Fig. 5: SAMs are derived from monocytes and are associated with EMT activation.

a Pseudotime analysis of CD14⁺Mon1, TIMD4⁺SAMs, CD300E⁺intMon and IL1B⁺Pi Mon. b Changes in expression of fibrosis-related genes, marker genes for SAMs and marker genes for Pi Mon following pseudotime. c GSVA differential enrichment analysis of IGHM⁺naïve B, CD19⁺T1B, IGHD⁺T2B, and MME⁺Immature B in BA and control groups. d Correlation analysis of signature genes of SAMs (CD9 and TREM2) and KRT18, CDH2 in GSE46960, GSE122340, and GSE15235 cohorts. SAMs scar-associated macrophages, EMT epithelial-mesenchymal transition, GSVA Gene set variation analysis, BA biliary atresia.