Anti-neutrophil cytoplasmic antibody
[Image:P anca.jpg|thumb|Perinuclear staining typical of p-ANCA]
[Image:C anca.jpg|thumb|The granular, cytoplasmic staining pattern of c-ANCA]
Anti-neutrophil cytoplasmic antibodies are a group of autoantibodies, mainly of the IgG type, against antigens in the cytoplasm of neutrophils and monocytes. They are detected as a blood test in a number of autoimmune disorders, but are particularly associated with systemic vasculitis, so called ANCA-associated vasculitides.
ANCA IF patterns
Immunofluorescence on ethanol-fixed neutrophils is used to detect ANCA, although formalin-fixed neutrophils may be used to help differentiate ANCA patterns. ANCA can be divided into four patterns when visualised by IF: cytoplasmic ANCA, C-ANCA, perinuclear ANCA and atypical ANCA, also known as x-ANCA. c-ANCA shows cytoplasmic granular fluorescence with central interlobular accentuation. C-ANCA shows cytoplasmic staining that is usually uniform and has no interlobular accentuation. p-ANCA has three subtypes: classical p-ANCA, p-ANCA without nuclear extension and granulocyte specific-antinuclear antibody. Classical p-ANCA shows perinuclear staining with nuclear extension, p-ANCA without nuclear extension has perinuclear staining without nuclear extension, and GS-ANA shows nuclear staining on granulocytes only. a-ANCA often shows combinations of both cytoplasmic and perinuclear staining.ANCA antigens
The c-ANCA antigen is specifically proteinase 3. p-ANCA antigens include myeloperoxidase and bacterial permeability increasing factor Bactericidal/permeability-increasing protein. Other antigens exist for c-ANCA ; however, many are as yet unknown. Classical p-ANCA occurs with antibodies directed to MPO. p-ANCA without nuclear extension occurs with antibodies to BPI, cathepsin G, elastase, lactoferrin and lysozyme. GS-ANA are antibodies directed to granulocyte-specific nuclear antigens. Atypical ANCA are thought to be antigens similar to those of the p-ANCAs; however, they may occur due to differences in neutrophil processing.Other less common antigens include HMG1, HMG2, alpha enolase, catalase, beta glucuronidase, azurocidin, actin and h-lamp-2.
ELISA
Enzyme-linked immunosorbent assay is used in diagnostic laboratories to detect ANCAs. Although IF can be used to screen for many ANCAs, ELISA is used to detect antibodies to individual antigens. The most common antigens used on an ELISA microtitre plate are MPO and PR3, which are usually tested for after a positive IF test.Development
It is poorly understood how ANCA are developed, although several hypotheses have been suggested. There is probably a genetic contribution, particularly in genes controlling the level of immune response, although genetic susceptibility is likely to be linked to an environmental factor, some possible factors including vaccination or exposure to silicates. Two possible mechanisms of ANCA development are postulated, although neither of these theories answers the question of how the different ANCA specificities are developed, and there is much research still being undertaken on the development of ANCA.Theory of molecular mimicry
Microbial superantigens are molecules expressed by bacteria and other microorganisms that have the power to stimulate a strong immune response by activation of T-cells. These molecules generally have regions that resemble self-antigens that promote a residual autoimmune response – this is the theory of molecular mimicry. Staphylococcal and streptococcal superantigens have been characterized in autoimmune diseases – the classical example in post group A streptococcal rheumatic heart disease, where there is similarity between M proteins of Streptococcus pyogenes to cardiac myosin and laminin. It has also been shown that up to 70% of patients with granulomatosis with polyangiitis are chronic nasal carriers of Staphylococcus aureus, with carriers having an eight times increased risk of relapse. This would therefore be considered a type II hypersensitivity reaction.Theory of defective apoptosis
Neutrophil apoptosis, or programmed cell death, is vital in controlling the duration of the early inflammatory response, thus restricting damage to tissues by the neutrophils. ANCA may be developed either via ineffective apoptosis or ineffective removal of apoptotic cell fragments, leading to the exposure of the immune system to molecules normally sequestered inside the cells. This theory solves the paradox of how it could be possible for antibodies to be raised against the intracellular antigenic targets of ANCA.Role in disease
Disease associations
ANCAs are associated with small vessel vasculitides including granulomatosis with polyangiitis, microscopic polyangiitis, primary pauci-immune necrotizing crescentic glomerulonephritis, eosinophilic granulomatosis with polyangiitis and drug induced vasculitides. ANCA-associated vasculitides have new classification criteria, updated in 2022.PR3-directed c-ANCA is present in 80-90% of granulomatosis with polyangiitis, 20-40% of microscopic polyangiitis, 20-40% of pauci-immune crescentic glomerulonephritis and 35% of eosinophilic granulomatosis with polyangiitis. c-ANCA is present in 80% of cystic fibrosis and also in inflammatory bowel disease, primary sclerosing cholangitis and rheumatoid arthritis. p-ANCA with MPO specificity is found in 50% of microscopic polyangiitis, 50% of primary pauci-immune necrotizing crescentic glomerulonephritis and 35% of eosinophilic granulomatosis with polyangiitis. p-ANCA with specificity to other antigens are associated with inflammatory bowel disease, rheumatoid arthritis, drug-induced vasculitis, autoimmune liver disease, drug-induced syndromes and parasitic infections. Atypical ANCA is associated with drug-induced systemic vasculitis, inflammatory bowel disease and rheumatoid arthritis. The ANCA-positive rate is much higher in patients with type 1 diabetes mellitus than in healthy individuals.
Levamisole, which is a common adulterant of cocaine, can cause an ANCA positive vasculitis.
The presence or absence of ANCA cannot indicate the presence or absence of disease, and results are correlated with clinical features. The association of ANCA and disease activity remains controversial; however, the reappearance of ANCA after treatment can indicate a relapse.