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Aspirin treatment hampers the use of plasma microRNA-126 as a biomarker for the progression of vascular disease

Authors :
Ton J. Rabelink
Menno V. Huisman
Jacques M.G.J. Duijs
Hetty C. de Boer
Coen van Solingen
Jurriën Prins
Anton Jan van Zonneveld
Source :
European Heart Journal, 34(44), 3451-3457
Publication Year :
2013

Abstract

Aims MicroRNA-126 (miR-126) facilitates angiogenesis and regulates endothelial cell function. Recent data suggest that miR-126 can serve as a biomarker for vascular disease. Although endothelial cells are enriched for miR-126, platelets also contain miR-126. In this paper, we investigated the contribution of platelets to the pool of miR-126 in plasma of patients with type 2 diabetes (DM2) and how this is affected by aspirin. Methods and results In vitro platelet activation resulted in the transfer of miR-126 from the platelet to the plasma compartment, which was prevented by aspirin. In vivo platelet activation, monitored in patients with DM2 by measuring soluble P-selectin, correlated directly with circulating levels of miR-126. The administration of aspirin resulted both in platelet inhibition and concomitantly reduced circulating levels of platelet-derived microRNAs including miR-126. Conclusion Platelets are a major source of circulating miR-126. Consequently, in patho-physiological conditions associated with platelet activation, such as diabetes type 2, the administration of aspirin may lead to reduced levels of circulating miR-126. Thus, the use of platelet inhibitors should be taken into account when using plasma levels of miR-126 as a biomarker.

Details

Language :
English
Database :
OpenAIRE
Journal :
European Heart Journal, 34(44), 3451-3457
Accession number :
edsair.doi.dedup.....8d8a10bcda45602b6583ff4aeb0ee3d3