Metabolic reprogramming of macrophage polarization by creatine [ATAC-seq]

We found that the creatine metabolic pathway was differentially regulated under M1 versus M2 polarizing conditions. In return, creatine could suppress M1 by blocking STAT1 tyrosine phosphorylation while promote M2 by sustaining chromatin accessibility of specific gene loci. Overall design: Analyze the changes of chromatin accessibility in macrophages lack of creatine during macrophage polarization