Two streams of E cells converge before hemogenic endothelium. (A) UMAP of EHT trajectory (from Figure 1C, with FL-HSC removed) showing the 7 clusters identified by Louvain clustering in supplemental Figure 5A, with Wnt^hi E subdivided into Wnt^hi AE and Wnt^hi VE, plus Wnt^lo E subdivided into Wnt^lo AE and Wnt^lo VE based on the arterial/venous score determined as shown in panels B and C. (B) Enlarged UMAP highlighting the 2 streams of endothelial cells converging to conflux AE. Numbers in yellow circles represent pseudotime bins up to the point of convergence. The dotted gray line represents the boundary between AE and VE. (C) Arterial score vs venous score over pseudotime bins. Cluster VE from panel A is used as the first pseudotime bin. Curves are fitted for AE score and VE score of each branch using a generalized additive model. (D) Violin plots of expression of cluster-specific genes, including venous marker Nr2f2, arterial marker Sox17, Wnt^lo AE-specific gene Tmem255a, Wnt^hi AE-specific genes Foxq1 and Nkd1, and Notch ligand Dll4. (E) Average expression of Wnt^lo E, Wnt^hi E, and pre-HE-specific genes over pseudotime. Differentially expressed genes were derived by pairwise expression analysis between Wnt^lo E and Wnt^hi E. Pre-HE specific genes were derived by comparing pre-HE with Wnt^lo plus Wnt^hi E. (F) Heatmap showing stream-specific Reactome pathway activity over pseudotime. AUCell package⁶³  was used to compute a pathway activity score for each cell. One vs the rest Student t test was used to identify group-specific pathways and the top 6 most significant pathways were plotted.