Abstract

Formation and remodeling of vascular beds are complex processes orchestrated by multiple signaling pathways. Although it is well accepted that vessels of a particular organ display specific features that enable them to fulfill distinct functions, the embryonic origins of tissue-specific vessels and the molecular mechanisms regulating their formation are poorly understood. The subintestinal plexus of the zebrafish embryo comprises vessels that vascularize the gut, liver and pancreas and, as such, represents an ideal model in which to investigate the early steps of organ-specific vessel formation. Here, we show that both arterial and venous components of the subintestinal plexus originate from a pool of specialized angioblasts residing in the floor of the posterior cardinal vein (PCV). Using live imaging of zebrafish embryos, in combination with photoconvertable transgenic reporters, we demonstrate that these angioblasts undergo two phases of migration and differentiation. Initially, a subintestinal vein forms and expands ventrally through a Bone Morphogenetic Protein-dependent step of collective migration. Concomitantly, a Vascular Endothelial Growth Factor-dependent shift in the directionality of migration, coupled to the upregulation of arterial markers, is observed, which culminates with the generation of the supraintestinal artery. Together, our results establish the zebrafish subintestinal plexus as an advantageous model for the study of organ-specific vessel development and provide new insights into the molecular mechanisms controlling its formation. More broadly, our findings suggest that PCV-specialized angioblasts contribute not only to the formation of the early trunk vasculature, but also to the establishment of late-forming, tissue-specific vascular beds.

Highlights

  • Establishment of a functional vascular system is essential for proper tissue development

  • Confocal imaging of 3.5 dpf Tg(fli1: EGFPy1;gata1a:dsRedsd2) (Yaniv et al, 2006) embryos revealed the presence of rostrocaudal blood flow in the supraintestinal artery (SIA), whereas circulation in the subintestinal vein (SIV) followed the directionality observed in the posterior cardinal vein (PCV; Fig. 1A, white arrows)

  • Our data track the embryonic origins and the derivatives of each component of the subintestinal vessel network and characterize the molecular circuits governing morphological changes that model the plexus into its final stereotypical shape

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Summary

Introduction

Establishment of a functional vascular system is essential for proper tissue development. In vertebrates, this process involves the formation of the main axial vessels through vasculogenesis, followed by a step of sprouting angiogenesis, to generate the systemic vasculature (Adams and Alitalo, 2007). As development proceeds, additional vascular beds form in order to support the establishment, growth and proper functionality of. A large bulk of data describing the development of the systemic vasculature has accumulated during the past decades (Potente et al, 2011), little is known about the embryonic origins and the molecular mechanisms underlying the formation of organ-specific vessels (Nolan et al, 2013)

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