Publication | Open Access
Enhanced cytotoxic T‐cell function and inhibition of tumor progression by Mst1 deficiency
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Citations
26
References
2015
Year
Cancer ImmunosurveillanceKinase Mst1Mst1 DeficiencyApoptosisImmunologyTumor ImmunityCell DeathTumor ProgressionTumor GrowthMammalian Ste-20T Cell ImmunityCellular Immune ResponseImmunotherapyMedicineCell BiologyCell SignalingTumor Biology
Mammalian ste-20 like kinase Mst1 plays important roles during apoptosis, proliferation, cell polarity, and migration. Here, we report a novel role of Mst1 for cytotoxic T-cell responses and tumor suppression. The defect of Mst1 caused decreased levels of FoxO, and promoted cytotoxicity in vitro. Mst1(-/-) cytotoxic T cells also exhibited enhanced T-bet expression that was associated with elevated expression levels of IFNγ and granzyme B. Moreover, Mst1(-/-) cytotoxic T cells suppressed tumor growth in vivo. The data suggest that Mst1 inhibits cytotoxicity via T-bet suppression by FoxO1 and FoxO3a. Thus, Mst1 is a potential therapeutic target for tumor immunotherapy.
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