Expression of the monocarboxylate transporter MCT1 is required for virus-specific mouse CD8 + T cell memory development.
Stefania d'AriaCéline MaquetShuang LiSuveera DhupAnouk LepezArnaud KohlerVincent F Van HéeRajesh K DadhichMarine FrenièreFabienne AndrisIvan NemazanyyPierre SonveauxBénédicte MachielsLaurent GilletMichel Y BraunPublished in: Proceedings of the National Academy of Sciences of the United States of America (2024)
Lactate-proton symporter monocarboxylate transporter 1 (MCT1) facilitates lactic acid export from T cells. Here, we report that MCT1 is mandatory for the development of virus-specific CD8 + T cell memory. MCT1-deficient T cells were exposed to acute pneumovirus (pneumonia virus of mice, PVM) or persistent γ-herpesvirus (Murid herpesvirus 4, MuHV-4) infection. MCT1 was required for the expansion of virus-specific CD8 + T cells and the control of virus replication in the acute phase of infection. This situation prevented the subsequent development of virus-specific T cell memory, a necessary step in containing virus reactivation during γ-herpesvirus latency. Instead, persistent active infection drove virus-specific CD8 + T cells toward functional exhaustion, a phenotype typically seen in chronic viral infections. Mechanistically, MCT1 deficiency sequentially impaired lactic acid efflux from activated CD8 + T cells, caused an intracellular acidification inhibiting glycolysis, disrupted nucleotide synthesis in the upstream pentose phosphate pathway, and halted cell proliferation which, ultimately, promoted functional CD8 + T cell exhaustion instead of memory development. Taken together, our data demonstrate that MCT1 expression is mandatory for inducing T cell memory and controlling viral infection by CD8 + T cells.