Conserved and context-dependent roles for pdgfrb signaling during zebrafish 
vascular mural cell development

Ando, Koji; Shih, Yu-Huan; Ebarasi, Lwaki; Grosse, Ann; Portman, Daneal; Chiba, Ayano; Mattonet, Kenny; Gerri, Claudia; Stainier, Didier Y. R.; Mochizuki, Naoki; Fukuhara, Shigetomo; Betsholtz, Christer; Lawson, Nathan D.

doi:10.1016/j.ydbio.2021.06.010

Item

ITEM ACTIONSEXPORT

Add to Basket

Local TagsRelease HistoryDetailsSummary

Released

Journal Article

Conserved and context-dependent roles for pdgfrb signaling during zebrafish vascular mural cell development

MPS-Authors

/persons/resource/persons239397

Mattonet, Kenny
Developmental Genetics, Max Planck Institute for Heart and Lung Research, Max Planck Society;

/persons/resource/persons224235

Gerri, Claudia
Developmental Genetics, Max Planck Institute for Heart and Lung Research, Max Planck Society;

/persons/resource/persons224278

Stainier, Didier Y. R.
Developmental Genetics, Max Planck Institute for Heart and Lung Research, Max Planck Society;

External Resource

No external resources are shared

Fulltext (restricted access)

There are currently no full texts shared for your IP range.

Fulltext (public)

There are no public fulltexts stored in PuRe

Supplementary Material (public)

There is no public supplementary material available

Citation

Ando, K., Shih, Y.-H., Ebarasi, L., Grosse, A., Portman, D., Chiba, A., et al. (2021). Conserved and context-dependent roles for pdgfrb signaling during zebrafish vascular mural cell development. DEVELOPMENTAL BIOLOGY, 479, 11-22. doi:10.1016/j.ydbio.2021.06.010.

Cite as: https://hdl.handle.net/21.11116/0000-0009-2420-A

Abstract

Platelet derived growth factor beta and its receptor, Pdgfrb, play essential roles in the development of vascular mural cells, including pericytes and vascular smooth muscle cells. To determine if this role was conserved in zebrafish, we analyzed pdgfb and pdgfrb mutant lines. Similar to mouse, pdgfb and pdgfrb mutant zebrafish lack brain pericytes and exhibit anatomically selective loss of vascular smooth muscle coverage. Despite these defects, pdgfrb mutant zebrafish did not otherwise exhibit circulatory defects at larval stages. However, beginning at juvenile stages, we observed severe cranial hemorrhage and vessel dilation associated with loss of pericytes and vascular smooth muscle cells in pdgfrb mutants. Similar to mouse, pdgfrb mutant zebrafish also displayed structural defects in the glomerulus, but normal development of hepatic stellate cells. We also noted defective mural cell investment on coronary vessels with concomitant defects in their development. Together, our studies support a conserved requirement for Pdgfrb signaling in mural cells. In addition, these zebrafish mutants provide an important model for definitive investigation of mural cells during early embryonic stages without confounding secondary effects from circulatory defects.