Structural basis of Tie2 activation and Tie2/Tie1 heterodimerization

Abstract: 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-bind… Show more

“…Interestingly, while both novel ANGPT1 nonsense mutations we identified have a clear impact on ANGPT1 function and its ability to interact with the TEK receptor, each has a different mechanism. p.Q236* completely lacks the C-terminal receptor binding domain, which is required for interaction with TEK (19,20). In addition, the truncated ANGPT1 Q236* protein can readily form oligomeric complexes through its intact N-terminal domain with WT ANGPT1, a process that is critical to the signaling function of ANGPT1 (18,19).…”

“…p.Q236* completely lacks the C-terminal receptor binding domain, which is required for interaction with TEK (19,20). In addition, the truncated ANGPT1 Q236* protein can readily form oligomeric complexes through its intact N-terminal domain with WT ANGPT1, a process that is critical to the signaling function of ANGPT1 (18,19). We hypothesize that in heterozygous PCG patients, any truncated protein that escapes NMD might have a dominant-negative function on ANGPT1 signaling.…”

“…However, K249 is evolutionarily well conserved ( Figure 5C), and this mutation has been observed only once (in a South Asian individual) out of more than 121,000 alleles in the ExAC database. Owing to the location of this modified amino acid, we predicted that ANGPT1 K249R might be unable to properly oligomerize, which is important for its ability to activate TEK (18)(19)(20).…”

Angiopoietin-1 is required for Schlemm’s canal development in mice and humans

“…Interestingly, while both novel ANGPT1 nonsense mutations we identified have a clear impact on ANGPT1 function and its ability to interact with the TEK receptor, each has a different mechanism. p.Q236* completely lacks the C-terminal receptor binding domain, which is required for interaction with TEK (19,20). In addition, the truncated ANGPT1 Q236* protein can readily form oligomeric complexes through its intact N-terminal domain with WT ANGPT1, a process that is critical to the signaling function of ANGPT1 (18,19).…”

“…p.Q236* completely lacks the C-terminal receptor binding domain, which is required for interaction with TEK (19,20). In addition, the truncated ANGPT1 Q236* protein can readily form oligomeric complexes through its intact N-terminal domain with WT ANGPT1, a process that is critical to the signaling function of ANGPT1 (18,19). We hypothesize that in heterozygous PCG patients, any truncated protein that escapes NMD might have a dominant-negative function on ANGPT1 signaling.…”

“…However, K249 is evolutionarily well conserved ( Figure 5C), and this mutation has been observed only once (in a South Asian individual) out of more than 121,000 alleles in the ExAC database. Owing to the location of this modified amino acid, we predicted that ANGPT1 K249R might be unable to properly oligomerize, which is important for its ability to activate TEK (18)(19)(20).…”

Angiopoietin-1 is required for Schlemm’s canal development in mice and humans

“…Angiopoietin-1 (Ang1) is paracrine acting and is the primary agonistic ligand of Tie2 (8). Its multimeric structure can bind the Tie2 extracellular domain homodimer for strong Tie2 activation (9).…”

“…Indeed, because of its dimeric conformation, Ang2 fails to bridge Tie2 extracellular domain homodimers, limiting receptor dimerization and activation (9). As an antagonist of constitutive Ang1/Tie2 signaling, Ang2 acts contextually, enabling angiogenesis in the presence of angiogenic growth factors or driving vessels into regression in the absence of angiogenic stimuli (12).…”

Endothelial Tie1–mediated angiogenesis and vascular abnormalization promote tumor progression and metastasis

Angiopoietin‐Tie signaling in kidney diseases: an updated review