Tie1 controls angiopoietin function in vascular remodeling and inflammation
Emilia A. Korhonen, … , Kari Alitalo, Pipsa Saharinen
Emilia A. Korhonen, … , Kari Alitalo, Pipsa Saharinen
Published August 22, 2016
Citation Information: J Clin Invest. 2016;126(9):3495-3510. https://doi.org/10.1172/JCI84923.
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Research Article Angiogenesis Vascular biology Article has an altmetric score of 10

Tie1 controls angiopoietin function in vascular remodeling and inflammation

Abstract

The angiopoietin/Tie (ANG/Tie) receptor system controls developmental and tumor angiogenesis, inflammatory vascular remodeling, and vessel leakage. ANG1 is a Tie2 agonist that promotes vascular stabilization in inflammation and sepsis, whereas ANG2 is a context-dependent Tie2 agonist or antagonist. A limited understanding of ANG signaling mechanisms and the orphan receptor Tie1 has hindered development of ANG/Tie-targeted therapeutics. Here, we determined that both ANG1 and ANG2 binding to Tie2 increases Tie1-Tie2 interactions in a β1 integrin–dependent manner and that Tie1 regulates ANG-induced Tie2 trafficking in endothelial cells. Endothelial Tie1 was essential for the agonist activity of ANG1 and autocrine ANG2. Deletion of endothelial Tie1 in mice reduced Tie2 phosphorylation and downstream Akt activation, increased FOXO1 nuclear localization and transcriptional activation, and prevented ANG1- and ANG2-induced capillary-to-venous remodeling. However, in acute endotoxemia, the Tie1 ectodomain that is responsible for interaction with Tie2 was rapidly cleaved, ANG1 agonist activity was decreased, and autocrine ANG2 agonist activity was lost, which led to suppression of Tie2 signaling. Tie1 cleavage also occurred in patients with hantavirus infection. These results support a model in which Tie1 directly interacts with Tie2 to promote ANG-induced vascular responses under noninflammatory conditions, whereas in inflammation, Tie1 cleavage contributes to loss of ANG2 agonist activity and vascular stability.

Authors

Emilia A. Korhonen, Anita Lampinen, Hemant Giri, Andrey Anisimov, Minah Kim, Breanna Allen, Shentong Fang, Gabriela D’Amico, Tuomas J. Sipilä, Marja Lohela, Tomas Strandin, Antti Vaheri, Seppo Ylä-Herttuala, Gou Young Koh, Donald M. McDonald, Kari Alitalo, Pipsa Saharinen

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Figure 10

Model of Ang-Tie signaling during vessel remodeling and inflammation.

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Model of Ang-Tie signaling during vessel remodeling and inflammation. (A...
(A and B) ANG1- and ANG2-induced vascular remodeling requires Tie1, which is recruited to the Tie2 signaling complex at endothelial cell– cell junctions after ligand stimulation in a β1 integrin–dependent manner. Under noninflammatory conditions, ANG1 activates the Tie2/Akt pathway, leading to FOXO1 nuclear exclusion. Autocrine ANG2 has similar effects as a weak agonist. (C) In LPS-induced acute inflammation, ANG2 is released from Weibel-Palade bodies (WPBs), but Tie1 cleavage inhibits ANG2 agonist activity, leading to FOXO1 nuclear translocation and Ang2 gene transcription via a self-enforcing loop. These rapid changes are followed by decreased phospho-Tie2, Tie2, and ANG1 and impaired integrity of the inflamed vasculature. In these conditions, ANG2 switches from Tie2 agonist to antagonist and via β1 integrin, may further promote vascular destabilization. EC, endothelial cell; PC, pericyte; ECM, extracellular matrix.