Date published: 2025-11-9

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Tie-2 Inhibitors

Tie-2 inhibitors represent a class of chemical compounds that target the angiopoietin-Tie signaling pathway, specifically inhibiting the Tie-2 receptor tyrosine kinase. The Tie-2 receptor, predominantly expressed in endothelial cells, plays a crucial role in vascular development and stability by mediating cellular responses to angiopoietin ligands, particularly Angiopoietin-1 (Ang1) and Angiopoietin-2 (Ang2). The inhibition of Tie-2 disrupts the downstream signaling cascades that regulate endothelial cell survival, migration, and vascular permeability. This disruption results in altered angiogenesis, the process by which new blood vessels form from pre-existing vasculature, and can significantly impact the structural integrity of blood vessels. Tie-2 inhibitors, therefore, provide a unique chemical means to modulate these complex biological processes, offering insights into the mechanisms underlying vascular development and homeostasis. From a molecular perspective, Tie-2 inhibitors typically act by binding to the ATP-binding site of the Tie-2 receptor kinase domain, thereby blocking its autophosphorylation and subsequent activation of downstream signaling pathways. The specificity and affinity of these inhibitors for the Tie-2 receptor are crucial factors that determine their efficacy in modulating angiopoietin-Tie signaling. By inhibiting Tie-2, these compounds can reduce endothelial cell survival signals and increase vascular permeability, leading to changes in the architecture of the vascular network. The chemical diversity among Tie-2 inhibitors reflects the varied approaches to achieving this inhibition, ranging from small-molecule kinase inhibitors to more complex chemical entities. This diversity not only highlights the structural adaptability of these compounds but also underscores the intricate balance required to selectively target Tie-2 without affecting other receptor tyrosine kinases that share similar structural motifs.

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