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L-Citrulline Metabolism in Mice Augments CD4+ T Cell Proliferation and Cytokine Production In Vitro, and Accumulation in the Mycobacteria-Infected Lung.


ABSTRACT: Activation, recruitment, and effector function of T lymphocytes are essential for control of mycobacterial infection. These processes are tightly regulated in T cells by the availability of l-arginine within the microenvironment. In turn, mycobacterial infection dampens T cell responsiveness through arginase induction in myeloid cells, promoting sequestration of l-arginine within the local milieu. Here, we show T cells can replenish intracellular l-arginine through metabolism of l-citrulline to mediate inflammatory function, allowing anti-mycobacterial T cells to overcome arginase-mediated suppression. Furthermore, T cell l-citrulline metabolism is necessary for accumulation of CD4+ T cells at the site of infection, suggesting this metabolic pathway is involved during anti-mycobacterial T cell immunity in vivo. Together, these findings establish a contribution for l-arginine synthesis by T cells during mycobacterial infection, and implicate l-citrulline as a potential immuno-nutrient to modulate host immunity.

SUBMITTER: Lange SM 

PROVIDER: S-EPMC5696333 | biostudies-literature | 2017

REPOSITORIES: biostudies-literature

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l-Citrulline Metabolism in Mice Augments CD4<sup>+</sup> T Cell Proliferation and Cytokine Production <i>In Vitro</i>, and Accumulation in the Mycobacteria-Infected Lung.

Lange Shannon M SM   McKell Melanie C MC   Schmidt Stephanie M SM   Hossfeld Austin P AP   Chaturvedi Vandana V   Kinder Jeremy M JM   McAlees Jaclyn W JW   Lewkowich Ian P IP   Way Sing Sing SS   Turner Joanne J   Qualls Joseph E JE  

Frontiers in immunology 20171116


Activation, recruitment, and effector function of T lymphocytes are essential for control of mycobacterial infection. These processes are tightly regulated in T cells by the availability of l-arginine within the microenvironment. In turn, mycobacterial infection dampens T cell responsiveness through arginase induction in myeloid cells, promoting sequestration of l-arginine within the local milieu. Here, we show T cells can replenish intracellular l-arginine through metabolism of l-citrulline to  ...[more]

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