Ligand oligomerization state controls Tie2 receptor trafficking and Angiopoietin-2 ligand-specific responses

Pietilä, Riikka; Nätynki, Marjut; Tammela, Tuomas; Kangas, J.; Pulkki, Kristina H.; Limaye, Nisha; Vikkula, Miikka; Koh, Gou Young; Saharinen, Pipsa; Alitalo, Kari; Eklund, Lauri

doi:10.1242/jcs.098020

Cited by 23 publications

(23 citation statements)

References 52 publications

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“…Interestingly, it has been shown previously that after activation, Tie2 forms clusters at cell-cell contacts in confluent cells where it regulates endothelial cell permeability and also has been shown to localize at the trailing edge of migrating cells. 13,44 We now show that during collective migration, Tie2 clusters form at the leading edge of leader cells but do not colocalize with adherens junction proteins or PKC, similar to what has been observed at cell junctions. 13 This suggests that distinct signaling events must emerge from Tie2 to promote the formation of ␤-catenin/PKC complexes at cell junctions and for the localization of polarity and adherens junction proteins at the leading edge.…”

Section: Discussionsupporting

confidence: 72%

Formation of a PKCζ/β-catenin complex in endothelial cells promotes angiopoietin-1–induced collective directional migration and angiogenic sprouting

Oubaha

Lin

Margaron

et al. 2012

Blood

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Section: Discussionsupporting

confidence: 72%

Formation of a PKCζ/β-catenin complex in endothelial cells promotes angiopoietin-1–induced collective directional migration and angiogenic sprouting

Oubaha

Lin

Margaron

et al. 2012

Blood

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“…We show that Tie1/Tie2 heterodimerization may involve interactions between the Fn3 domains, but it is not clear how Tie1 interacts with the arrays of Tie2 homodimers in trans or how angiopoietins bridge Tie2 association across EC-EC junctions. The context-dependent differences in angiopoietin-activated Tie2 signaling pathways may depend on differences in other subcellular protein constituents, such as integrins in the ECM contacts and VE-PTP in EC-EC contacts (10,13,19,47). Further structural and functional investigation is required to understand how Tie1 acts to modulate the effects of Ang1 and Ang2 on Tie2 and the mechanism of Ang2 antagonism in the Tie2 trans association.…”

Section: Discussionmentioning

confidence: 99%

Structural basis of Tie2 activation and Tie2/Tie1 heterodimerization

Leppänen

Saharinen

Alitalo

2017

Proc. Natl. Acad. Sci. U.S.A.

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The endothelial cell (EC)-specific receptor tyrosine kinases Tie1 and Tie2 are necessary for the remodeling and maturation of blood and lymphatic vessels. Angiopoietin-1 (Ang1) growth factor is a Tie2 agonist, whereas Ang2 functions as a contextdependent agonist/antagonist. The orphan receptor Tie1 modulates Tie2 activation, which is induced by association of angiopoietins with Tie2 in cis and across EC-EC junctions in trans. Except for the binding of the C-terminal angiopoietin domains to the Tie2 ligand-binding domain, the mechanisms for Tie2 activation are poorly understood. We report here the structural basis of Ang1-induced Tie2 dimerization in cis and provide mechanistic insights on Ang2 antagonism, Tie1/Tie2 heterodimerization, and Tie2 clustering. We find that Ang1-induced Tie2 dimerization and activation occurs via the formation of an intermolecular β-sheet between the membrane-proximal (third) Fibronectin type III domains (Fn3) of Tie2. The structures of Tie2 and Tie1 Fn3 domains are similar and compatible with Tie2/ Tie1 heterodimerization by the same mechanism. Mutagenesis of the key interaction residues of Tie2 and Tie1 Fn3 domains decreased Ang1-induced Tie2 phosphorylation and increased the basal phosphorylation of Tie1, respectively. Furthermore, the Tie2 structures revealed additional interactions between the Fn 2 (Fn2) domains that coincide with a mutation of Tie2 in primary congenital glaucoma that leads to defective Tie2 clustering and junctional localization. Mutagenesis of the Fn2-Fn2 interface increased the basal phosphorylation of Tie2, suggesting that the Fn2 interactions are essential in preformed Tie2 oligomerization. The interactions of the membrane-proximal domains could provide new targets for modulation of Tie receptor activity.eceptor tyrosine kinases (RTKs) expressed in the endothelial cells (ECs) of blood and lymphatic vessels control the development and function of the cardiovascular and lymphatic systems. The VEGFs and their endothelial receptors (VEGFRs) are key regulators of angiogenesis and vascular integrity (1, 2). The angiopoietin ligand/Tie receptor pathway is necessary for blood and lymphatic vessel remodeling during embryonic and postnatal development and for homeostasis of the mature vasculature (3, 4). Recently significant interest has focused on targeting the VEGFR and Tie receptor pathways in antiangiogenic and antilymphangiogenic therapies (5).Ang1 activation of Tie2 is indispensable for embryonic cardiac development and angiogenesis, and both Ang1 and Ang2 are necessary for the development of lymphatic and ocular vasculature. In adult tissues, Ang1 is required for vessel stabilization after angiogenesis (6-8). Ang2, which is produced by ECs and stored in their Weibel-Palade bodies for rapid release, can function as a weak Tie2 agonist or as a context-dependent antagonist that inhibits Ang1-induced Tie2 activation and vascular stability (9-11). Tie2 is the major signal-transducing receptor of the angiopoietin/Tie signaling axis, and the homologous Tie1 receptor m...

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“…For instance, angiopoietin 2 modulates the endothelial receptor tyrosine kinase Tie2 and induces Tie2 translocation to the specific cell-matrix contact sites located at the distal end of focal adhesions. It is reported that the different oligomeric/multimeric forms of the angiopoietins cause induction of distinct patterns of Tie2 trafficking (68). Similarly phosphorylation and dimerization regulate nucleocytoplasmic shuttling of mammalian STE20-like kinase (69).…”

Section: Discussionmentioning

confidence: 99%

Erythrocytic Stage-dependent Regulation of Oligomerization of Plasmodium Ribosomal Protein P2

Sudarsan

Sivakami

et al. 2012

Journal of Biological Chemistry

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Background: Plasmodium falciparum P2 (PfP2) protein plays nonribosomal roles through SDS-and DTT-resistant oligomerization. Results: For SDS-and DTT-sensitive oligomerization, the 53rd cysteine of PfP2 plays an important role. Conclusion: DTT-and SDS-resistant oligomerization of PfP2 was propagated by differentially expressed parasite proteins. Significance: Analysis of regulation of PfP2 oligomerization in parasite-infected erythrocytes may help in understanding the export of P2 to erythrocyte surface.

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Ligand oligomerization state controls Tie2 receptor trafficking and Angiopoietin-2 ligand-specific responses

Cited by 23 publications

References 52 publications

Formation of a PKCζ/β-catenin complex in endothelial cells promotes angiopoietin-1–induced collective directional migration and angiogenic sprouting

Formation of a PKCζ/β-catenin complex in endothelial cells promotes angiopoietin-1–induced collective directional migration and angiogenic sprouting

Structural basis of Tie2 activation and Tie2/Tie1 heterodimerization

Erythrocytic Stage-dependent Regulation of Oligomerization of Plasmodium Ribosomal Protein P2

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