Circulating Memory CD4+ T Cells Target Conserved Epitopes of Rhinovirus Capsid Proteins and Respond Rapidly to Experimental Infection in Humans

Muehling, Lyndsey M.; Tien, Duy; Kwok, William W.; Heymann, Peter W.; Pomés, Anna; Woodfolk, Judith A.

doi:10.4049/jimmunol.1600663

Cited by 36 publications

(48 citation statements)

References 82 publications

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“…As such, the T cell response must occur through activation of preexisting effector/memory T cells responding to common epitope(s) displayed by the infecting RV. Consistent with this, epitope mapping of RV targeting T cells had identified an HLA-DR4-restricted CD4-specific epitope of RV39 VP1 maps to a region that is conserved across RV groups A, B, and C [68••]. …”

Section: Adaptive Immune Response To Rhinovirusmentioning

confidence: 76%

Immune Responses in Rhinovirus-Induced Asthma Exacerbations

Steinke

Borish

2016

Curr Allergy Asthma Rep

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Acute asthma exacerbations are responsible for urgent care visits and hospitalizations; they interfere with school and work productivity, thereby driving much of the morbidity and mortality associated with asthma. Approximately 80 to 85 % of asthma exacerbations in children, adolescents, and less frequently adults are associated with viral upper respiratory tract viral infections, and rhinovirus (RV) accounts for ~60–70 % of these virus-associated exacerbations. Evidence suggests that it is not the virus itself but the nature of the immune response to RV that drives this untoward response. In particular, evidence supports the concept that RV acts to exacerbate an ongoing allergic inflammatory response to environmental allergens present at the time of the infection. The interaction of the ongoing IgE- and T cell-mediated response to allergen superimposed on the innate and adaptive immune responses to the virus and how this leads to triggering of an asthma exacerbation is discussed.

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Section: Adaptive Immune Response To Rhinovirusmentioning

confidence: 76%

Immune Responses in Rhinovirus-Induced Asthma Exacerbations

Steinke

Borish

2016

Curr Allergy Asthma Rep

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“…Thus, studying this phenomenon could yield insight into the pathogenicity of T H 1 cells in asthmatic patients. After experimental infection of healthy subjects with HRV-A16, circulating HRV-specific CD4 + T cells identified by means of tetramer staining that expanded after infection were predominantly IFN-γ + 142 . Moreover, IFN-γ + CD4 + T cells are readily detected in BAL fluid from allergic asthmatic patients experimentally infected with HRV.…”

Section: Heterogeneity Of T Cells and Influence Of The Tissue Microenmentioning

confidence: 99%

Pathogenic CD4 + T cells in patients with asthma

Muehling

Lawrence

Woodfolk

2017

Journal of Allergy and Clinical Immunology

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Asthma encompasses a variety of clinical phenotypes that involve distinct T cell–driven inflammatory processes. Improved understanding of human T-cell biology and the influence of innate cytokines on T-cell responses at the epithelial barrier has led to new asthma paradigms. This review captures recent knowledge on pathogenic CD4+ T cells in asthmatic patients by drawing on observations in mouse models and human disease. In patients with allergic asthma, TH2 cells promote IgE-mediated sensitization, airway hyperreactivity, and eosinophilia. Here we discuss recent discoveries in the myriad molecular pathways that govern the induction of TH2 differentiation and the critical role of GATA-3 in this process. We elaborate on how cross-talk between epithelial cells, dendritic cells, and innate lymphoid cells translates to T-cell outcomes, with an emphasis on the actions of thymic stromal lymphopoietin, IL-25, and IL-33 at the epithelial barrier. New concepts on how T-cell skewing and epitope specificity are shaped by multiple environmental cues integrated by dendritic cell “hubs” are discussed. We also describe advances in understanding the origins of atypical TH2 cells in asthmatic patients, the role of TH1 cells and other non-TH2 types in asthmatic patients, and the features of T-cell pathogenicity at the single-cell level. Progress in technologies that enable highly multiplexed profiling of markers within a single cell promise to overcome barriers to T-cell discovery in human asthmatic patients that could transform our understanding of disease. These developments, along with novel T cell–based therapies, position us to expand the assortment of molecular targets that could facilitate personalized treatments.

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“…Since there are over 160 distinct RV strains characterized to date [9], reinfection with other strains is common. Viral capsid proteins (VP) of RV contain sequences [79] and T cell epitopes [80], which are conserved across strains. erefore, humoral or cellular cross-reactivity might provide cross-strain protection against heterologous RV infection.…”

Section: Rhinovirus (Rv)mentioning

confidence: 99%

“…Co culture of DCs, RV-A39 and T cells resulted in proliferation of CD4 + and CD8 + T cells and enhanced IFNγ production. Muehling et al [80] showed that pre-existing CD4 + Tm cells, speci c to conserved epitopes of the VP region, proliferate upon RV-A16 challenge in seronegative donors. CD4 + T m cells mainly showed a 1 or T follicular helper phenotype.…”

Section: Rhinovirus (Rv)mentioning

confidence: 99%

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Respiratory virus-induced heterologous immunity

2018

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Purpose: To provide current knowledge on respiratory virus-induced heterologous immunity (HI) with a focus on humoral and cellular cross-reactivity. Adaptive heterologous immune responses have broad implications on infection, autoimmunity, allergy and transplant immunology. A better understanding of the mechanisms involved might ultimately open up possibilities for disease prevention, for example by vaccination. Methods: A structured literature search was performed using Medline and PubMed to provide an overview of the current knowledge on respiratoryvirus induced adaptive HI. Results: In HI the immune response towards one antigen results in an alteration of the immune response towards a second antigen. We provide an overview of respiratory virus-induced HI, including viruses such as respiratory syncytial virus (RSV), rhinovirus (RV), coronavirus (CoV) and in uenza virus (IV). We discuss T cell receptor (TCR) and humoral cross-reactivity as mechanisms of HI involving those respiratory viruses. Topics covered include HI between respiratory viruses as well as between respiratory viruses and other pathogens. Newly developed vaccines, which have the potential Cite this as Pusch E, Renz H, Skevaki C. Respiratory virus-induced heterologous immunity -Part of the problem or part of the solution? Allergo J Int 2018; 27:79-96

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Circulating Memory CD4+ T Cells Target Conserved Epitopes of Rhinovirus Capsid Proteins and Respond Rapidly to Experimental Infection in Humans

Cited by 36 publications

References 82 publications

Immune Responses in Rhinovirus-Induced Asthma Exacerbations

Immune Responses in Rhinovirus-Induced Asthma Exacerbations

Pathogenic CD4 + T cells in patients with asthma

Respiratory virus-induced heterologous immunity

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