Use your antibodies-online credentials, if available.
No Products on your Comparison List.
Your basket is empty.
Find out more
Show all species
Show all synonyms
Select your species
Human Complement Factor I ELISA Kit for Sandwich ELISA - ABIN415156
Peyvandi, Rossio, Ferrari, Lotta, Pontiggia, Ghiringhelli Borsa, Pizzuti, Donadelli, Piras, Cugno, Noris: Thrombotic microangiopathy without renal involvement: two novel mutations in complement-regulator genes. in Journal of thrombosis and haemostasis : JTH 2016
Show all 2 Pubmed References
Factor I-mediated generation of activated C3 fragments in the circulation is a critical determinant for the development of MPGN2 associated with factor H (show CFH ELISA Kits) deficiency.
This finding although rare does suggest that screening for chromosomal rearrangements affecting CFI should be undertaken in all aHUS patients particularly if the factor I level is unexplainably low.
Factor I binds C3b-Factor H (show CFH ELISA Kits) between Factor H (show CFH ELISA Kits) domains 2 and 3 and a reoriented C3b C-terminal domain and docks onto the first scissile bond, while stabilizing its catalytic domain for proteolytic activity.
Taken together, our data argue that multiple rare and ultra-rare alleles in CFI contribute to AMD (show AMD1 ELISA Kits) pathogenesis; they improve the precision of the assessment of the contribution of CFI to AMD (show AMD1 ELISA Kits)
Case Report: thrombotic microangiopathy with mutations in complement factor I and thrombomodulin (show THBD ELISA Kits).
Our results indicate that CFI polymorphisms are not significantly associated with VKH syndrome.
Patients with advanced atrophic AMD (show AMD1 ELISA Kits) carried these rare variants more frequently than patients with neovascular AMD (show AMD1 ELISA Kits) (11 of 93 [11.8%] vs 40 of 835 [4.8%]; P = .04).
Low FI levels are strongly associated with rare CFI variants and age-related macular degeneration.
A missense variant (p.V412M) in CFI was discovered in two Tunisian Jewish families with early-onset age-related macular degeneration.
Regulatory components of the alternative complement pathway in endothelial cell cytoplasm, factor H (show CFH ELISA Kits) and factor I, are not packaged in Weibel-Palade bodies.
In this study, the odds of AMD (show AMD1 ELISA Kits) were highest in those with deficient vitamin D status and 2 risk alleles for the CFH (show CFH ELISA Kits) and CFI genotypes, suggesting a synergistic effect between vitamin D status and complement cascade protein function.
This gene encodes a serine proteinase that is essential for regulating the complement cascade. The encoded preproprotein is cleaved to produce both heavy and light chains, which are linked by disulfide bonds to form a heterodimeric glycoprotein. This heterodimer can cleave and inactivate the complement components C4b and C3b, and it prevents the assembly of the C3 and C5 convertase enzymes. Defects in this gene cause complement factor I deficiency, an autosomal recessive disease associated with a susceptibility to pyogenic infections. Mutations in this gene have been associated with a predisposition to atypical hemolytic uraemic syndrome, a disease characterized by acute renal failure, microangiopathic hemolytic anemia and thrombocytopenia. Primary glomerulonephritis with immmune deposits is another condition associated with mutation of this gene.
complement factor I
, I factor (complement)
, complement factor 1
, C3B/C4B inactivator
, Konglutinogen-activating factor
, complement component I
, complement control protein factor I
, complement factor I heavy chain
, light chain of factor I
, complement component 1