Gamma Interferon Production Is Critical for Protective Immunity to Infection with Blood-Stage<i>Plasmodium berghei</i>XAT but Neither NO Production nor NK Cell Activation Is Critical

Yoneto, Toshihiko; Yoshimoto, Takayuki; Wang, Chrong‐Reen; Takahama, Yasuhiro; Tsuji, Moriya; Waki, Seiji; Nariuchi, Hideo

doi:10.1128/iai.67.5.2349-2356.1999

Cited by 77 publications

(28 citation statements)

References 42 publications

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“…Wild-type and TCR-d KO mice were infected with PbXAT. On days 14,16,18,20,22 and 24 post-infection (p.i. ), serum was taken from the PbXAT-infected WT mice.…”

Section: Passive Transfer Of Serummentioning

confidence: 99%

“…Inhibition of IFN-c signalling by gene knockout (KO) or injection of neutralizing anti-IFN-c antibody led to worsening of the parasitaemia, resulting in loss of fluctuation of the parasitaemia. 9,22 Interferon-c activates phagocytosis by macrophages and monocytes. Therefore, the fluctuations in the parasitaemia of bloodstage PbXAT parasites are strongly related to IFN-c.…”

Section: Introductionmentioning

confidence: 99%

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γδ T cells modulate humoral immunity against Plasmodium berghei infection

et al. 2018

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It is unclear whether γδ T cells are involved in humoral immunity against Plasmodium infection. Here, we show that B-cell-immunodeficient mice and γδ T-cell-deficient mice were incapable of protecting against Plasmodium berghei XAT parasites. γδ T-cell-deficient mice developed reduced levels of antigen-specific antibodies during the late phase of infection. The numbers of follicular helper T cells and germinal centre B cells in γδ T-cell-deficient mice were lower than in wild-type mice during the late phase of infection. Expression profiling of humoral immunity-related cytokines in γδ T cells showed that interleukin-21 (IL-21) and interferon-γ (IFN-γ) are increased during the early stage of infection. Furthermore, blockade of IL-21 and IFN-γ signalling during the early stage of infection led to reduction in follicular helper T cells and germinal centre B cells. γδ T-cell production of IL-21 and IFN-γ is crucial for the development and maintenance of follicular helper T cells and germinal centre B cells during the late phase of infection. Our data suggest that γδ T cells modulate humoral immunity against Plasmodium infection.

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“…Wild-type and TCR-d KO mice were infected with PbXAT. On days 14,16,18,20,22 and 24 post-infection (p.i. ), serum was taken from the PbXAT-infected WT mice.…”

Section: Passive Transfer Of Serummentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

γδ T cells modulate humoral immunity against Plasmodium berghei infection

et al. 2018

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“…The data presented confirm and extend published results for NO and other RNI (23), and show iNOS mRNA expression is altered during these murine malarias. These observations indicate that increased iNOS, particularly in the spleen, contributes to the control of malaria, although its presence may not be essential (36,37,46). However, RNI can cause adverse as well as beneficial effects and other experimental approaches, especially pharmacological studies, are required to determine the benefits and risks associated with changes in iNOS during malaria.…”

Section: Figurementioning

confidence: 99%

Expression of inducible nitric oxide synthase (iNOS) mRNA in target organs of lethal and non‐lethal strains of murine malaria

Nahrevanian

Dascombe

2002

Parasite Immunology

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Nitric oxide (NO) is a putative mediator of the immunological and/or pathological responses to malaria, consequently it is a potential target for novel drug therapy. Numerous cell types increase expression of inducible nitric oxide synthase (iNOS) under inflammatory conditions, the most relevant stimuli being cytokines and endotoxins. In this study the expression of iNOS mRNA in several target organs (brain, liver, spleen) of malaria have been investigated in MF1 mice during lethal Plasmodium (P.) berghei and non-lethal P. c. chabaudi infection. In P. berghei malaria, iNOS mRNA decreased in liver and was unchanged in spleen during the period of rising parasitaemia, but increased in both organs late in the infection, when parasitaemia was high and death imminent. In mice infected with P. c. chabaudi, spleen iNOS mRNA increased progressively throughout the early, peak and recovery periods of parasitaemia, but decreased in liver. Brain iNOS mRNA decreased in samples collected throughout the time courses of both infections. Hence it is evident that changes in iNOS mRNA in murine malaria depend upon the tissue, day of infection, degree of parasitaemia and strain of Plasmodium. These data indicate induction of iNOS mRNA in the spleen has a role in combating these strains of Plasmodium in MF1 mice. Failure to clear lethal P. berghei parasitaemia was associated with increased iNOS mRNA expression in the liver, which may contribute to the pathology of this malaria.

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“…42,43 These susceptibility differences may again be explained by systemic compared with local transgene expression or the differential requirement of IFN-c for host survival. IFN-c production is required for survival of P. berghei and L. major infections, and IFN-c expression was decreased in SAP-IL-12 p40 transgenic mice, [42][43][44][45][46] whereas we have shown that mortality from a Sendai viral infection is independent of IFN-c production. 3 Lastly, overexpression of IL-12 p40 using the keratinocyte-specific (K14) promoter resulted in the spontaneous accumulation of immune cells (macrophages, lymphocytes, eosinophils, mast cells and neutrophils) in the skin and the development of an inflammatory skin disease.…”

Section: Discussionmentioning

confidence: 98%

IL‐12 p80‐dependent macrophage recruitment primes the host for increased survival following a lethal respiratory viral infection

et al. 2009

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Summary A protective immune response to a respiratory viral infection requires a series of coordinated cellular and molecular responses. We have previously demonstrated that increased expression of airway epithelial cell interleukin (IL)‐12 p80, a macrophage chemoattractant, is associated with human respiratory viral infection and mediates post‐viral mortality in the mouse. To better understand the role of IL‐12 p80‐dependent macrophage chemotaxis in mediating viral immunity, we generated a transgenic mouse strain utilizing a promoter to drive IL‐12 p40 gene expression in the airway epithelium. This transgenic strain secreted biologically active IL‐12 p80 in a lung‐specific manner, and demonstrated a selective increase in the number of resident, unactivated airway macrophages at baseline. Following infection with a sublethal dose of mouse parainfluenza virus type 1 (Sendai virus), the transgenic mice demonstrated an earlier peak and decline in the number of airway inflammatory cells. The transgenic mice were resistant to a lethal dose of virus and this viral resistance was dependent on the increased number of airway macrophages at baseline as partial depletion prior to infection abrogated this phenotype. The survival advantage in the transgenic mice was independent of viral load but was associated with a more rapid decline in the number of airway inflammatory cells and concentrations of multiple chemokines including the CC chemokine ligand 2 (CCL2)/JE, CCL3/macrophage inflammatory protein (MIP)‐1α, CCL4/MIP‐1β, and CCL5/RANTES. Collectively, these results suggest that IL‐12 p80‐driven increases in the number of resident airway macrophages prime the host for a protective immune response that can confer increased survival following a lethal respiratory viral infection.

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Gamma Interferon Production Is Critical for Protective Immunity to Infection with Blood-StagePlasmodium bergheiXAT but Neither NO Production nor NK Cell Activation Is Critical

Cited by 77 publications

References 42 publications

γδ T cells modulate humoral immunity against Plasmodium berghei infection

γδ T cells modulate humoral immunity against Plasmodium berghei infection

Expression of inducible nitric oxide synthase (iNOS) mRNA in target organs of lethal and non‐lethal strains of murine malaria

IL‐12 p80‐dependent macrophage recruitment primes the host for increased survival following a lethal respiratory viral infection

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