IgG-complex stimulated platelets: A source of sCD40L and RANTES in initiation of inflammatory cascade

Platelets are a crucial element in maintenance of hemostasis. Other functions attributable to platelets are now being appreciated such as their role in inflammatory reactions and vascular remodeling. Platelets have been reported to bind immunological stimuli like IgG-complexes and the understanding...

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Bibliographic Details
Published in:Cellular immunology 2010, Vol.263 (1), p.129-133
Main Authors: Antczak, Adam J., Singh, Navinderjit, Gay, Steven R., Worth, Randall G.
Format: Article
Language:English
Subjects:
Antigen-Antibody Complex - immunology
Antigen-Antibody Complex - metabolism
Biomarkers - metabolism
Blood Platelets - immunology
Blood Platelets - metabolism
Blood Platelets - pathology
CD40 Ligand - biosynthesis
CD40 Ligand - genetics
CD40 Ligand - immunology
Cells, Cultured
Chemokine CCL5 - biosynthesis
Chemokine CCL5 - genetics
Chemokine CCL5 - immunology
Cytokines
Cytokines - secretion
FcγRIIA
Humans
IgG-complex
Inflammation
P-Selectin - biosynthesis
P-Selectin - genetics
P-Selectin - immunology
Platelet activation
Platelet Activation - immunology
RANTES
Receptors, Fibrinogen - biosynthesis
Receptors, Fibrinogen - genetics
Receptors, Fibrinogen - immunology
sCD40L
Thrombin - immunology
Thrombin - metabolism
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Summary:Platelets are a crucial element in maintenance of hemostasis. Other functions attributable to platelets are now being appreciated such as their role in inflammatory reactions and vascular remodeling. Platelets have been reported to bind immunological stimuli like IgG-complexes and the understanding that platelets may participate in immunological reactions has been speculated for nearly 50 years. In previous observations, we demonstrated that platelets could bind and internalize aggregated IgG-complexes without inducing platelet aggregation or granule release. To characterize this observation further, we tested the hypothesis that aggregated IgG-complexes do not activate platelets. To this end, platelets were stimulated with IgG-complexes or thrombin as a positive control and evaluated for activation by aggregation, expression of surface markers and production of cytokines. Activation with thrombin resulted in aggregation, expression of high levels of CD62P (P-selectin) expression and activation of the fibrinogen receptor, α IIbβ 3. Furthermore, stimulation with thrombin resulted in significant amounts of sCD40L (CD154) and RANTES (CCL5). However, platelets stimulated with IgG-complexes resulted in no aggregation and low levels of CD62P expression. Surprisingly, platelets stimulated with aggregated IgG-complexes released similar amounts of sCD40L and RANTES as platelets activated by thrombin. These data suggest that platelets are capable of secreting inflammatory molecules in response to IgG-complexes.
ISSN:0008-8749
1090-2163
DOI:10.1016/j.cellimm.2010.03.009