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A conformational change in C-Reactive protein enhances leukocyte recruitment and reactive Oxygen species generation in Ischemia/Reperfusion injury

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peer-reviewed

Erstveröffentlichung
2018-04-16
Authors
Thiele, Jan R.
Zeller, Johannes
Kiefer, Jurij
Braig, David
Kreuzaler, Sheena
et al.
Wissenschaftlicher Artikel


Published in
Frontiers in Immunology ; 9 (2018). - Art.-Nr. 675. - eISSN 1664-3224
Link to original publication
https://dx.doi.org/10.3389/fimmu.2018.00675
Institutions
UKU. Institut für Klinische und Experimentelle Trauma-Immunologie
External cooperations
Roosevelt University
Universitätsklinikum Hamburg-Eppendorf
Albert-Ludwigs-Universität Freiburg
Baker Heart and Diabetes Institute
Document version
published version (publisher's PDF)
Abstract
Introduction C-reactive protein circulates as a pentameric protein (pCRP). pCRP is a well-established diagnostic marker as plasma levels rise in response to tissue injury and inflammation. We recently described pro-inflammatory properties of CRP, which are mediated by conformational changes from pCRP to bioactive isoforms expressing pro-inflammatory neo-epitopes [pCRP* and monomeric C-reactive protein (mCRP)]. Here, we investigate the role of CRP isoforms in renal ischemia/reperfusion injury (IRI). Methods Rat kidneys in animals with and without intraperitoneally injected pCRP were subjected to IRI by the time of pCRP exposure and were subsequently analyzed for monocyte infiltration, caspase-3 expression, and tubular damage. Blood urea nitrogen (BUN) was analyzed pre-ischemia and post-reperfusion. CRP effects on leukocyte recruitment were investigated via intravital imaging of rat-striated muscle IRI. Localized conformational CRP changes were analyzed by immunohistochemistry using conformation specific antibodies. 1,6-bis(phosphocholine)-hexane (1,6-bisPC), which stabilizes CRP in its native pentameric form was used to validate CRP effects. Leukocyte activation was assessed by quantification of reactive oxygen species (ROS) induction by CRP isoforms ex vivo and in vitro through electron spin resonance spectroscopy. Signaling pathways were analyzed by disrupting lipid rafts with nystatin and subsequent ROS detection. In order to confirm the translational relevance of our findings, biopsies of microsurgical human free tissue transfers before and after IRI were examined by immunofluorescence for CRP deposition and co-localization of CD68+ leukocytes. Results The application of pCRP aggravates tissue damage in renal IRI. 1,6-bisPC reverses these effects via inhibition of the conformational change that leads to exposure of pro-inflammatory epitopes in CRP (pCRP* and mCRP). Structurally altered CRP induces leukocyte–endothelial interaction and induces ROS formation in leukocytes, the latter can be abrogated by blocking lipid raft-dependent signaling pathways with Nystatin. Stabilizing pCRP in its native pentameric state abrogates these pro-inflammatory effects. Importantly, these findings are confirmed in human IRI challenged muscle tissue. Conclusion These results suggest that CRP is a potent modulator of IRI. Stabilizing the native pCRP conformation represents a promising anti-inflammatory therapeutic strategy by attenuation of leukocyte recruitment and ROS formation, the primary pathomechanisms of IRI.
Subject headings
[GND]: C-reaktives Protein | Leukozyt
[MeSH]: C-reactive protein | Ischemia | Reactive oxygen species | Leukocytes
[Free subject headings]: therapeutic targets | conformational change | translational medical research | leukocyte recruitment | rat models
[DDC subject group]: DDC 610 / Medicine & health
License
CC BY 4.0 International
https://creativecommons.org/licenses/by/4.0/

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DOI & citation

Please use this identifier to cite or link to this item: http://dx.doi.org/10.18725/OPARU-40187

Thiele, Jan R. et al. (2021): A conformational change in C-Reactive protein enhances leukocyte recruitment and reactive Oxygen species generation in Ischemia/Reperfusion injury. Open Access Repositorium der Universität Ulm und Technischen Hochschule Ulm. http://dx.doi.org/10.18725/OPARU-40187
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