Heterogeneous and Tissue-Specific Regulation of Effector T Cell Responses by IFN-γ during <i>Plasmodium berghei</i> ANKA Infection

Villegas-Mendéz, Ana; Souza, J. Brian de; Murungi, Linda M.; Hafalla, Julius Clemence R.; Shaw, Tovah N.; Greig, Rachel; Riley, Eleanor M.; Couper, Kevin N.

doi:10.4049/jimmunol.1100241

Cited by 41 publications

(56 citation statements)

References 42 publications

(58 reference statements)

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“…1B). These data suggest that the IL-12 and IFN-γ responses to blood-stage malaria are involved in promoting CD4 T-cell contraction and support a recent report that CD4 T-cell contraction is reduced in P. berghei-infected IFN-γ −/− mice (16).…”

Section: Il-12 and Ifn-γ Interfere With The Development Of T-cell-medsupporting

confidence: 77%

“…In viral infections, elevated expression of IL-12 favors the development of responding T cells into short-lived, terminal effector cells rather than memory precursor effector cells (11,15); however less is known about the effects of inflammatory cytokines on the development of memory T cells during Plasmodium infections. There is evidence that during blood-stage Plasmodium infection IFN-γ is detrimental to the survival of Plasmodium-specific CD4 T cells by regulating its contraction phase (12,16). The observation that concurrent infection with Plasmodium falciparum impairs the development of vaccine-induced Plasmodium antigen-specific memory CD4 T cells (17) further suggests that the formation of T-cell-mediated immunological memory is impaired during malaria.…”

mentioning

confidence: 96%

“…Upon infection, the cytokines IL-12 and IFN-γ promote the differentiation of naive CD4 T cells into Th1 cells, which are known to mediate antibody-independent protection against Plasmodium infection (3). IL-12 and IFN-γ can further influence CD4 T-cell fate (19,20), and malaria-induced IFN-γ has been implicated in regulating the contraction of Plasmodium-specific CD4 T cells (12,16). Although the effects of IL-12 and IFN-γ on T-cell development and survival are well characterized in many infection models (11,15,21,22), they have not been investigated thoroughly during malaria.…”

Section: Il-12 and Ifn-γ Interfere With The Development Of T-cell-medmentioning

confidence: 99%

“…S1A), a finding that is consistent with reports from other murine Plasmodium blood-stage infection models (23,24). The peak of the inflammatory response to PbA infection of BALB/c mice occurs around days 4 and 5 post infection (25), and this acute phase of the response is followed by contraction of responding CD4 T cells starting around day 7 post infection (16).…”

Section: Il-12 and Ifn-γ Interfere With The Development Of T-cell-medmentioning

confidence: 99%

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APlasmodium-encoded cytokine suppresses T-cell immunity during malaria

Sun¹,

Holowka²,

Song³

et al. 2012

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

116

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The inability to acquire protective immunity against Plasmodia is the chief obstacle to malaria control, and inadequate T-cell responses may facilitate persistent blood-stage infection. Malaria is characterized by a highly inflammatory cytokine milieu, and the lack of effective protection against infection suggests that memory T cells are not adequately formed or maintained. Using a genetically targeted strain of Plasmodium berghei, we observed that the Plasmodium ortholog of macrophage migration inhibitory factor enhanced inflammatory cytokine production and also induced antigen-experienced CD4 T cells to develop into short-lived effector cells rather than memory precursor cells. The short-lived effector CD4 T cells were more susceptible to Bcl-2–associated apoptosis, resulting in decreased CD4 T-cell recall responses against challenge infections. These findings indicate that Plasmodia actively interfere with the development of immunological memory and may account for the evolutionary conservation of parasite macrophage migration inhibitory factor orthologs.

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Section: Il-12 and Ifn-γ Interfere With The Development Of T-cell-medsupporting

confidence: 77%

mentioning

confidence: 96%

Section: Il-12 and Ifn-γ Interfere With The Development Of T-cell-medmentioning

confidence: 99%

Section: Il-12 and Ifn-γ Interfere With The Development Of T-cell-medmentioning

confidence: 99%

See 2 more Smart Citations

APlasmodium-encoded cytokine suppresses T-cell immunity during malaria

Sun¹,

Holowka²,

Song³

et al. 2012

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

116

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show abstract

“…Whereas IFN-g regulates T cell number in many Ag-based systems, these studies have not always addressed whether these outcomes result from its effects on T cell differentiation, on APCs, or other immune cells, and are in some instances confounded by its effect on T cell proliferation (23,(34)(35)(36)(37). Indeed, the deficiency of IFN-g also compromises AICD (38), a pathway by which activated T cells generated in response to high concentrations of Ag or in situations of chronic infection or autoreactive cells are deleted (9).…”

Section: Discussionmentioning

confidence: 99%

Apoptotic Programs Are Determined during Lineage Commitment of CD4+ T Effectors: Selective Regulation of T Effector-Memory Apoptosis by Inducible Nitric Oxide Synthase

Purushothaman

Marcel

Garg

et al. 2013

The Journal of Immunology

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Lineage-committed T effectors generated in response to Ag during the inflammatory phase are destined to die during termination of the immune response. We present evidence to suggest that molecular signatures of lineage commitment are reflected in apoptotic cascades activated in CD4+ T effectors. Exemplifying this, ablation of inducible NO synthase (iNOS) protected effector-memory T (TEM) cells, but not TNaive or central-memory T cells, activated in vitro, from apoptosis triggered by cytokine deprivation. Furthermore, attrition of T effectors generated in the secondary, but not the primary, response to Ag was substantially reduced in mice, which received iNOS inhibitors. Distinct patterns of iNOS expression were revealed in wild-type TEM effectors undergoing apoptosis, and ablation of iNOS protein in primary and TEM wild-type effectors confirmed observations made in iNOS−/− cells. Describing molecular correlates of this dependence, mitochondrial damage, activation of the protein Bax, and release from mitochondria of the apoptosis-inducing factor were selectively abrogated in iNOS−/− TEM effectors. Suggesting that iNOS dependence was linked to the functional identity of T cell subsets, both iNOS induction and apoptosis were compromised in IFN-γ−/− TEM effectors, which mirrored the response patterns of iNOS−/− TEM. Collectively, these observations suggest that programs regulating deletion and differentiation are closely integrated and likely encoded during lineage commitment of T effectors.

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Increased Resistance to Malaria in Mice with Methylenetetrahydrofolate Reductase (Mthfr) Deficiency Suggests a Mechanism for Selection of theMTHFR677C>T (c.665C>T) Variant

Meadows

Pyzik

et al. 2014

Human Mutation

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The polymorphism 677C>T (NM_005957.4:c.665C>T/p.Ala222Val, rs1801133:C>T) in methylenetetrahydrofolate reductase (MTHFR) results in mild enzymatic deficiency and increased risk for several complex traits including adverse reproductive outcomes, birth defects, and heart disease. Despite these deleterious effects, homozygosity is high (5%-15%) in many populations, and among the highest in Mediterranean regions, where malaria was historically endemic and may have conferred a selective advantage for other mutations. We infected Mthfr-deficient (Mthfr(+) (/-) ) and MTHFR overexpressing (MTHFR(Tg) ) mice with Plasmodium berghei ANKA to induce cerebral malaria. Mthfr(+/-) mice survived longer (P < 0.02, log-rank test), and MTHFR(Tg) mice died earlier (P < 0.05, log-rank test) after infection compared with wild-type littermates. Flow cytometry revealed increased lymphocyte populations and increased CCR4(+) NK cells in spleen of Mthfr(+) (/-) mice; MTHFR(Tg) animals had decreased numbers of these NK cells. Interferon-γ and interleukin-10 immunoreactive proteins were increased and decreased, respectively, in brain of Mthfr(+/-) mice compared with wild-type. We suggest that mild MTHFR deficiency protects against malarial infection and that this phenomenon may have led to the high frequency of the 677C>T/c.665C>T variant in human populations.

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Heterogeneous and Tissue-Specific Regulation of Effector T Cell Responses by IFN-γ during Plasmodium berghei ANKA Infection

Cited by 41 publications

References 42 publications

APlasmodium-encoded cytokine suppresses T-cell immunity during malaria

APlasmodium-encoded cytokine suppresses T-cell immunity during malaria

Apoptotic Programs Are Determined during Lineage Commitment of CD4+ T Effectors: Selective Regulation of T Effector-Memory Apoptosis by Inducible Nitric Oxide Synthase

Increased Resistance to Malaria in Mice with Methylenetetrahydrofolate Reductase (Mthfr) Deficiency Suggests a Mechanism for Selection of theMTHFR677C>T (c.665C>T) Variant

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