6533b826fe1ef96bd1283b70
RESEARCH PRODUCT
Induced arginine transport via cationic amino acid transporter-1 is necessary for human T-cell proliferation
Markus MunderNadine LeuchtnerVanessa SchnitziusEllen I. ClossEva AmannAlice HabermeierJohanna RuppClaudia Luckner-mindenAnke Wernersubject
0301 basic medicinechemistry.chemical_classificationArginine transportArginineT cellImmunologyCD28BiologyMolecular biologyAmino acid03 medical and health sciences030104 developmental biologyImmune systemmedicine.anatomical_structureDownregulation and upregulationchemistrymedicineImmunology and AllergyAmino acid transporterdescription
Availability of the semiessential amino acid arginine is fundamental for the efficient function of human T lymphocytes. Tumor-associated arginine deprivation, mainly induced by myeloid-derived suppressor cells, is a central mechanism of tumor immune escape from T-cell-mediated antitumor immune responses. We thus assumed that transmembranous transport of arginine must be crucial for T-cell function and studied which transporters are responsible for arginine influx into primary human T lymphocytes. Here, we show that activation via CD3 and CD28 induces arginine transport into primary human T cells. Both naive and memory CD4(+) T cells as well as CD8(+) T cells specifically upregulated the human cationic amino acid transporter-1 (hCAT-1), with an enhanced and persistent expression under arginine starvation. When hCAT-1 induction was suppressed via siRNA transfection, arginine uptake, and cellular proliferation were impaired. In summary, our results demonstrate that hCAT-1 is a key component of efficient T-cell activation and a novel potential target structure to modulate adaptive immune responses in tumor immunity or inflammation.
| year | journal | country | edition | language |
|---|---|---|---|---|
| 2015-11-02 | European Journal of Immunology |