorly characterized. To define the role of CD4 cells in protection against a highly pathogenic strain of influenza, virus-specific TCR transgenic CD4 effectors were generated in vitro and transferred into mice given lethal influenza infection. Primed CD4 effectors conferred protection against lethal infection over a broad range of viral dose. The protection mediated by CD4 effectors did not require IFN-γ or host T cells, but did result in increased anti-influenza Ab titers compared with untreated controls. Further studies indicated that CD4-mediated protection at high doses of influenza required B cells, and that passive transfer of anti-influenza immune serum was therapeutic in B cell-deficient mice, but only when CD4 effectors were present. Primed CD4 cells also acquired perforin (Pfn)-mediated cytolytic activity during effector generation, suggesting a second mechanism used by CD4 cells to confer protection. Pfn-deficient CD4 effectors were less able to promote survival in intact BALB/c mice and were unable to provide protection in B cell-deficient mice, indicating that Ab-independent protection by CD4 effectors requires Pfn. Therefore, CD4 effectors mediate protection to lethal influenza through at least two mechanisms: Pfn-mediated cytotoxicity early in the response promoted survival independently of Ab production, whereas CD4-driven B cell responses resulted in high titer Abs that neutralized remaining virus.

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“…IgG therapy (53)(54)(55)(56). Especially in the case of neurotropic viruses, Abs have been shown to limit or prevent virus spread to the CNS system or restrict virus expression (57)(58)(59)(60). Other viruses infecting epithelia such as pulmonary influenza virus can be cleared by application of Abs after establishment of infection (61).…”

Section: Different Strategies Leading To Similar Outcomes: Mmtv Vs Ebvmentioning

confidence: 99%

The role of neutralizing antibodies for mouse mammary tumor virus transmission and mammary cancer development

Finke

Luther²,

Acha‐Orbea³

2002

Proc. Natl. Acad. Sci. U.S.A.

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Mouse mammary tumor virus (MMTV) infection establishes chronic germinal centers and a lifelong neutralizing Ab response. We show that removal of the draining lymph node after establishment of the germinal center reaction led to complete loss of neutralizing Abs despite comparable infection levels in peripheral lymphocytes. Importantly, in the absence of neutralization, only the exocrine organs mammary gland, salivary gland, pancreas, and skin showed strikingly increased infection, resulting in accelerated mammary tumor development. Induction of stronger neutralization did not influence chronic infection levels of peripheral lymphoid organs but strongly inhibited mammary gland infection and virus transmission to the next generation. Taken together, we provide evidence that a tight equilibrium in virus neutralization allows limited infection of exocrine organs and controls cancer development in susceptible mouse strains. These experiments show that a strong neutralizing Ab response induced after infection is not able to control lymphoid MMTV infection. Strong neutralization, however, is capable of blocking amplification of mammary gland infection, tumor development, and virus transmission to the next generation. The results also indicate a role of neutralization in natural resistance to MMTV infection.

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Mechanisms of Central Nervous System Viral Persistence: the Critical Role of Antibody and B Cells

Cited by 111 publications

References 51 publications

Type I IFN-Mediated Protection of Macrophages and Dendritic Cells Secures Control of Murine Coronavirus Infection

Type I IFN-Mediated Protection of Macrophages and Dendritic Cells Secures Control of Murine Coronavirus Infection

CD4 T Cell-Mediated Protection from Lethal Influenza: Perforin and Antibody-Mediated Mechanisms Give a One-Two Punch

The role of neutralizing antibodies for mouse mammary tumor virus transmission and mammary cancer development

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