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Complement Factor P (Properdin)

Aladdin

Catalog No.
C09-0826-834
Manufacturer No.
C501379-100μg
Manufacturer Name
Aladdin Scientific
Quantity
1
Unit of Measure
EA
Price: $923.01
List Price: $1,025.57

Extinction Coeff.A280 nm = 1.78 at 1.0 mg/mLMolecular weight53,000 Da (single chain)Purity>90% by SDS-PAGEGeneral DescriptionComplement factor P (properdin) is purified from normal human serum. Factor P is a 53,000 dalton cationic protein that

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Extinction Coeff.A280 nm = 1.78 at 1.0 mg/mLMolecular weight53,000 Da (single chain)Purity>90% by SDS-PAGEGeneral DescriptionComplement factor P (properdin) is purified from normal human serum. Factor P is a 53,000 dalton cationic protein that circulates in blood in the form of dimers, trimers and tetramers. It binds rapidly to C3b on surfaces where complement has begun to activate. Properdin binds most avidly to C3b,Bb the alternative pathway C3/C5 convertase, but also binds to C3b < C3b,B < C3b,Bb. Its primary function is to stabilize the C3b,Bb complex allowing increased alternative pathway activation (Pangburn, M.K., (1988); Nolan, K.F. and Reid, K.B.M. (1993)). Properdin enhances formation of the alternative pathway C3 convertase by increasing binding of factor B to P,C3b complexes.Thus, properdin is an accelerator (positive regulator) of complement activation. Properdin has recently been proposed to be able to also initiate activation of the alternative pathway by binding to the target surface and initiating C3/C5 convertase formation (Kemper C. and Hourcade D.E. (2008)).Physical Characteristics & StructureThe basic subunit of this protein is a 53,000 dalton single chain molecule which is composed of six thrombospondin-like repeat (TSR) domains. These basic units are linked at the ends (C-terminal to N-terminal) to form circular dimers, trimers, tetramers and perhaps higher forms in blood (Pangburn, M.K. (1989)). Electron microscopic images (Smith, C.A. et al. (1984)) have clearly demonstrated these structures. Higher oligomers of properdin are formed upon freeze thaw and perhaps during complement activation and were originally called “activated” properdin due to their enhanced ability to bind and activate complement. Properdin has a rare post-translational modification in that its tryptophan residues are highly mannosylated (Hartmann, S. and Hofsteenge, J. (2000)). There is also a single N-linked glycosylation site near the C-terminal. These contribute to a carbohydrate content estimated at 10%. Properdin is highly positively charged at neutral pH and has a pI greater than 9.5. It is one of the most positively charged proteins in blood (Morley, B.J. and Walport, M.J. (2000)).FunctionProperdin binds most avidly to C3b,Bb the alternative pathway C3/C5 convertase, but also binds to C3b < C3b,B < C3b,Bb. Its primary function is to stabilize the C3b,Bb complex allowing increased alternative pathway activation. Properdin enhances formation of the alternative pathway C3 convertase by increasing binding of factor B to P,C3b complexes. Thus, properdin is an accelerator (positive regulator) of complement activation.AssaysAssays depend on the ability of properdin to bind to clusters of C3b or to accelerate the activation of the alternative pathway. ELISA assays for protein may be performed by coating plates with excess C3b, binding properdin and detection with goat anti-Properdin. Functional assays are best performed using P-depleted serum and then measuring the accelerated lysis of rabbit erythrocytes in the presence of properdin and MgEGTA. Lysis does occur slowly in the absence of properdin so these assays must be timed assays to compare the rates of lysis with and without properdin. Assays for “activated” properdin consist of incubating properdin in NHS for extended periods of time (30 to 60 min) and measuring the residual C3 activity using C3-depleted serum and rabbit erythrocytes.In vivoBlood contains approximately 5 µg/mL properdin (Pangburn, M.K. (1989)). Properdin does not appear to be synthesized in the liver where most complement proteins are synthesized. It is primarily made by monocytes, T-cells and neutrophils. In neutrophils it is stored in granules that release the properdin in response to C5a, FMLP, IL8 and TNF-alpha.RegulationSee In vivo above.GeneticsThe gene for properdin is X-linked and resides on the short arm of the X chromosome between Xp11.3-Xp11.23. The gene is 6 kb is size with 10 exons. Accession numbers: Human (X70872, X70872.1, X57748, M83652, S49355), Mouse (X12905), Guinea pig (S81116).DeficienciesDeficiencies are rare and can be the result of a total lack of properdin protein in blood or the presence of immunochemically detectable, but functionally inactive properdin.DiseasesDeficiency of properdin results in recurrent fulminant meningococcal infections. Neisserial infections typically occur in young males, progress rapidly and can be fatal.Reoccurrences are rare probably due to the generation of protective antibodies during the first incident.Precautions/Toxicity/HazardsThis protein is purified from human serum, therefore precautions appropriate for handling any blood-derived product must be used even though the source was shown by certified tests to be negative for HBsAg, HTLV-I/II, STS, and for antibodies to HCV, HIV-1 and HIV-II.Hazard Code: B WGK Germany 3MSDS available upon request. Specifications and Purity: 1.0 mg/mLe, 0.22 µm filtered. Related Document: https://ald-pub-files.oss-cn-shanghai.aliyuncs.com/aladdinsci/pdp/sds/1/C501379-SCI_cb915805097ad9abe2d92d9c98799667.pdf.
UPC:
12352005
Condition:
New
Availability:
8-12 weeks
Weight:
1.06 Ounces
HazmatClass:
No
WeightUOM:
LB
MPN:
C501379-100μg
Product Size:
100μg


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