Indirect effect of alpha-1-antitrypsin on endotoxin-induced IL-1β secretion from human PBMCs

Janciauskiene, Sabina; Tumpara, Srinu; Schebb, Nils Helge; Buettner, Falk F.R.; Mainka, Malwina; Sivaraman, Kokilavani; Immenschuh, Stephan; Grau, Veronika; Welte, Tobias; Olejnicka, Beata

Indirect effect of alpha-1-antitrypsin on endotoxin-induced IL-1β secretion from human PBMCs

Mark

Janciauskiene, Sabina ^LU ; Tumpara, Srinu ; Schebb, Nils Helge ; Buettner, Falk F.R. ; Mainka, Malwina ; Sivaraman, Kokilavani ; Immenschuh, Stephan ; Grau, Veronika ; Welte, Tobias and Olejnicka, Beata ^LU (2022) In Frontiers in Pharmacology 13.

Abstract: Human alpha-1-antitrypsin (AAT) encoded by the SERPINA1 gene, is an acute phase glycoprotein that regulates inflammatory responses via both protease inhibitory and non-inhibitory activities. We previously reported that AAT controls ATP-induced IL-1β release from human mononuclear cells by stimulating the release of small bioactive molecules. In the current study, we aimed to elucidate the identity of these putative effectors released from human PBMCs in response to AAT, which may inhibit the LPS-induced release of IL-1β. We pre-incubated human PBMCs alone or with different preparations of AAT (4 mg/ml) for 30 min at 37°C, 5% CO₂, and collected cell supernatants filtered through centrifugal filters (cutoff 3 kDa) to eliminate... (More); Human alpha-1-antitrypsin (AAT) encoded by the SERPINA1 gene, is an acute phase glycoprotein that regulates inflammatory responses via both protease inhibitory and non-inhibitory activities. We previously reported that AAT controls ATP-induced IL-1β release from human mononuclear cells by stimulating the release of small bioactive molecules. In the current study, we aimed to elucidate the identity of these putative effectors released from human PBMCs in response to AAT, which may inhibit the LPS-induced release of IL-1β. We pre-incubated human PBMCs alone or with different preparations of AAT (4 mg/ml) for 30 min at 37°C, 5% CO₂, and collected cell supernatants filtered through centrifugal filters (cutoff 3 kDa) to eliminate AAT and other high molecular weight substances. Supernatants passed through the filters were used to culture PBMCs isolated from the autologous or a heterologous donors with or without adding LPS (1 μg/ml) for 6 h. Unexpectedly, supernatants from PBMCs pre-incubated with AAT (Zemaira^®), but not with other AAT preparations tested or with oxidized AAT (Zemaira^®), lowered the LPS-induced release of IL-1β by about 25%–60% without affecting IL1B mRNA. The reversed-phase liquid chromatography coupled with mass spectrometry did not confirm the hypothesis that small pro-resolving lipid mediators released from PBMCs after exposure to AAT (Zemaira^®) are responsible for lowering the LPS-induced IL-1β release. Distinctively from other AAT preparations, AAT (Zemaira^®) and supernatants from PBMCs pre-treated with this protein contained high levels of total thiols. In line, mass spectrometry analysis revealed that AAT (Zemaira^®) protein contains freer Cys232 than AAT (Prolastin^®). Our data show that a free Cys232 in AAT is required for controlling LPS-induced IL-1β release from human PBMCs. Further studies characterizing AAT preparations used to treat patients with inherited AAT deficiency remains of clinical importance.
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Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/98cc8d1b-3f80-4ef0-8fd3-b94ece3bef5d

author

Janciauskiene, Sabina ^LU ; Tumpara, Srinu ; Schebb, Nils Helge ; Buettner, Falk F.R. ; Mainka, Malwina ; Sivaraman, Kokilavani ; Immenschuh, Stephan ; Grau, Veronika ; Welte, Tobias and Olejnicka, Beata ^LU

organization

publishing date

2022-09

type

Contribution to journal

publication status

published

subject

Rheumatology and Autoimmunity

keywords

alpha-1-antitrypsin, Cytokines, Interleukin-1β, LPS, mass-spectrometry, PBMCs, supernatants, total thiols

in

Frontiers in Pharmacology

volume

13

article number

995869

publisher

Frontiers Media S. A.

external identifiers

pmid:36249781
scopus:85139830022

ISSN

1663-9812

DOI

10.3389/fphar.2022.995869

language

English

LU publication?

yes

id

98cc8d1b-3f80-4ef0-8fd3-b94ece3bef5d

date added to LUP

2022-12-16 10:48:22

date last changed

2024-04-03 20:45:31

@article{98cc8d1b-3f80-4ef0-8fd3-b94ece3bef5d,
  abstract     = {{<p>Human alpha-1-antitrypsin (AAT) encoded by the SERPINA1 gene, is an acute phase glycoprotein that regulates inflammatory responses via both protease inhibitory and non-inhibitory activities. We previously reported that AAT controls ATP-induced IL-1β release from human mononuclear cells by stimulating the release of small bioactive molecules. In the current study, we aimed to elucidate the identity of these putative effectors released from human PBMCs in response to AAT, which may inhibit the LPS-induced release of IL-1β. We pre-incubated human PBMCs alone or with different preparations of AAT (4 mg/ml) for 30 min at 37°C, 5% CO<sub>2</sub>, and collected cell supernatants filtered through centrifugal filters (cutoff 3 kDa) to eliminate AAT and other high molecular weight substances. Supernatants passed through the filters were used to culture PBMCs isolated from the autologous or a heterologous donors with or without adding LPS (1 μg/ml) for 6 h. Unexpectedly, supernatants from PBMCs pre-incubated with AAT (Zemaira<sup>®</sup>), but not with other AAT preparations tested or with oxidized AAT (Zemaira<sup>®</sup>), lowered the LPS-induced release of IL-1β by about 25%–60% without affecting IL1B mRNA. The reversed-phase liquid chromatography coupled with mass spectrometry did not confirm the hypothesis that small pro-resolving lipid mediators released from PBMCs after exposure to AAT (Zemaira<sup>®</sup>) are responsible for lowering the LPS-induced IL-1β release. Distinctively from other AAT preparations, AAT (Zemaira<sup>®</sup>) and supernatants from PBMCs pre-treated with this protein contained high levels of total thiols. In line, mass spectrometry analysis revealed that AAT (Zemaira<sup>®</sup>) protein contains freer Cys232 than AAT (Prolastin<sup>®</sup>). Our data show that a free Cys232 in AAT is required for controlling LPS-induced IL-1β release from human PBMCs. Further studies characterizing AAT preparations used to treat patients with inherited AAT deficiency remains of clinical importance.</p>}},
  author       = {{Janciauskiene, Sabina and Tumpara, Srinu and Schebb, Nils Helge and Buettner, Falk F.R. and Mainka, Malwina and Sivaraman, Kokilavani and Immenschuh, Stephan and Grau, Veronika and Welte, Tobias and Olejnicka, Beata}},
  issn         = {{1663-9812}},
  keywords     = {{alpha-1-antitrypsin; Cytokines; Interleukin-1β; LPS; mass-spectrometry; PBMCs; supernatants; total thiols}},
  language     = {{eng}},
  publisher    = {{Frontiers Media S. A.}},
  series       = {{Frontiers in Pharmacology}},
  title        = {{Indirect effect of alpha-1-antitrypsin on endotoxin-induced IL-1β secretion from human PBMCs}},
  url          = {{http://dx.doi.org/10.3389/fphar.2022.995869}},
  doi          = {{10.3389/fphar.2022.995869}},
  volume       = {{13}},
  year         = {{2022}},
}

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Indirect effect of alpha-1-antitrypsin on endotoxin-induced IL-1β secretion from human PBMCs