Acute-phase protein alpha 1-anti-trypsin: diverting injurious innate and adaptive immune responses from non-authentic threats

Acute-phase protein alpha 1-anti-trypsin: diverting injurious innate and adaptive immune responses from non-authentic threats

One would assume that the anti-inflammatory activity of alpha 1-anti-trypsin (AAT) is the result of inhibiting neutrophil enzymes. However, AAT exhibits tolerogenic activities that are difficult to explain by serine-protease inhibition or by reduced inflammatory parameters. Targets outside the serin...

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Veröffentlicht in:Clinical and experimental immunology 2015-02, Vol.179 (2), p.161-172
Hauptverfasser: Guttman, O, Baranovski, B M, Schuster, R, Kaner, Z, Freixo-Lima, G S, Bahar, N, Kalay, N, Mizrahi, MI, Brami, I, Ochayon, DE, Lewis, E C
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container_end_page 172
container_issue 2
container_start_page 161
container_title Clinical and experimental immunology
container_volume 179
creator Guttman, O
Baranovski, B M
Schuster, R
Kaner, Z
Freixo-Lima, G S
Bahar, N
Kalay, N
Mizrahi, MI
Brami, I
Ochayon, DE
Lewis, E C
description One would assume that the anti-inflammatory activity of alpha 1-anti-trypsin (AAT) is the result of inhibiting neutrophil enzymes. However, AAT exhibits tolerogenic activities that are difficult to explain by serine-protease inhibition or by reduced inflammatory parameters. Targets outside the serine-protease family have been identified, supporting the notion that elastase inhibition, the only functional factory release criteria for clinical-grade AAT, is over-emphasized. Non-obvious developments in the understanding of AAT biology disqualify it from being a straightforward anti-inflammatory agent: AAT does not block dendritic cell activities, nor does it promote viral and tumour susceptibilities, stunt B lymphocyte responses or render treated patients susceptible to infections; accordingly, outcomes of elevated AAT do not overlap those attained by immunosuppression. Aside from the acute-phase response, AAT rises during the third trimester of pregnancy and also in advanced age. At the molecular level, AAT docks onto cholesterol-rich lipid-rafts and circulating lipid particles, directly binds interleukin (IL)-8, ADAM metallopeptidase domain 17 (ADAM17) and danger-associated molecular pattern (DAMP) molecules, and its activity is lost to smoke, high glucose levels and bacterial proteases, introducing a novel entity - 'relative AAT deficiency'. Unlike immunosuppression, AAT appears to help the immune system to distinguish between desired responses against authentic threats, and unwanted responses fuelled by a positive feedback loop perpetuated by, and at the expense of, inflamed injured innocent bystander cells. With a remarkable clinical safety record, AAT treatment is currently tested in clinical trials for its potential benefit in a variety of categorically distinct pathologies that share at least one common driving force: cell injury.
doi_str_mv 10.1111/cei.12476
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title Acute-phase protein alpha 1-anti-trypsin: diverting injurious innate and adaptive immune responses from non-authentic threats
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