Tissue Distribution of Memory T and B Cells in Rhesus Monkeys following Influenza A Infection

Pichyangkul, Sathit; Yongvanitchit, Kosol; Limsalakpetch, Amporn; Kum-Arb, Utaiwan; Im-Erbsin, Rawiwan; Boonnak, Kobporn; Arunee, Thitithayanont; Jongkaewwattana, Anan; Wiboon-ut, Suwimon; Mongkolsirichaikul, Duangrat; Mahanonda, Rangsini; Spring, Michele; Chuang, Ilin; Mason, Carl J.; Saunders, David

doi:10.4049/jimmunol.1501702

Cited by 35 publications

(37 citation statements)

References 67 publications

(76 reference statements)

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“…5). Interestingly, some of the human CD3 + T-cell infiltrates appeared to be fairly organized, such those described in the epithelial lung niches of severely-infected mice and humans with influenza viruses [60][61][62][63][64] (Fig. 5E).…”

Section: Sars-cov-2 Infected His-draga Mice Display Human-like Lung Imentioning

confidence: 83%

A Human-Immune-System (HIS) humanized mouse model (DRAGA: HLA-A2. HLA-DR4. Rag1 KO.IL-2Rγc KO. NOD) for COVID-19

Brumeanu

Vir

Shashikumar

et al. 2020

Preprint

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The current SARS-CoV-2 pandemic is accompanied by high morbidity and mortality rates, and there is a compelling need for effective vaccines and therapeutic agents to lessen the severity of COVID-19 disease. Appropriate animal models are essential for testing of vaccines and therapeutics and for mechanistic studies of infection and the host response. The Spike (S) protein of SARS-COV-2 has a high affinity for the human ACE2 receptor, which is expressed on multiple cell types including alveolar epithelial and vascular endothelial cells. Wild-type mice are not susceptible to developing coronavirus-mediated diseases. Accordingly, several human (h)ACE2 transgenic mouse models have been developed for coronavirus research. However, these mice have failed to closely mimic important aspects of the human immunopathological responses to SARS-CoV-2. We report herein that DRAGA (HLA-A2.HLA-DR4.Rag1KO.IL-2R. gammac KO.NOD) mice infused with human hematopoietic stem cells from cord blood reconstitute a fully functional human immune system, as well as engraft human epithelial and endothelial cells, sustain SARS-CoV-2 infection, and develop severe COVID-19-like symptoms. In pilot experiments, infected mice developed parenchymal and epithelial lung infiltrations with granzyme B+ and perforin+ CD8+ T cells and alveolar CD61+ microthrombi, mimicking human immunopathological responses to SARS-CoV-2. We propose the DRAGA mouse as a novel pre-clinical tool for studying COVID-19 immunopathology and human immune responses to SARS-CoV-2, including events leading to the cytokine storm and coagulopathies, as well as for testing of candidate vaccines and therapeutics.

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Section: Sars-cov-2 Infected His-draga Mice Display Human-like Lung Imentioning

confidence: 83%

A Human-Immune-System (HIS) humanized mouse model (DRAGA: HLA-A2. HLA-DR4. Rag1 KO.IL-2Rγc KO. NOD) for COVID-19

Brumeanu

Vir

Shashikumar

et al. 2020

Preprint

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“…Measurement of IL‐17 and IFN‐γ production in recirculating versus gingiva‐resident memory T cells based on CD69 expression was not possible because in vitro stimulation with SEB leads to CD69 expression on most T cells . We next compared the cytokine response between the memory T cell CD103 + and CD103 − subsets.…”

Section: Resultsmentioning

confidence: 99%

“…Measurement of IL-17 and IFN-production in recirculating versus gingiva-resident memory T cells based on CD69 expression was not possible because in vitro stimulation with SEB leads to CD69 expression on most T cells. 29 We next compared the cytokine response between the memory T cell CD103 + and CD103 − subsets. We found that the frequency of CD4 + CD103 + memory T cells that produced IFN-was 4.4-fold higher than that of CD4 + CD103 − memory T cells however, the differences did not reach statistical significance (12.87% ± 4.82% versus 2.92% ± 1.55%; P = 0.06) ( Figure 5B).…”

Section: Il-17 and Ifn-responses From Memory T Cells Isolated From Pementioning

confidence: 99%

Memory T cell subsets in healthy gingiva and periodontitis tissues

Mahanonda

Champaiboon

Subbalekha

et al. 2018

Journal of Periodontology

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Our findings suggest that recirculating and gingiva-resident memory T cells could represent an important part of the immune surveillance network in the connective tissue, maintaining periodontal homeostasis. Imbalance of subgingival bacterial communities could damage gingival barrier allowing bacterial antigens to get access to the deeper connective tissue where they activate memory T cells leading to deleterious inflammation; a hallmark of periodontitis.

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“…IgG-secreting plasma cells localized to the lung and peak at 2 weeks, finally resolving the infection. 98,99 Organisms lacking adaptive immunity were shown to have enhanced resistance to subsequent infections (trained immunity). Innate trained immunity occurs in human monocytes and MØ; mTOR/Akt/PI3K-regulated metabolic reprogramming, including increased glutamine metabolism, a shift from OXPHOS-to-aerobic glycolysis, and cholesterol synthesis contribute to this process.…”

Section: Igg2a and Other Isotypes Are Largely Th-dependent And Occurmentioning

confidence: 99%

Fueling influenza and the immune response: Implications for metabolic reprogramming during influenza infection and immunometabolism

Bahadoran

Bezavada

Smallwood

2020

Immunological Reviews

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The metabolic impact of influenza A virus (IAV) infections on immune cells remains largely uncharacterized. However, much is known about the metabolism of IAV infection and immunometabolism. Thus, we will consider four main factors: the metabolic requirements of influenza virus, metabolic reprogramming of immune cells that are mobilized to fight IAV infection, the impact of systemic or local metabolism on the infection and immune response, and vice versa. We will also address the interplay of metabolism and cytokines with a focus on those relevant to IAV infections. Finally, we will limit information on immunometabolism to key cell types critical to fighting IAV infection. We will relate this information to the unique metabolic demands on immune cells and discuss how their translocation through nutrient diverse and changing environments may affect their functions in IAV infection. | ME TABOLIS M AND THE LUNG MICROENVIRONMENT | Steady-state metabolismUnder aerobic conditions, cells sustain themselves catabolically using glycolytic carbons to fuel the tricarboxylic acid (TCA) cycle. AbstractRecent studies support the notion that glycolysis and oxidative phosphorylation are rheostats in immune cells whose bioenergetics have functional outputs in terms of their biology. Specific intrinsic and extrinsic molecular factors function as molecular potentiometers to adjust and control glycolytic to respiratory power output. In many cases, these potentiometers are used by influenza viruses and immune cells to support pathogenesis and the host immune response, respectively. Influenza virus infects the respiratory tract, providing a specific environmental niche, while immune cells encounter variable nutrient concentrations as they migrate in response to infection. Immune cell subsets have distinct metabolic programs that adjust to meet energetic and biosynthetic requirements to support effector functions, differentiation, and longevity in their ever-changing microenvironments. This review details how influenza coopts the host cell for metabolic reprogramming and describes the overlap of these regulatory controls in immune cells whose function and fate are dictated by metabolism. These details are contextualized with emerging evidence of the consequences of influenzainduced changes in metabolic homeostasis on disease progression. K E Y W O R D Shost pathogen, immune response, Immunometabolism, Influenza, metabolism, viral infection, virus | 141 BAHADORAN et Al.

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Tissue Distribution of Memory T and B Cells in Rhesus Monkeys following Influenza A Infection

Cited by 35 publications

References 67 publications

A Human-Immune-System (HIS) humanized mouse model (DRAGA: HLA-A2. HLA-DR4. Rag1 KO.IL-2Rγc KO. NOD) for COVID-19

A Human-Immune-System (HIS) humanized mouse model (DRAGA: HLA-A2. HLA-DR4. Rag1 KO.IL-2Rγc KO. NOD) for COVID-19

Memory T cell subsets in healthy gingiva and periodontitis tissues

Fueling influenza and the immune response: Implications for metabolic reprogramming during influenza infection and immunometabolism

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