MicroVue™ Bb Plus EIA

The MicroVue Bb Plus EIA kit measures the amount of the complement fragment Bb in human plasma or serum.


Product Specifications

Citations45
Specimen

Serum 25 μL, EDTA Plasma 50 μL

LLOQ0.033 μg/mL
ULOQ0.836 μg/mL
Assay Time1.5 hours
Cross Reactivity

Cynomolgous monkey, Pig, Rhesus monkey

Ordering Information

For In Vitro Diagnostic Use.
Catalog NumberA027
Catalog Number (CE) 
Size96 wells/test
Price (USD)$725.00
Price (EURO)650,00 €

Contact us

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

Specifications

Description

The MicroVue Bb Plus EIA kit measures the amount of the complement fragment Bb in human plasma or serum.

Size96 wells/test
Form

96 well plate with 12 eight-well strips in a resealable foil pouch

SpecimenSerum 25 μL, EDTA Plasma 50 μL
Limit of Detection (LOD)0.018 μg/mL
Lower Limit of Quantitation (LLOQ)0.033 μg/mL
Upper Limit of Quantitation (ULOQ)0.836 μg/mL
Intra Assay2.4–4.0%
Inter Assay6.2–9.1%
Standards5
Controls2
Sample Values

Serum 0.0–7.6 μg/mL, EDTA Plasma 0.3–1.7 μg/mL

Assay Time1.5 hours
Cross Reactivity

Cynomolgous monkey, Pig, Rhesus monkey

Storage

Store the unopened kit at 2°C to 8°C. Refer to Product Insert for additional storage details.

Background

The alternative complement pathway provides innate protection against microbial agents in the absence of specific antibody. The activation of this complement pathway can be triggered by a variety of substances including microbial polysaccharides or lipids, gram-negative bacterial lipopolysaccharides, and surface determinants present on some viruses, parasites, virally infected mammalian cells, and cancer cells. In autoimmune diseases, the alternative complement pathway may contribute directly to tissue damage. A centrally important reaction that occurs during alternative pathway activation is the conversion of the 93 Kd molecular weight Factor B zymogen to an active proteolytic enzyme. This is accomplished in a two-step reaction. During the first reaction step the Factor B forms a magnesium-dependent complex with C3(H20) or C3b.4 The C3(H20),B complex is formed only in fluid-phase while the C3b,B complex can be formed either in fluid-phase or on a target surface. Factor B, which is present in the C3(H20),B or the C3b,B complex, is cleaved into the Ba (33 Kd) and Bb (60 Kd) fragments in the second reaction step by the alternative pathway enzyme, Factor D. The resulting C3b,Bb bimolecular complex is the C3 convertase enzyme of the alternative pathway. The Bb subunit is the catalytically active site of the complex that is capable of cleaving C3 to C3a and C3b fragments. The additional C3b fragments produced in this manner may form the C3b,Bb,C3b trimolecular complex that is the C5 convertase enzyme of the alternative pathway. This C5 convertase is capable of cleaving C5 to C5a and C5b fragments. The C3 and C5 convertases of the alternative pathway can be stabilized by Factor P (also called Properdin), a component of the alternative pathway normally present in human plasma or serum, or by C3 nephritic factor, an autoantibody produced in some patients experiencing extensive alternative pathway activation. The C3 and C5 convertases of the alternative pathway can be dissociated, and thereby inactivated, by spontaneous decay dissociation, or by the binding of Factor H or Complement Receptor 1 (CR1 ). The Bb fragment that is dissociated from either convertase retains some biological activities, e.g., retention of functional hemolytic activity, the ability to induce macrophage- spreading, and plasminogen activation. Although alternative pathway activation is thought to occur primarily in the absence of specific antibody, many situations arise in which alternative pathway activation can occur as the result of classical pathway activation. For example, immune complexes that are present in autoimmune disease patients can trigger classical complement pathway activation with resultant production of C3b fragments. As described above, these C3b molecules are capable of binding Factor B and initiating its cleavage into the Ba and Bb fragments. Thus, alternative pathway activation can occur in antibody-mediated autoimmune disease states and may contribute significantly to enhanced complement activation and concomitant tissue destruction. By assessing Factor B cleavage products in test specimens, one can estimate the extent of alternative pathway utilization occurring at the time of sample collection in the disease state under investigation. The MicroVue Bb Plus EIA provides a simple, rapid, non-radioactive, highly specific, and quantitative procedure for measuring Factor B activation. It is ideal for investigations involving the role or status of the alternative complement pathway in numerous research and clinical settings, and for monitoring the generation of Bb in vitro.

Citations

TitleYearApplicationsSample SpeciesSampleSample Details

Decrease in multiple complement protein levels is associated with the development of islet autoimmunity and type 1 diabetes.

2023ELISAHuman

Plasma

Diabetes

Persistently elevated complement alternative pathway biomarkers in COVID-19 correlate with hypoxemia and predict in-hospital mortality.

2022ELISAHuman

Plasma

COVID-19

Complement activation during cardiopulmonary bypass and association with clinical outcomes.

2022ELISAHuman

Plasma

Cardiopulmonary bypass

Indices of complement activation and coagulation changes in trauma patients

2022ELISAHuman

Plasma

Trauma

Persistently elevated complement alternative pathway biomarkers in COVID-19 correlate with hypoxemia and predict in-hospital mortality.

2022ELISAHuman

Serum

COVID-19

Comparison of Complement Pathway Activation in Autoimmune Glomerulonephritis.

2022ELISAHuman

Urine

AAV, FSGS, IgAN, MN, and LN

von Willebrand factor variants in C3 glomerulopathy: A Chinese cohort study.

2021ELISAHuman

Plasma

C3G

Elevated complement mediator levels in endothelial-derived plasma exosomes implicate endothelial innate inflammation in diminished brain function of aging humans.

2021ELISAHuman

Plasma

N/A

Dendrimer end-terminal motif-dependent evasion of human complement and complement activation through IgM hitchhiking.

2021ELISAHuman

Plasma

N/A

Complement levels at admission as a reflection of coronavirus disease 2019 (COVID-19) severity state.

2021ELISAHuman

Serum

COVID-19

Complement dysregulation is associated with severe COVID-19 illness.

2021ELISAHuman

Serum

COVID-19

von Willebrand factor variants in C3 glomerulopathy: A Chinese cohort study.

2021ELISAHuman

Urine

C3G

Complement Activation Profile of Patients With Primary Focal Segmental Glomerulosclerosis.

2020ELISAHuman

Plasma

FSGS

Interrelationship between ADAMTS13 activity, von Willebrand factor, and complement activation in remission from immune-mediated trhrombotic thrombocytopenic purpura.

2020ELISAHuman

Plasma

Immune‐mediated thrombotic thrombocytopenic purpura

Subvisible Particles in IVIg Formulations Activate Complement in Human Serum.

2020ELISAHuman

Serum

IVIg formulations

Complement Activation Profile of Patients With Primary Focal Segmental Glomerulosclerosis.

2020ELISAHuman

Serum

FSGS

Cloaking Silica Nanoparticles with Functional Protein Coatings for Reduced Complement Activation and Cellular Uptake.

2020ELISAHuman

Serum

SiNP coated proteins

Measuring Circulating Complement Activation Products in Myeloperoxidase- and Proteinase 3-Antineutrophil Cytoplasmic Antibody-Associated Vasculitis.

2019ELISAHuman

Plasma

ANCA-AAV

Prognostic utility of ADAMTS13 activity for the atypical hemolytic uremic syndrome (aHUS) and comparison of complement serology between aHUS and thrombotic thrombocytopenic purpura.

2019ELISAHuman

Plasma

aHUS

Clinical Value of Complement Activation Biomarkers in Overt Diabetic Nephropathy

2019ELISAHuman

Urine

Diabetic nephropathy

Complement activation predicts adverse pregnancy outcome in patients with systemic lupus erythematosus and/or antiphospholipid antibodies

2018ELISAHuman

Serum

N/A

Immunological response to nitroglycerin-loaded shear-responsive liposomes in vitro and in vivo

2017ELISAHuman

Serum

N/A

Activation of Human Complement System by Dextran-Coated Iron Oxide Nanoparticles Is Not Affected by Dextran/Fe Ratio, Hydroxyl Modifications, and Crosslinking.

2016ELISAHuman

Serum

N/A

Complement Split Products in Amniotic Fluid in Pregnancies Subsequently Developing Early-Onset Preeclampsia

2015ELISAHuman

Amniotic Fluid

N/A

Activation of the alternative pathway of complement during the acute phase of typical haemolytic uraemic syndrome

2015ELISAHuman

Plasma

Stx-HUS

Plasma complement factor H is associated with disease activity of patients with ANCA-associated vasculitis

2015ELISAHuman

Plasma

N/A

Nanoparticle biointerfacing by platelet membrane cloaking

2015ELISAHuman

Serum

Nanoparticles incubated

Genetic engineering strategies to prevent the effects of antibody and complement on xenogeneic chondrocytes

2015ELISAHuman

Serum

N/A

Complement factor B activation in patients with preeclampsia

2015ELISAHuman

Umbillical cord blood

N/A

Multifunctional silk-heparin biomaterials for vascular tissue engineering applications

2014ELISAHuman

Plasma

N/A

Clinicopathological characteristics and outcomes of Chinese patients with scanty immune deposits lupus nephritis: a large cohort study from a single center

2014ELISAHuman

Plasma

Lupus Nephritis

Defining the complement biomarker profile of C3 glomerulopathy

2014ELISAHuman

Plasma

C3G

Mechanisms of complement activation by dextran-coated superparamagnetic iron oxide (SPIO) nanoworms in mouse versus human serum

2014ELISAHuman

Serum

SPIO nanoworms

In Vitro Hematological and In Vivo Vasoactivity Assessment of Dextran Functionalized Graphene

2013ELISAHuman

Plasma

N/A

Elevated Properdin and Enhanced Complement Activation in First-Degree Relatives of South Asian Subjects With Type 2 Diabetes

2012ELISAHuman

Plasma

N/A

Mannose binding lectin is required for alphavirus-induced arthritis/myositis

2012ELISAHuman

Synovial fluid

N/A

Macrophage scavenger receptor A mediates the uptake of gold colloids by macrophages in vitro

2011ELISAHuman

Plasma

N/A

Heightened measures of immune complex and complement function and immune complex-mediated granulocyte activation in human lymphatic filariasis

2011ELISAHuman

Plasma

Lymphatic filariasis

Complement activation is responsible for acute toxicities in rhesus monkeys treated with a phosphorothioate oligodeoxynucleotide

2002ELISACynomolgus Monkey

Serum

N/A

Evidence for activation of the alternative complement pathway in patients with juvenile rheumatoid arthritis

2000ELISAHuman

Plasma

Rheumatoid Arthritis

Effects of Synthetic Oligonucleotides on human complement and coagulation

1997ELISAHuman

Plasma

N/A

Sensitivity and Specificity of plasma and urine complement split products as indicators of lupus disease activity

1996ELISAHuman

Plasma

Systemic Lupus Erythematosus

Complement activation during painful crisis in sickle cell anemia

1995ELISAHuman

Plasma

Sickel Cell Anemia

Complement activation and immune complexes in children with polyarticular juvenile rhuematoid arthritis: a longitudinal study

1994ELISAHuman

Plasma

Rheumatoid Arthritis

Assessment of Disease activity and impending flare in patients with systemic lupus erythematosis

1992ELISAHuman

Plasma

Systemic Lupus Erythematosus