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Nephropathy in type 1 diabetes is associated with increased circulating activated platelets and platelet hyperreactivity.

机译:1型糖尿病的肾病与循环激活的血小板增多和血小板高反应性有关。

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Patients with diabetes mellitus (DM) have increased platelet activation compared to non-diabetic controls. Platelet hyperreactivity has been associated with adverse cardiovascular outcomes in Type 2 DM, and with diabetic nephropathy. We investigated the relationship between platelet activation and nephropathy in Type 1 DM. Patients with Type 1 DM and diabetic nephropathy (n = 35), age- and sex-matched Type 1 DM patients with persistent normoalbuminuria (n = 51), and healthy age- and sex-matched controls (n = 30) were studied. Platelet surface P-selectin, platelet surface activated GPIIb/IIIa, monocyte-platelet aggregates (MPAs) and neutrophil-platelet aggregates (NPAs) were measured by whole blood flow cytometry as markers of platelet activation. Platelet reactivity was assessed in response to exogenously added ADP and thrombin receptor activating peptide (TRAP). Platelet surface P-selectin (basal and in response to 0.5 or 20 microM ADP) was higher in nephropathy patients compared with normoalbuminuric patients (P = 0.027), and non-diabetic controls (P = 0.0057). NPAs were higher in nephropathy patients compared to normoalbuminuric patients (P = 0.0088). MPAs were higher in nephropathy patients compared to non-diabetic controls (P = 0.0075). There were no differences between groups in activated GPIIb/IIIa or in response to TRAP at any end-point. More patients with nephropathy received aspirin (71.4%) compared to normoalbuminuric patients (27.4%) (P < 0.0001). Type 1 diabetic nephropathy, as compared with normoalbuminuria, is associated with circulating activated platelets and platelet hyperreactivity to ADP, despite the confounding variable of more nephropathy patients receiving aspirin. This platelet activation is likely to contribute to the known increased risk of cardiovascular events in patients with diabetic nephropathy.
机译:与非糖尿病对照组相比,患有糖尿病(DM)的患者的血小板活化增加。血小板高反应性与2型DM的不良心血管预后以及糖尿病肾病有关。我们调查了1型糖尿病患者血小板活化与肾病之间的关系。研究对象为1型DM和糖尿病肾病(n = 35),年龄和性别相匹配的1型DM伴有持续性白蛋白尿(n = 51)和健康的年龄和性别相匹配的对照组(n = 30)。通过全血流式细胞术测量血小板表面P-选择素,血小板表面活化的GPIIb / IIIa,单核细胞-血小板聚集体(MPA)和中性粒细胞-血小板聚集体(NPA)作为血小板活化的标志。评估血小板反应性是对外源添加的ADP和凝血酶受体激活肽(TRAP)的反应。与正常白蛋白尿患者(P = 0.027)和非糖尿病对照组(P = 0.0057)相比,肾病患者的血小板表面P-选择素(基础和对0.5或20 microM ADP的反应)更高。与正常白蛋白尿患者相比,肾病患者的NPA更高(P = 0.0088)。与非糖尿病对照组相比,肾病患者的MPA更高(P = 0.0075)。在激活的GPIIb / IIIa或在任何终点对TRAP的反应之间,组之间没有差异。与正常白蛋白尿患者(27.4%)相比,接受阿司匹林治疗的肾病患者更多(71.4%)(P <0.0001)。与正常白蛋白尿相比,尽管有更多接受阿司匹林治疗的肾病患者存在混杂变量,但与正常白蛋白尿相比,1型糖尿病肾病与循环活化血小板和血小板对ADP的反应性强有关。血小板活化可能导致已知的糖尿病肾病患者发生心血管事件的风险增加。

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