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Human Apo-Transferrin Protein, CF

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Product Details

Summary
Reactivity HuSpecies Glossary
Applications Bioactivity
Format
Carrier-Free

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Human Apo-Transferrin Protein, CF Summary

Details of Functionality
Measured in a serum-free cell proliferation assay using CHO-K1 cells.

The ED50 for this effect is <6.00 μg/mL.
Source
Human plasma-derived Apo-Transferrin protein
The human plasma used for the isolation of this product were certified by the supplier to be negative for HIV I and II antibodies, Hepatitis C antibody and Hepatitis B antigen at the time of shipment. Human blood products should always be treated in accordance with universal handling precautions.
Protein/Peptide Type
Natural Proteins
Endotoxin Note
<0.10 EU per 1 μg of the protein by the LAL method.

Applications/Dilutions

Dilutions
  • Bioactivity
  • Bioactivity2
SDS-PAGE
76-81 kDa, reducing conditions
Publications
Read Publications using
3188-AT in the following applications:

Packaging, Storage & Formulations

Storage
Use a manual defrost freezer and avoid repeated freeze-thaw cycles.
• 12 months from date of receipt at -20 to -70 °C as supplied.
• 1 month at 2-8 °C under sterile conditions after reconstitution.
• 3 months at -20 to -70 °C under sterile conditions after reconstitution.
Buffer
Lyophilized from a 0.2 μm filtered solution in deionized water.
Reconstitution Instructions
Reconstitute at 10 mg/mL in sterile, deionized water.

Notes

This product is produced by and ships from R&D Systems, Inc., a Bio-Techne brand.

Alternate Names for Human Apo-Transferrin Protein, CF

  • ApoTransferrin
  • Apo-Transferrin
  • CD71
  • p90
  • T9
  • TFR
  • TFR1
  • TFRC
  • TR
  • transferrin receptor (p90, CD71)
  • TRFR

Background

Human Transferrin (Tf) is a single chain, 80 kDa member of the anion-binding superfamily of proteins (1 - 5). It is a bilobed molecule that is the product of an ancient gene duplication event (1, 6). Transferrin is synthesized as a 698 amino acid (aa) precursor that is divided into a 19 aa signal sequence plus a 679 aa mature segment that contains 19 intrachain disulfide bonds. The crystal structure of Tf reveals a protein with two flanking 340 aa globular domains. Each are composed of a beta -sheet surrounded by series of alpha -helices (1, 7). The N- and C-terminal flanking regions (or domains) will bind ferric iron through the interaction of an obligate anion (usually bicarbonate) and four amino acids (His, Asp, and two Tyr) (7, 8). Apotransferrin (or iron-free) will initially bind one atom of iron at the C-terminus, and this is followed by subsequent iron binding by the N-terminus to form holotransferrin (diferric Tf) (8, 9). Through its C-terminal iron-binding domain, holotransferrin will interact with the type I Tf receptor (TfR) on the surface of cells where it is internalized into acidified endosomes. Iron dissociates from the Tf molecule within these endosomes, and is transported into the cytosol as ferrous iron. At physiological pH, iron-free Apotransferrin is not bound by TfR. But at acidic pH, such as exists in the endosome, Apotransferrin has considerable affinity for TfR. Thus, it remains bound to TfR and is recycled back to the cell surface where a neutral pH environment dissociates ligand from receptor. Each Tf molecule recycles 100 - 150 times during its lifetime (8 - 11). In addition to TfR, transferrin is reported to bind to cubulin, IGFBP3, microbial iron-binding proteins and liver-specific TfR2 (7, 12, 13, 14). Transferrin is variably glycosylated and the degree of sialylation is suggestive of certain clinical conditions (15). Finally, Tf is highly allelic and the gene codominant, with many single aa changes noted. Three general forms are known, based on standard electrophoretic mobility. Fast Tf is known as transferrin B, slow transferrin is transferrin D, and the middle migrating transferrin is type/variant C, the most common (16, 17). Mature human TF is 73% aa identical to both mouse and rat Tf, and 68% and 71% aa identical to bovine and equine Tf, respectively.

  1. Brus, C.M. et al. (2001) Nat. Struct. Biol. 4:919.
  2. Schaeffer, E. et al. (1987) Gene 56:109.
  3. MacGillivray, R.T.A. et al. (1983) J. Biol. Chem. 258:3543.
  4. Yang, F. et al. (1984) Proc. Natl. Acad. Sci. USA 81:2752.
  5. Uzan, G. et al. (1984) Biochem. Biophys. Res. Commun. 119:273.
  6. Zak, O. et al. (2002) Biochemistry 41:7416.
  7. Gomme, P.T. and K. B. McCann (2005) Drug Discov. Today 10:267.
  8. Liu, R. et al. (2003) Biochemistry 42:12447.
  9. Pakdaman, R. et al. (1999) J. Mol. Biol. 293:1273.
  10. Hemadi, M. et al. (2004) Biochemistry 43:1736.
  11. Aisen, P. et al. (2001) Int. J. Biochem. Cell Biol. 33:940.
  12. Kozyraki, R. et al. (2001) Proc. Natl. Acad. Sci. USA 98:12941.
  13. Boulton, I.C. et al. (1998) Biochem. J. 334:269.
  14. Robb, A. and M. Wessling-Resnick (2004) Blood 104:4294.
  15. Landberg, E. et al. (1995) Biochem. Biophys. Res. Commun. 210:267.
  16. Gorg, A. et al. (1983) Hum. Genet. 64:222.
  17. Bean, P. and J.B. Peter (1994) Clin. Chem. 40:2078.

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Publications for Apo-Transferrin (3188-AT)(6)

We have publications tested in 2 confirmed species: Human, Mouse.

We have publications tested in 2 applications: Bioassay, Reference Standard.


Filter By Application
Bioassay
(4)
Reference Standard
(1)
All Applications
Filter By Species
Human
(5)
Mouse
(1)
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Showing Publications 1 - 6 of 6.
Publications using 3188-AT Applications Species
Lau, KYC;Amadei, G;Zernicka-Goetz, M; Assembly of complete mouse embryo models from embryonic and induced stem cell types in vitro Nature protocols 2023-10-11 [PMID: 37821625] (Bioassay, Mouse) Bioassay Mouse
C Agliardi, FR Guerini, M Zanzottera, E Bolognesi, M Meloni, G Riboldazzi, R Zangaglia, A Sturchio, C Casali, C Di Lorenzo, B Minafra, M Clerici The VDR FokI (rs2228570) polymorphism is involved in Parkinson&#039;s disease Journal of the neurological sciences, 2021-08-03;428(0):117606. 2021-08-03 [PMID: 34365149] (Human) Human
KRQ Lim, A Bittel, R Maruyama, Y Echigoya, Q Nguyen, Y Huang, K Dzierlega, A Zhang, YW Chen, T Yokota DUX4 transcript knockdown with antisense 2&#039;-O-methoxyethyl gapmers for the treatment of facioscapulohumeral muscular dystrophy Mol Ther, 2020-10-15;0(0):. 2020-10-15 [PMID: 33068777] (Bioassay, Human) Bioassay Human
RM Giadone, DC Liberti, TM Matte, JD Rosarda, C Torres-Ara, S Ghosh, JK Diedrich, S Pankow, N Skvir, JC Jean, JR Yates, AA Wilson, LH Connors, DN Kotton, RL Wiseman, GJ Murphy Expression of Amyloidogenic Transthyretin Drives Hepatic Proteostasis Remodeling in an Induced Pluripotent Stem Cell Model of Systemic Amyloid�Disease Stem Cell Reports, 2020-07-30;0(0):. 2020-07-30 [PMID: 32735824] (Bioassay, Human) Bioassay Human
WF Zeno, AS Thatte, L Wang, WT Snead, EM Lafer, JC Stachowiak Molecular Mechanisms of Membrane Curvature Sensing by a Disordered Protein J. Am. Chem. Soc., 2019-06-20;0(0):. 2019-06-20 [PMID: 31180661] (Reference Standard, Human) Reference Standard Human
Staquicini FI, Ozawa MG, Moya CA, Driessen WH, Barbu EM, Nishimori H, Soghomonyan S, Flores LG, Liang X, Paolillo V, Alauddin MM, Basilion JP, Furnari FB, Bogler O, Lang FF, Aldape KD, Fuller GN, Höök M, Gelovani JG, Sidman RL, Cavenee WK, Pasqualini R, Arap W Systemic combinatorial peptide selection yields a non-canonical iron-mimicry mechanism for targeting tumors in a mouse model of human glioblastoma. J. Clin. Invest., 2010-12-22;121(1):161-73. 2010-12-22 [PMID: 21183793] (Bioassay, Human) Bioassay Human

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