iC3b Antibody (Monoclonal - neoantigen)

A murine monoclonal antibody to a neo-epitope expressed on iC3b.

Product Specifications

Citations	26
Clonality	Monoclonal
Immnogen
Applications	See citations and technical data sheet for application info.
Concentration	≥ 1.0 mg/mL
Conjugate	Unconjugated
Cross Reactivity	Human

Technical Documents

Ordering Information

For Research Use Only in the United States. Not for use in diagnostic procedures.

Catalog Number	A209
Catalog Number (CE)	N/A
Size	100 µl
Price (USD)	$365.00
Price (EURO)	330,00 €

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Contact us

US Phone	+1 (858) 552 1100
EU Phone	+353 (91) 412 474
US Email	contact-us@quidelortho.com
EU Email	contact-emea@quidelortho.com

Specifications
Citations
Certificate of Analysis

Specifications

Description	A murine monoclonal antibody to a neo-epitope expressed on iC3b.
Size	100 µl
Concentration	≥ 1.0 mg/mL
Applications	See citations and technical data sheet for application info.
Form	Liquid. Borate Buffered Saline (pH 8.4 ± 0.2), with ≤ 0.1% Sodium Azide.
Clonality	Monoclonal
Immunogen	Purified human protein.
Conjugate	Unconjugated
Cross Reactivity	Human
Isotype	IgG2bk
Purity	> 95% by SDS PAGE
Source	Mouse
Specificity	This monoclonal antibody was raised against purified human iC3b. It is specific for a neo-antigen on iC3b.
Storage	Short term (30 days) 4˚C. Long term at or below –20˚C.
Background	Under normal conditions, activation of either of the complement pathways leads to the formation of C3 convertase enzymes which cleave C3 into two fragments C3a, an anaphylatoxin, and C3b.The C3b fragment has many biologic functions including promotion of phagocytosis and participation as a structural component in both the C3 and C5 convertase enzymes. These processes are under stringent control in vivo. One control mechanism involves a two-site cleavage of C3b by Factor I with the cooperation of Factor H or CR1 as cofactors. When cleaved in this way the biologic functions of C3b are lost. The resulting protein is termed iC3b.This fragment, in turn, has a host of new biologic activities. iC3b fragments, either in fluid phase or bound to biological surfaces, can interact with a variety of cell types expressing complement receptors (either CR2 or CR3). iC3b levels in fluid phase are elevated in a variety of disease states including Systemic Lupus Erythematosis, Rheumatoid Arthritis as well as in a variety of pathologic conditions including sepsis and Myocardial Infarct. Quidel’s monoclonal antibodies to complement antigens were prepared using standard techniques. They are purified from mouse ascites fluid via protein A affinity chromatography. 3 The specificity of the monoclonal antibody was established via a series of immunological techniques including ELISA, hemagglutination and RIA. Firstly, the antibody was shown by ELISA to bind to C3 antigens using highly pure, immobilized C3. Subsequent studies showed that this antibody agglutinates EC3bi but not EC3b or EC3d cells in an indirect hemagglutination assay. Further experiments showed that this antibody bound to radio-labeled purified iC3b but not to similarly labeled C3, C3b, C3d, or C3c.

Citations

Title	Year	Applications	Sample Species	Sample	Sample Details
Pneumolysin, PspA, and PspC Contribute to Pneumococcal Evasion of Early Innate Immune Responses During Bacteremia in Mice.	2007	WB	Bacteria	Pneumococci
Opsonization of apoptotic cells by autologous iC3b facilitates clearance by immature dendritic cells, down-regulates DR and CD86, and up-regulates CC chemokine receptor 7.	2002	Confocal Microscopy	Cell Culture	Jurkat Cells
Heme Interferes With Complement Factor I-Dependent Regulation by Enhancing Alternative Pathway Activation.	2021	ELISA	Human	Plasma	Sickel Cell Anemia
Complement Activation on Platelets Correlates with a Decrease in Circulating Immature Platelets in Patients with Immune Thrombocytopenic Purpura	2009	ELISA	Human	Plasma
Arabinosylation of recombinant human immunoglobulin-based protein therapeutics	2017	ELISA	Human	Serum
Inhibition of Immune Complex Complement Activation and Neutrophil Extracellular Trap Formation by Peptide Inhibitor of Complement C1.	2018	ELISA	Human	Serum
A monoclonal antibody targeting amyloid β (Aβ) restores complement factor I bioactivity: Potential implications in age-related macular degeneration and Alzheimer's disease	2018	ELISA	Human	Plasma	Age-Related Macular Degeneration
A monoclonal antibody targeting amyloid β (Aβ) restores complement factor I bioactivity: Potential implications in age-related macular degeneration and Alzheimer's disease	2018	ELISA	Human	Plasma	Alzheimer's Disease
Complement-dependent proinflammatory properties of the Alzheimer's disease beta-peptide.	1998	ELISA	Human	Amyloid-βeta peptides & NHS
Complement activation by heme as a secondary hit for atypical hemolytic uremic syndrome.	2013	FC	Human	HUVEC Cells	aHUS
Bacillus anthracis Spore Surface Protein BclA Mediates Complement Factor H Binding to Spores and Promotes Spore Persistence.	2016	FC	Human	Serum	B. anthracis incubated
Eculizumab treatment: stochastic occurrence of C3 binding to individual PNH erythrocytes.	2017	FC	Human	Red Blood Cells	PNH
Complement Receptor 3 Has Negative Impact on Tumor Surveillance through Suppression of Natural Killer Cell Function	2017	FC	Human	NK Cells
Complement activation in the Parkinson’s disease substantia nigra: an immunocytochemical study.	2006	ICC, IHC	Human	Brain Tissue
Plaque complement activation and cognitive loss in Alzheimer’s disease.	2008	ICC, IHC	Human	Brain Tissue
Sequential Increase in Complement Factor I, iC3b, and Cells Expressing CD11b or CD14 in Cutaneous Vasculitis.	2022	IHC	Human	Skin Tissue	Cutaneous Vasculitis
Spontaneous classical pathway activation and deficiency of membrane regulators render human neurons susceptible to complement lysis.	2000	IHC	Human	Brain Tissue	Fetal
Design and development of TT30, a novel C3d-targeted C3/C5 convertase inhibitor for treatment of human complement alternative pathway-mediated diseases	2011	IHC	Human	Lung Tissue	Asthmatic Alzheimer's
Design and development of TT30, a novel C3d-targeted C3/C5 convertase inhibitor for treatment of human complement alternative pathway-mediated diseases	2011	IHC	Human	Lung Tissue
Tumor necrosis-initiated complement activation stimulates proliferation of medulloblastoma cells.	2015	IHC	Human	Brain Tissue	Medullablastoma
quantitative lateral flow assay to detect complement activation in blood.	2015	Lateral Flow Assay	Human	Plasma
Complement receptor 3 mediates Aspergillus fumigatus internalization into alveolar epithelial cells with the increase of intracellular phosphatidic acid by activating FAK.	2021	WB	Human	Serum	Aspergillus incubated
Efficient complement-mediated clearance of immunosuppressed T cells by macrophages.	2023	IF	Human	T Cells	Immunosuppressed
Increased expression of complement C3c, iC3b and cells containing CD11b or CD14 in experimentally induced psoriatic lesion	2024	IHC	Human	Skin Tissue	Psoriasis
Increased expression of complement C3c, iC3b and cells containing CD11b or CD14 in experimentally induced psoriatic lesion	2024	ICC	Human	Keratinocytes	Psoriasis
Control of Entamoeba histolytica adherence involves metallosurface protease 1, an M8 family surface metalloprotease with homology to leishmanolysin.	2012	FC	Parasite	Entamoeba histolytica

Certificate of Analysis

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