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DOI: 10.1016/j.celrep.2019.03.004
¤ OpenAccess: Gold
This work has “Gold” OA status. This means it is published in an Open Access journal that is indexed by the DOAJ.

Lymphocyte Activation Gene-3 Maintains Mitochondrial and Metabolic Quiescence in Naive CD4+ T Cells

Dana M. Previte,Christina Martins,Erin C. O’Connor,M Marre,Gina M. Coudriet,Noah W. Beck,Ashley V. Menk,Rebecca H. Wright,Hubert M. Tse,Greg M. Delgoffe,Jon D. Piganelli

Cell biology
Biology
Mitochondrial biogenesis
2019
Lymphocyte activation gene-3 (LAG-3) is an inhibitory receptor expressed by CD4+ T cells and tempers their homeostatic expansion. Because CD4+ T cell proliferation is tightly coupled to bioenergetics, we investigate the role of LAG-3 in modulating naive CD4+ T cell metabolism. LAG-3 deficiency enhances the metabolic profile of naive CD4+ T cells by elevating levels of mitochondrial biogenesis. In vivo, LAG-3 blockade partially restores expansion and the metabolic phenotype of wild-type CD4+ T cells to levels of Lag3-/- CD4+ T cells, solidifying that LAG-3 controls these processes. Lag3-/- CD4+ T cells also demonstrate greater signal transducer and activator of transcription 5 (STAT5) activation, enabling resistance to interleukin-7 (IL-7) deprivation. These results implicate this pathway as a target of LAG-3-mediated inhibition. Additionally, enhancement of STAT5 activation, as a result of LAG-3 deficiency, contributes to greater activation potential in these cells. These results identify an additional mode of regulation elicited by LAG-3 in controlling CD4+ T cell responses.
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    Lymphocyte Activation Gene-3 Maintains Mitochondrial and Metabolic Quiescence in Naive CD4+ T Cells” is a paper by Dana M. Previte Christina Martins Erin C. O’Connor M Marre Gina M. Coudriet Noah W. Beck Ashley V. Menk Rebecca H. Wright Hubert M. Tse Greg M. Delgoffe Jon D. Piganelli published in 2019. It has an Open Access status of “gold”. You can read and download a PDF Full Text of this paper here.