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Lithium carbonate revitalizes tumor-reactive CD8 + T cells by shunting lactic acid into mitochondria.

Jingwei MaLiang TangYaoyao TanJingxuan XiaoKeke WeiXin ZhangYuan MaShuai TongJie ChenNannan ZhouLi YangZhang LeiYonggang LiJiadi LvJunwei LiuHuafeng ZhangKe TangYi ZhangBo Huang
Published in: Nature immunology (2024)
The steady flow of lactic acid (LA) from tumor cells to the extracellular space via the monocarboxylate transporter symport system suppresses antitumor T cell immunity. However, LA is a natural energy metabolite that can be oxidized in the mitochondria and could potentially stimulate T cells. Here we show that the lactate-lowering mood stabilizer lithium carbonate (LC) can inhibit LA-mediated CD8 + T cell immunosuppression. Cytoplasmic LA increased the pumping of protons into lysosomes. LC interfered with vacuolar ATPase to block lysosomal acidification and rescue lysosomal diacylglycerol-PKCθ signaling to facilitate monocarboxylate transporter 1 localization to mitochondrial membranes, thus transporting LA into the mitochondria as an energy source for CD8 + T cells. These findings indicate that targeting LA metabolism using LC could support cancer immunotherapy.
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