Thromb Haemost 2008; 99(03): 558-569
DOI: 10.1160/TH07-06-0410
Platelets and Blood Cells
Schattauer GmbH

C-reactive protein induces pro- and anti-inflammatory effects, including activation of the liver X receptor α, on human monocytes

Didier Hanriot*
1   INSERM, U684, Nancy, France
2   Henri Poincarè University, Nancy, France
,
Gaëlle Bello*
1   INSERM, U684, Nancy, France
2   Henri Poincarè University, Nancy, France
,
Armelle Ropars
1   INSERM, U684, Nancy, France
2   Henri Poincarè University, Nancy, France
,
Carole Seguin-Devaux
5   CRP-Sante, Luxembourg Hospital, Luxembourg
,
Gaël Poitevin
1   INSERM, U684, Nancy, France
2   Henri Poincarè University, Nancy, France
,
Sandrine Grosjean
3   CHU Nancy, Nancy, France
,
Vèronique Latger-Cannard
2   Henri Poincarè University, Nancy, France
3   CHU Nancy, Nancy, France
4   INSERM, U734, Nancy, France
,
Yvan Devaux
1   INSERM, U684, Nancy, France
2   Henri Poincarè University, Nancy, France
5   CRP-Sante, Luxembourg Hospital, Luxembourg
,
Faiez Zannad
1   INSERM, U684, Nancy, France
2   Henri Poincarè University, Nancy, France
,
Vèronique Regnault
2   Henri Poincarè University, Nancy, France
4   INSERM, U734, Nancy, France
,
Patrick Lacolley
1   INSERM, U684, Nancy, France
2   Henri Poincarè University, Nancy, France
,
Paul-Michel Mertes
1   INSERM, U684, Nancy, France
2   Henri Poincarè University, Nancy, France
,
Ketsia Hess*
1   INSERM, U684, Nancy, France
2   Henri Poincarè University, Nancy, France
,
Dan Longrois*
1   INSERM, U684, Nancy, France
2   Henri Poincarè University, Nancy, France
› Author Affiliations
Financial support: This work was supported financially by the Association de Recherche et d’Information Scientifique en Cardiologie (ARISC) and INSERM U689 by the Association des Infirmiers et Mèdecins Anesthésistes Rèanimateurs (AIMAR).
Further Information

Publication History

Received: 14 June 2007

Accepted after major revision: 23 January 2008

Publication Date:
07 December 2017 (online)

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Summary

Non-specific markers of inflammation such as C-reactive protein (CRP) are associated statistically with an increased risk of atherosclerosis through mechanisms that have not yet been fully elucidated.We investigated the effects of CRP on several aspects of human monocyte biology, a cell type involved in the initiation and progression of atherosclerosis. Blood monocytes isolated from healthy men and premenopausal women (n=9/group) were exposed to purified CRP (25 μg/ml) for 12 hours. Changes in gene expression were analyzed using a custom-made array containing oligonucleotide sequences of 250 genes expressed by activated monocytes and confirmed by quantitative PCR. CRP increased significantly the expression of the cytokines interleukin (IL)-1α, IL-1β and IL-6, and the chemokines GRO-α, GRO-β and IL-8. CRP also displayed anti-inflammatory effects through upregulation of liver X receptor (LXR) α and activin receptor expression, and down-regulation of alpha 2-macroglobulin expression. Increased LXRα mRNA expression in both monocytes and the monocytic cell lineTHP-1 was associated with increased LXRα protein expression and nuclear translocation, as well as increased ABCA1 mRNA expression, a target gene of LXRα. Western Blot analysis revealed CRP-induced nuclear translocation of NF-κB and activation of p42/44, MAP and Akt kinases. CRP-induced LXRá mRNA expression was inhibited by anti-CD64 (FcγRI) antibodies and by p42/44 and PI3 kinase inhibitors. This hypothesis-generating study demonstrates that CRP modulates the expression of genes that contribute to both pro- and anti-inflammatory responses in human monocytes. Among these novel anti-inflammatory effects, we show clearly that CRP activates the LXRα pathway.

Notes

* These authors contributed equally to this work.