Secreted phospholipase A2 type IIA as a mediator connecting innate and adaptive immunity: new role in atherosclerosis

doi:10.1093/cvr/cvn234

Cardiovascular Research Advance Access first published online on August 28, 2008
This version [Corrected Proof] published online on September 20, 2008
Cardiovascular Research, doi:10.1093/cvr/cvn234

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Secreted phospholipase A₂ type IIA as a mediator connecting innate and adaptive immunity: new role in atherosclerosis

Elvira Ibeas, Lucía Fuentes, Rubén Martín, Marita Hernández and Maria Luisa Nieto^*

Instituto de Biología y Genética Molecular, Consejo Superior de Investigaciones Científicas/Universidad de Valladolid, C/ Sanz y Fores s/n., 47005 Valladolid, Spain

^* Corresponding author. Tel: +34 983 184836; fax: +34 983 184800. E-mail address: mlnieto{at}ibgm.uva.es

Aims: Human atherosclerotic plaques express markers of macrophage/dendriticcells as well as high levels of inflammatory proteins such assecreted phospholipase A₂ type IIA (sPLA₂-IIA). To understandthe cellular changes associated with the progress of atherosclerosis,we evaluated the role of sPLA₂-IIA in mediating monocyte recruitmentand differentiation into antigen-presenting cells.

Methods and results: The effect of sPLA₂-IIA on monocyte differentiation was evaluatedin human THP-1 cells, a cellular line widely used as a modelfor monocyte–macrophage differentiation. Changes in functionalprocesses, morphology and expression of antigens, characteristicof differentiated cells, were monitored over a 1–3 dayperiod. sPLA₂-IIA inhibited CD14 expression in a time- and concentration-dependentmanner and upregulated dendritic cell-specific ICAM-3 grabbingnon-integrin levels at the cell surface, findings that werethe same for human monocytes. In addition, sPLA₂-IIA-differentiatedcells showed a dendritic cell phenotype characterized by thegeneration of fine dendritic protrusions and an increase insurface markers such as CD40, CD83, CD54, CD61, and CD62L. Furthermore,cell adhesion, migration, endocytic activity, and allogeneicT cell proliferation capacity were markedly increased aftersPLA₂-IIA treatment.

Conclusion: sPLA₂-IIA induces the differentiation of mononuclear cells andincreases their adhesive and migratory capabilities, which suggestsa novel function for sPLA₂-IIA as a mediator connecting innateand adaptive immunity. These findings may provide insight intothe immuno-inflammatory processes occurring in atherosclerosis,helping us to understand the cellular changes associated withthe development of atherosclerosis.

KEYWORDS Atherosclerosis; Dendritic cells; Macrophages; Inflammation; sPLA₂-IIA

Time for primary review: 23 days

These two authors contributed equally to this work.

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