Due to the central role that factor H plays in the regulation of complement, there are a number of clinical implications arising from aberrant factor H activity. Overactive factor H may result in reduced complement activity on pathogenic cells – increasing susceptibility to microbial infections. Underactive factor H may result in increased complement activity on healthy host cells – resulting in autoimmune diseases. It is not surprising, therefore, that rare
mutations or common
single nucleotide polymorphisms (SNPs) in the complement factor H gene (CFH) often result in pathologies. Moreover, the complement inhibitory activities of factor H, and other complement regulators, are often used by pathogens to increase
virulence.
Age-related macular degeneration In 2005, several independent research groups identified an SNP in CFH, which results in the protein change p.Y402H, as a risk factor for
Age Related Macular Degeneration (AMD) present in around a third of Europeans. Although its allele frequency varies considerably between different populations, Y402H has been consistently associated with AMD onset and progression. an integral part of the outer
Blood-retinal barrier and a major site of early AMD. Further studies suggested that haploinsufficiency of FHL-1 lead to the manifestation of an AMD-like disease at a significantly earlier age. However, the genetic variants in CFH with the greatest effect on an individual's risk of AMD have been shown to affect CCPs 1 to 4, which are involved in dampening the effects of the alternative pathway of complement. Variation in other genes of the regulators of complement activation locus, such as complement factor H-related genes, as well as in other complement proteins (e.g. factor I, C2/factor B, and C3) have also been associated with greater AMD risk. Gemini Therapeutics merged with Disc Medicine in 2022 Other companies currently focusing on developing FH, FHL-1, or variations thereof, as therapeutics for treating AMD, include Character Biosciences Inc, and 4D Molecular Therapeutics
Atypical hemolytic uremic syndrome Hemolytic uremic syndrome (HUS) is a disease associated with microangiopathic hemolytic anemia, thrombocytopenia, and acute renal failure. It can be either acquired (e.g. following infection with shigatoxigenic
Escherichia coli), or inherited (also known as atypical hemolytic uremic syndrome, aHUS). aHUS has been strongly linked to mutations in genes of the complement system, especially factor H.
Schizophrenia Alterations in the immune response are involved in pathogenesis of many neuropsychiatric disorders including
schizophrenia. Recent studies indicated alterations in the
complement system, including those which may result in the overactivation of the
alternative complement pathway, may predispose to schizophrenia. For example, the CFH SNP rs424535 (2783-526T>A) was positively associated with schizophrenia.
Ischemic stroke It was found that rs800292(184G >A) SNP was positively associated with stroke and rs800912 minor allele of the CFH gene might be considered as a risk factor for ischemic stroke.
Francisella tularensis;
Haemophilus influenzae;
Neisseria gonorrhoeae;
N. meningitidis;
Streptococcus pneumoniae; The Gram-negative bacterium
B. burgdorferi has five factor H–binding proteins: CRASP-1, CRASP-2, CRASP-3, CRASP-4 and CRASP-5. Each CRASP protein also binds
plasminogen. It is possible that the allele frequency of CFH variants across the globe reflects selective pressure from infectious diseases. == Interactions ==