Recombinant Cynomolgus Monkey Fas/TNFRSF6/CD95 Fc, CF Summary
Details of Functionality |
Measured by its ability to inhibit Fas Ligand-induced apoptosis of Jurkat human acute T cell leukemia cells. Cheng, J. et al. (1994) Science 263:1759. The ED50 for this effect is 40.0-240 ng/mL. |
Source |
Chinese Hamster Ovary cell line, CHO-derived cynomolgus monkey Fas/TNFRSF6/CD95 protein Cynomolgus Monkey Fas/TNFRSF6/CD95 (Gln26-Asp173) Accession # Q9TSN4.1 | IEGRMD | Human IgG1 (Pro100-Lys330) | N-terminus | | C-terminus | |
|
Accession # |
|
N-terminal Sequence |
Gln26, inferred from deblocking revealing Val27 |
Structure / Form |
Disulfide-linked homodimer |
Protein/Peptide Type |
Recombinant Proteins |
Purity |
>95%, by SDS-PAGE visualized with Silver Staining and quantitative densitometry by Coomassie® Blue Staining. |
Endotoxin Note |
<0.10 EU per 1 μg of the protein by the LAL method. |
Applications/Dilutions
Dilutions |
|
Theoretical MW |
43 kDa. Disclaimer note: The observed molecular weight of the protein may vary from the listed predicted molecular weight due to post translational modifications, post translation cleavages, relative charges, and other experimental factors. |
SDS-PAGE |
55-70 kDa, under reducing conditions |
Packaging, Storage & Formulations
Storage |
Use a manual defrost freezer and avoid repeated freeze-thaw cycles.- 12 months from date of receipt, -20 to -70 °C as supplied.
- 1 month, 2 to 8 °C under sterile conditions after reconstitution.
- 3 months, -20 to -70 °C under sterile conditions after reconstitution.
|
Buffer |
Lyophilized from a 0.2 μm filtered solution in PBS. |
Purity |
>95%, by SDS-PAGE visualized with Silver Staining and quantitative densitometry by Coomassie® Blue Staining. |
Reconstitution Instructions |
Reconstitute at 500 μg/mL in PBS. |
Notes
This product is produced by and ships from R&D Systems, Inc., a Bio-Techne brand.
Alternate Names for Recombinant Cynomolgus Monkey Fas/TNFRSF6/CD95 Fc, CF
Background
Fas (
fibroblast
associated; also
known as APO-1 or CD95) is a member of the death receptor subfamily of the TNF
receptor superfamily and is designated TNFRSF6 (1-3). The human Fas precursor
is 335 amino acids (aa) in length, and contains a 25 aa signal peptide, a 148
aa extracellular domain (ECD), a 17 aa transmembrane sequence, and a 145 aa
cytoplasmic region. The ECD possesses three cysteine-rich TNFR repeats, while
the cytoplasmic region contains one death domain (DD) that is required for the
transduction of apoptotic signals (4). Cynomolgus monkey Fas ECD shares 91% aa
sequence identity with human Fas ECD. A human Fas isoform of 314 aa that lacks
the transmembrane sequence is secreted by resting lymphocytes, while isoforms
of 149, 132, 103 and 86 aa that also lack the DD and show substitutions for
parts of the TNFR repeats are less prominently expressed (4-6). All five
isoforms block the extrinsic apoptosis pathway induced by Fas ligand binding.
Fas ligand (FasL; also TNFSF6) is a type II transmembrane protein that belongs
to the TNF family and is expressed on activated T-cells, NK cells, and cells
found in immune privileged sites. Alternatively, FasL is also shed as a soluble
form (2, 6). Engagement of FasL induces oligomerization of preformed Fas
trimers (1, 2). This activated receptor complex recruits the adaptor molecule
FADD to form the Death-Inducing Signaling Complex (DISC). Upon activation,
caspases in the DISC initiate the apoptotic signaling cascade (7). Fas is
prominent in epithelial cells, hepatocytes, activated mature lymphocytes,
virus-transformed lymphocytes and tumor cells. It is an essential mediator in
the activation-induced death of T lymphocytes that terminates the immune
reaction (1, 2, 8). In immune-privileged tissues, infiltrating Fas-bearing
lymphocytes and inflammatory cells are killed by FasL engagement (9). Both
humans and mice with genetic defects in Fas accumulate abnormal lymphocytes and
develop systemic autoimmunity (1-3). The Fas pathway also appears to intersect
with the BIM (mitochondrial/intrinsic) apoptosis pathway (1).
- Bouillet, P. and L.A. O’Reilly (2009) Nat. Rev. Immunol. 9:514.
- Strasser, A. et al. (2009) Immunity 30:180.
- Ashkenazi, A. and V. Dixit (1999) Curr. Opin. Cell Biol. 11:255.
- SwissProt Accession # P25445.
- Liu, C. et al. (1995) Biochem. J. 310:957.
- Papoff, G. et al. (1996) J. Immunol. 156:4622.
- Thorburn, A. (2003) Cellular Signaling 16:139.
- Barreiro, R. et al. (2004) J. Immunol. 173:1519.
- Ferguson, T.A. and T.S Griffith (2006) Immunol. Rev. 213:228.
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