EphB3, also known as Cek10, Tyro6, Sek4, Hek2, and Mdk5, is a 130 kDa member of the transmembrane Eph receptor tyrosine kinase family. The A and B classes of Eph proteins are distinguished by Ephrin ligand binding preference but have a common structural organization. Eph-Ephrin interactions are widely involved in the regulation of cell migration, tissue morphogenesis, and cancer progression (1). The 526 amino acid (aa) extracellular domain (ECD) of mature human EphB3 contains a ligand binding domain followed by a cysteine rich region and two fibronectin type III domains. The 418 aa cytoplasmic domain contains a tyrosine kinase domain, a sterile alpha motif (SAM), and a PDZ binding motif (2). Within the ECD, human EphB3 shares 96% aa sequence identity with mouse and rat EphB3. Binding of EphB3 to its ligands Ephrin-B1, B2, and B3 triggers forward signaling through EphB3 as well as reverse signaling through the Ephrin (1, 3). EphB3 also interacts in cis with the receptor tyrosine kinase Ryk (4). Activation of its kinase is required for some but not all of the effects of EphB3 on cellular adhesion, motility, and morphology (5). EphB3 is widely expressed during development and in the adult; it shows a complementary tissue distribution to the Ephrin-B ligands (6‑9). EphB3 function is important in vascular, nervous system, thymocyte, and palate development (6, 7, 10‑12). It directs embyronic neuronal axon pathfinding, and its upregulation on local macrophages following neuronal injury promotes the growth of regenerating axons (10, 13). EphB3 inhibits colorectal carcinogenesis and invasion by preventing the migration of tumor cells out of the intestinal crypt (9, 14). EphB3 function is supported by the cooperative action of EphB2 in several of these processes (6, 10‑12, 15).
Human EphB3 Alexa Fluor™ Plus 488‑conjugated Antibody
R&D Systems | Catalog # FAB5667AFP488
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Applications for Human EphB3 Alexa Fluor™ Plus 488‑conjugated Antibody
Western Blot
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Formulation
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Background: EphB3
References
- Pasquale, E.B. (2008) Cell 133:38.
- Bohme, B. et al. (1993) Oncogene 8:2857.
- Pasquale, E.B (2004) Nat. Neurosci. 7:417.
- Trivier, E. and T.S. Ganesan (2002) J. Biol. Chem. 277:23037.
- Miao, H. et al. (2005) J. Biol. Chem. 280:923.
- Adams, R.H. et al. (1999) Genes Dev. 13:295.
- Krull, C.E. et al. (1997) Curr. Biol. 7:571.
- Willson, C.A. et al. (2006) J. Mol. Histol. 37:369.
- Cortina, C. et al. (2007) Nature Genet. 39:1376.
- Birgbauer, E. et al. (2000) Development 127:1231.
- Alfaro, D. et al. (2008) Immunology 125:131.
- Risley, M. et al. (2009) Mech. Dev. 126:230.
- 13. Liu, X. et al. (2006) J. Neurosci. 26:3087.
- 14. Batlle, E. et al. (2005) Nature 435:1126.
- 15. Holmberg, J. et al. (2006) Cell 125:1151.
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This product is provided under an intellectual property license from Life Technologies Corporation. The transfer of this product is conditioned on the buyer using the purchased product solely in research conducted by the buyer, excluding contract research or any fee for service research, and the buyer must not (1) use this product or its components for (a) diagnostic, therapeutic or prophylactic purposes; (b) testing, analysis or screening services, or information in return for compensation on a per-test basis; or (c) manufacturing or quality assurance or quality control, and/or (2) sell or transfer this product or its components for resale, whether or not resold for use in research. For information on purchasing a license to this product for purposes other than as described above, contact Life Technologies Corporation, 5781 Van Allen Way, Carlsbad, CA 92008 USA or outlicensing@thermofisher.com.
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Protocols
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- Cellular Response to Hypoxia Protocols
- R&D Systems Quality Control Western Blot Protocol
- Troubleshooting Guide: Western Blot Figures
- Western Blot Conditions
- Western Blot Protocol
- Western Blot Protocol for Cell Lysates
- Western Blot Troubleshooting
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