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Publication : HIVEP3 inhibits fate decision of CD8+ invariant NKT cells after positive selection.

First Author  Wu Q Year  2023
Journal  J Leukoc Biol Volume  114
Issue  4 Pages  335-346
PubMed ID  37479674 Mgi Jnum  J:342666
Mgi Id  MGI:7550557 Doi  10.1093/jleuko/qiad082
Citation  Wu Q, et al. (2023) HIVEP3 inhibits fate decision of CD8+ invariant NKT cells after positive selection. J Leukoc Biol 114(4):335-346
abstractText  CD8+ invariant natural killer T (iNKT) cells are functionally different from other iNKT cells and are enriched in human but not in mouse. To date, their developmental pathway and molecular basis for fate decision remain unclear. Here, we report enrichment of CD8+ iNKT cells in neonatal mice due to their more rapid maturation kinetics than CD8- iNKT cells. Along developmental trajectories, CD8+ and CD8- iNKT cells separate at stage 0, following stage 0 double-positive iNKT cells, and differ in HIVEP3 expression. HIVEP3 is lowly expressed in stage 0 CD8+ iNKT cells and negatively controls their development, whereas it is highly expressed in stage 0 CD8- iNKT cells and positively controls their development. Despite no effect on IFN-gamma, HIVEP3 inhibits granzyme B but promotes interleukin-4 production in CD8+ iNKT cells. Together, we reveal that, as a negative regulator for CD8+ iNKT fate decision, low expression of HIVEP3 in stage 0 CD8+ iNKT cells favors their development and T helper 1-biased cytokine responses as well as high cytotoxicity.
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