MicroRNA-29a attenuates CD8 T cell exhaustion and induces memory-like CD8 T cells during chronic infection.
Erietta StelekatiZhangying CaiSasikanth ManneZeyu ChenJean-Christophe BeltraLance Alec BuchnessXuebing LengSvetlana RistinKito NzinghaViktoriya EkshyyanChristina NiaviMohamed S Abdel HakeemMohammed-Alkhatim AliSydney DruryChi Wai LauZhen GaoYuguang BanSimon K ZhouKarl Mark AnselMakoto KurachiMartha S JordanAlejandro V VillarinoShin Foong NgiowE John WherryPublished in: Proceedings of the National Academy of Sciences of the United States of America (2022)
CD8 T cells mediate protection against intracellular pathogens and tumors. However, persistent antigen during chronic infections or cancer leads to T cell exhaustion, suboptimal functionality, and reduced protective capacity. Despite considerable work interrogating the transcriptional regulation of exhausted CD8 T cells (TEX), the posttranscriptional control of TEX remains poorly understood. Here, we interrogated the role of microRNAs (miRs) in CD8 T cells responding to acutely resolved or chronic viral infection and identified miR-29a as a key regulator of TEX. Enforced expression of miR-29a improved CD8 T cell responses during chronic viral infection and antagonized exhaustion. miR-29a inhibited exhaustion-driving transcriptional pathways, including inflammatory and T cell receptor signaling, and regulated ribosomal biogenesis. As a result, miR-29a fostered a memory-like CD8 T cell differentiation state during chronic infection. Thus, we identify miR-29a as a key regulator of TEX and define mechanisms by which miR-29a can divert exhaustion toward a more beneficial memory-like CD8 T cell differentiation state.