MicroRNAs (miRNAs) are major regulators of cell responses, particularly in stressed cell states and host immune responses. Some miRNAs have a role in pathogen defense, including regulation of immune responses to Plasmodium parasite infection. Using a nonlethal mouse model of blood stage malaria infection, we have found that miR-451^{-/-} mice infected with Plasmodium yoelii XNL cleared infection at a faster rate than did wild-type (WT) mice. MiR-451^{-/-} mice had an increased leukocyte response to infection, with the protective phenotype primarily driven by CD4^{+} T cells. WT and miR-451^{-/-} CD4^{+} T cells had similar activation responses, but miR-451^{-/-} CD4^{+} cells had significantly increased proliferation, both in vitro and in vivo. Myc is a miR-451 target with a central role in cell cycle progression and cell proliferation. CD4^{+} T cells from miR-451^{-/-} mice had increased postactivation Myc expression. RNA-Seq analysis of CD4^{+} cells demonstrated over 5000 differentially expressed genes in miR-451^{-/-} mice postinfection, many of which are directly or indirectly Myc regulated. This study demonstrates that miR-451 regulates T cell proliferative responses in part via a Myc-dependent mechanism.
【저자키워드】 miRNA, malaria, T cell, MYC, proliferation,