Endothelial smoothened-dependent hedgehog signaling is not required for sonic hedgehog induced angiogenesis or ischemic tissue repair

Rajesh Gupta; Alexander R Mackie; Sol Misener; Lijun Liu; Douglas W Losordo; Raj Kishore

doi:10.1038/s41374-018-0028-5

Endothelial smoothened-dependent hedgehog signaling is not required for sonic hedgehog induced angiogenesis or ischemic tissue repair

Lab Invest. 2018 May;98(5):682-691. doi: 10.1038/s41374-018-0028-5. Epub 2018 Feb 16.

Authors

Rajesh Gupta^{1

2}, Alexander R Mackie³, Sol Misener³, Lijun Liu⁴, Douglas W Losordo^{3

5}, Raj Kishore^{3

6}

Affiliations

¹ Department of Medicine, College of Medicine and Life Sciences,, University of Toledo,, Toledo, OH, USA. rajesh.gupta@utoledo.edu.
² Feinberg Cardiovascular Research Institute, Northwestern University, Chicago, IL, USA. rajesh.gupta@utoledo.edu.
³ Feinberg Cardiovascular Research Institute, Northwestern University, Chicago, IL, USA.
⁴ Department of Medicine, College of Medicine and Life Sciences,, University of Toledo,, Toledo, OH, USA.
⁵ Caladrius Biosciences Inc., Basking Ridge, NJ, USA.
⁶ Center for Translational Medicine and Department of Pharmacology, Temple University School of Medicine, Philadelphia, PA, USA.

Abstract

Sonic Hedgehog (Shh) signaling induces neovascularization and angiogenesis. It is not known whether the hedgehog signaling pathway in endothelial cells is essential to angiogenesis. Smoothened (Smo) transduces hedgehog signaling across the cell membrane. This study assessed whether endothelial Smoothened-dependent Shh signaling is required for Shh-mediated angiogenesis and ischemic tissue repair. Endothelial-specific smoothened knockout mice, eSmo^Null were created using Cre-lox recombination system. eSmo^Null mice had no observable phenotype at baseline and showed normal cardiac function. Smoothened in CD31+ cells isolated from eSmo^Null hearts was significantly reduced compared to CD31+ cells from eSmo^WT littermate control hearts. Fluorescence immunostaining of eSmo^Null heart sections showed Smo expression in endothelial cells was abolished. The hind-limb ischemia (HLI) model was used to assess the response to ischemic injury. Perfusion ratio, limb motor function, and limb necrosis were not significantly different after HLI between eSmo^Null mice and eSmo^WT. Capillary densities in the ischemic limb in eSmo^Null mice were also similar to eSmo^WT at 4 weeks after HLI. Next, response to exogenous Shh was assessed in the corneal angiogenesis model. There was no significant difference in corneal angiogenesis induced by administration of Shh pellets between eSmo^WT and eSmo^Null mice. Furthermore, in vitro experiments demonstrated that direct Shh had limited effects on endothelial cell proliferation and migration. However, conditioned media from Shh-treated fibroblasts had a more potent effect on endothelial cell proliferation and migration than non-treated conditioned media. Furthermore, Shh treatment of fibroblasts dramatically stimulated angiogenic growth factor expression, including PDGF-B, VEGF-A, HGF and IGF. PDGF-B was the most upregulated and may contribute to the large neo-vessels associated with Shh-induced angiogenesis. Taken together, these data demonstrate that Shh signaling via Smoothened in endothelial cells is not required for angiogenesis and ischemic tissue repair. Shh signaling via stromal cells likely mediates its angiogenic effects.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Animals
Cells, Cultured
Endothelial Cells / physiology*
Fibroblasts / physiology
Hedgehog Proteins / physiology*
Hindlimb / blood supply
Ischemia / physiopathology*
Male
Mice
Neovascularization, Physiologic*
Signal Transduction / physiology*
Smoothened Receptor / physiology*

Substances

Hedgehog Proteins
Shh protein, mouse
Smo protein, mouse
Smoothened Receptor

Abstract

Publication types

MeSH terms

Substances

Grants and funding