CD97 (F2F1F) Rabbit Monoclonal Antibody #92669
- WB
- IF
Product Specifications
| REACTIVITY | H |
| SENSITIVITY | Endogenous |
| MW (kDa) | 80, 50 |
| Source/Isotype | Rabbit IgG |
Application Key:
- WB-Western Blotting
- IF-Immunofluorescence
Species Cross-Reactivity Key:
- H-Human
Product Information
Product Usage Information
| Application | Dilution |
|---|---|
| Western Blotting | 1:1000 |
| Simple Western™ | 1:50 - 1:250 |
| Immunofluorescence (Immunocytochemistry) | 1:6400 |
Storage
Protocol
Specificity / Sensitivity
Species Reactivity:
Source / Purification
Background
CD97 exhibits the broadest expression pattern among EGF-TM7 family members, and is found on various cell types, including hematopoietic stem and progenitor cells, and other immune cells. It has been reported to play a role in leukocyte development, activation, and migration (3-5). It is also present on smooth muscle cells (e.g., vascular, skeletal, heart muscle cells), where it is thought to contribute to cell adhesion and muscle development (6). Through its EGF-like domains, CD97 can interact with various extracellular ligands, including CD55/DAF, chondroitin sulfate B, and selected integrins. These interactions mediate cell-cell and cell-matrix adhesion, and influence cell migration via activation of RhoA, Akt, and ERK signaling pathways (2,7,8). Upregulated CD97 is observed in a variety of human cancers, including gastric, colorectal, pancreatic, thyroid, and brain cancers, and its expression often correlates with advanced tumor stage, increased invasiveness, and poor patient prognosis. It has been shown that CD97 can enhance cancer cell migration, invasion, and metastasis, and promote angiogenesis by stimulating endothelial cell motility and invasion. Its soluble form can also act as a chemoattractant. In tumor cells, CD97 can activate pro-tumorigenic signaling via β-catenin, Akt, and RhoA pathways, contributing to cell proliferation and survival. CD97 interaction with tumor microenvironment components, including chondroitin sulfate and other adhesion molecules, can facilitate tumor growth and spread (2,6-9).
- Lin, H.H. et al. (2000) Genomics 67, 188-200.
- Safaee, M. et al. (2013) Int J Oncol 43, 1343-50.
- Stacey, M. et al. (2003) Blood 102, 2916-24.
- Kop, E.N. et al. (2009) Immunol Lett 123, 160-8.
- Capasso, M. et al. (2006) J Immunol 177, 1070-7.
- Aust, G. et al. (2006) Cell Tissue Res 324, 139-47.
- Somasundaram, A. et al. (2014) Neurosurg Focus 37, E14.
- Wang, T. et al. (2005) Blood 105, 2836-44.
- Ishikawa, N. et al. (2004) Clin Cancer Res 10, 8363-70.
Alternate Names
ADGRE5; Adhesion G protein-coupled receptor E5; Adhesion G protein-coupled receptor E5 subunit alpha; Adhesion G protein-coupled receptor E5 subunit beta; AGRE5; CD97; CD97 antigen; CD97 antigen subunit alpha; CD97 antigen subunit beta; CD97 molecule; Leukocyte antigen CD97; seven transmembrane helix receptor; seven-span transmembrane protein; seven-transmembrane, heterodimeric receptor associated with inflammation; TM7LN1
Limited Uses
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