and this was confirmed by whole mou

and this was confirmed by whole mount
immunostaining of the explants (Supplementary Figs 9 and 10a, b, and
Supplementary Video 4). Functional vessel formation was essential for
the successful engraftment because human iPSC-HEs transplanted without
endothelial cells failed to vascularize and engraft (Supplementary Fig.
10c–f). Human vessels were long-lasting as they were stabilized by human
MSC-derived perivascular cells (Fig. 3e–g)13,14. Interestingly, the human
iPSC-LB transplant vascular networkswere similar in density and morphology
to those of adult livers, whereas the vasculature in only HUVECs
and human MSC transplants were much less dense; functional vessels
were of similar diameter (approximately 12 mm) in both settings (in iPSCLB
transplants, and in HUVEC and human MSC transplants) (Fig. 3h, i,
and Supplementary Figs 11 and 12). Animal studies suggest that endothelial
cells not onlyform passive conduits to deliver nutrients and oxygen but
also establish an instructive vascular niche, which stimulates liver organogenesis
and regeneration through elaboration of paracrine trophogens.
Our transplantation approach provided a unique intravital monitoring
system for evaluating human iPSC-derived organ maturation and differentiation
throughout the organogenesis, enabling us to dissect the
previously uncharacterized roles of stromal cell types in human organ
development