Leinco Technologies

Anti-Human CD47 (Magrolimab)

Product Code:
 
LEI-C1070
Product Group:
 
Primary Antibodies
Host Type:
 
HEK 293 cells
Antibody Clonality:
 
Recombinant Antibody
Antibody Clone:
 
Hu5F9-G4
Regulatory Status:
 
RUO
Target Species:
 
Human
Applications:
  • Enzyme-Linked Immunosorbent Assay (ELISA)
  • Functional Study
Shipping:
 
2 - 8°C Wet Ice
Storage:
 
Functional grade biosimilar antibodies may be stored sterile as received at 2-8°C for up to one month. For longer term storage aseptically aliquot in working volumes without diluting and store at -80°C. Avoid Repeated Freeze Thaw Cycles.
 

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CodeSizePrice
LEI-C1070-1.0mg1.0 mg£207.00
Quantity:
LEI-C1070-5.0mg5.0 mg£532.00
Quantity:
LEI-C1070-25mg25 mg£1,677.00
Quantity:
LEI-C1070-50mg50 mg£2,902.00
Quantity:
LEI-C1070-100mg100 mg£4,066.00
Quantity:
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This product comes from: US.
Typical lead time: 14-21 working days.
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Further Information

Antigen Distribution:
CD47 is a cell-surface protein with ubiquitous expression that is also overexpressed on cancer cells.
Concentration:
? 5.0 mg/ml
Conjugate/Tag/Label:
Purified No Carrier Protein
Format:
This biosimilar antibody is aseptically packaged and formulated in 0.01 M phosphate buffered saline (150 mM NaCl) PBS pH 7.2 - 7.4 with no carrier protein, potassium, calcium or preservatives added. Due to inherent biochemical properties of antibodies, certain products may be prone to precipitation over time. Precipitation may be removed by aseptic centrifugation and/or filtration.
Formulation:
This biosimilar antibody is aseptically packaged and formulated in 0.01 M phosphate buffered saline (150 mM NaCl) PBS pH 7.2 - 7.4 with no carrier protein, potassium, calcium or preservatives added. Due to inherent biochemical properties of antibodies, certain products may be prone to precipitation over time. Precipitation may be removed by aseptic centrifugation and/or filtration.
Immunogen:
Humanized antibody derived from mouse clone 5F9
Long Description:
In healthy cells, signal molecules stimulate programmed cell removal via various proteins, phospholipids, and abnormal glycosylation1. However, cancer cells are able to evade phagocytic elimination, the normal method of cell removal by the innate immune system1, due to the inhibitory antiphagocytic ?don?t eat me? signal generated by CD472. The CD47 signal, which is overexpressed on cancer cells3, enables immune evasion from macrophages and other phagocytes2. Since CD47 overexpression has been found on all known solid tumors and leukemias, it is a universal blocking target for cancer immunotherapy1. Magrolimab was generated by immunizing Balb/c mice with a recombinant human-mouse CD47/mFC fusion protein composed of a cDNA fragment of human CD47 encoding the extracellular domain fused to mouse Fc1. Hybridomas were created by fusing spleen cells with SP2/0 cells, and screening resulted in clone 5F9. Humanization of mouse anti-CD47 5F9 was performed by CDR grafting onto a human IgG4 scaffold to minimize recruitment of antibody Fc-dependent effector functions. Magrolimab does not induce antibody-dependent cellular cytotoxicity, complement-dependent cytotoxicity, or apoptosis. Additionally, residue optimization was performed and the human IgG4 heavy chain constant region was modified by a Ser228Pro substitution to reduce the rate of Fab arm exchange, which can occur in human IgG4 molecules. Magrolimab blocks the interaction between CD47 and one of its ligands, signal regulatory protein alpha (SIRPα)1. As a result, magrolimab is able to induce potent macrophage-mediated phagocytosis of primary human acute myeloid leukemia cells1, HER2+ breast cancer cells4, and lymphoma cells5, either on its own or in combination with other antibodies.
NCBI Gene:
961
Purity:
?95% by SDS Page, ?95% monomer by analytical SEC
Target:
CD47

References

1. Liu J, Wang L, Zhao F, et al. PLoS One. 10(9):e0137345. 2015. 2. Advani R, Flinn I, Popplewell L, et al. N Engl J Med. 379(18):1711-1721. 2018. 3. Maute R, Xu J, Weissman IL. Immunooncol Technol. 13:100070. 2022. 4. Upton R, Banuelos A, Feng D, et al. Proc Natl Acad Sci U S A. 118(29):e2026849118. 2021. 5. Zeller T, Lutz S, M?nnich IA, et al. Front Immunol. 13:929339. 2022. 6. Sikic BI, Lakhani N, Patnaik A, et al. J Clin Oncol. 37(12):946-953. 2019.