Platelet Prothrombinase Activity, a Final Pathway Platelet Procoagulant Activity, Is Overexpressed in Type 1 Diabetes: No Relationship With Mean Platelet Volume or Background Retinopathy

Abstract

There is overwhelming evidence that platelets from diabetic individuals are hyperreactive, not only when mi crovascular complications are apparent, but already at an early stage of the disease. There is still controversy about the ques tion of whether primary hyperreactive platelets may contribute to the origin or progression of microangiopathy or whether diabetic platelet hyperfunctionality is just a logical conse quence of a continuous low-grade activation of platelets by contact with a diseased microvascular wall. As a consequence of platelet activation, the outer layer of its phospholipid mem brane is more procoagulant than in the quiescent state, stimu lating thrombin formation in plasma. This platelet function is called platelet procoagulant activity. We studied platelet pro thrombinase activity (PPA), a final pathway platelet procoagu lant activity of type 1 diabetic platelets, and looked for an eventual correlation with microvascular disease (background retinopathy) and mean platelet volume (MPV). Stypven clot ting times (SCTs), reflecting PPA expression, and MPV of citrated platelet-rich plasma (PRP), were measured in 21 pa tients with type 1 diabetes—10 with and 11 without back ground retinopathy—under clinically acceptable metabolic control and compared them to 20 disease-free voluntary con trols. We also compared PPA expression and MPV in diabetic individuals with and without retinopathy. With the SCT, a se lective test adapted for studying PPA in PRP, we found hyper expression of PPA in all diabetic patients. We found no differ ence in MPV between diabetic and control PRP. Comparing patients with and without background retinopathy we found no significant difference in PPA expression. From these results, we suggest that the phospholipid surface of diabetic platelets, more than the surface of normal control platelets, stimulate the expression of PPA. This diabetic platelet coagulant anomaly was not related to an increased platelet mass (higher MPV) nor to the presence of microangiopathy. We conclude that PPA hyperexpression is associated with patients with type 1 diabe tes, already occurring in an early stage of the disease, and not necessarily a consequence of early-stage microvascular disease, because the anomaly is also demonstrable, in the same degree, in patients with diabetes without microangiopathy.